Guideline ADA 2010

Standards of Medical Care in Diabetes2010
AMERICAN DIABETES ASSOCIATION

D
iabetes is a chronic illness that re-
quires continuing medical care and
ongoing patient self-management
education and support to prevent acute
complications and to reduce the risk of
long-term complications. Diabetes care is
complex and requires that many issues,
beyond glycemic control, be addressed. A
large body of evidence exists that sup-
ports a range of interventions to improve
diabetes outcomes.
These standards of care are intended
to provide clinicians, patients, research-
ers, payors, and other interested individ-
uals with the components of diabetes
care, general treatment goals, and tools to
evaluate the quality of care. While indi-
vidual preferences, comorbidities, and
other patient factors may require modi-
cation of goals, targets that are desirable
for most patients with diabetes are pro-
vided. These standards are not intended
to preclude clinical judgment or more ex-
tensive evaluation and management of the
patient by other specialists as needed. For
more detailed information about manage-
ment of diabetes, refer to references 13.
The recommendations included are
screening, diagnostic, and therapeutic ac-
tions that are known or believed to favor-
ably affect health outcomes of patients
with diabetes. Agrading system(Table 1),
developed by the American Diabetes As-
sociation (ADA) and modeled after exist-
ing methods, was used to clarify and
codify the evidence that forms the basis
for the recommendations. The level of ev-
idence that supports each recommenda-
tion is listed after each recommendation
using the letters A, B, C, or E.
These standards of care are revised
annually by the ADA multidisciplinary
Professional Practice Committee, and
new evidence is incorporated. Members
of the Professional Practice Committee
and their disclosed conicts of interest are
listed in the Introduction. Subsequently,
as with all position statements, the stan-
dards of care are reviewed and approved
by the Executive Committee of ADAs
Board of Directors.
I. CLASSIFICATION AND
DIAGNOSIS
A. Classication
The classication of diabetes includes
four clinical classes:
type 1 diabetes (results from -cell de-

struction, usually leading to absolute
insulin deciency)
type 2 diabetes (results from a progres-

sive insulin secretory defect on the
background of insulin resistance)
other specic types of diabetes due to

other causes, e.g., genetic defects in
-cell function, genetic defects in insu-
lin action, diseases of the exocrine pan-
creas (such as cystic brosis), and drug-
or chemical-induced diabetes (such as
in the treatment of AIDS or after organ
transplantation)
gestational diabetes mellitus (GDM)

(diabetes diagnosed during pregnancy)
Some patients cannot be clearly classied
as having type 1 or type 2 diabetes. Clin-
ical presentation and disease progression
vary considerably in both types of diabe-
tes. Occasionally, patients who otherwise
have type 2 diabetes may present with ke-
toacidosis. Similarly, patients with type 1
diabetes may have a late onset and slow
(but relentless) progression despite hav-
ing features of autoimmune disease. Such
difculties in diagnosis may occur in chil-
dren, adolescents, and adults. The true
diagnosis may become more obvious over
time.
B. Diagnosis of diabetes
Recommendations
For decades, the diagnosis of diabetes has
been based on plasma glucose (PG) crite-
ria, either fasting PG (FPG) or 2-h 75-g
oral glucose tolerance test (OGTT) values.
In 1997, the rst Expert Committee on
the Diagnosis and Classication of Diabe-
tes Mellitus revised the diagnostic criteria
using the observed association between

Originally approved 1988. Most recent review/revision October 2009.
DOI: 10.2337/dc10-S011
Abbreviations: ABI, ankle-brachial index; ACCORD, Action to Control Cardiovascular Risk in Diabetes;
ADAG, A1C-Derived Average Glucose Trial; ADVANCE, Action in Diabetes and Vascular Disease: Pre-
terax and Diamicron Modied Release Controlled Evaluation; ACE, angiotensin converting enzyme; ARB,
angiotensin receptor blocker; ACT-NOW, ACTos Now Study for the Prevention of Diabetes; BMI, body
mass index; CBG, capillary blood glucose; CFRD, cystic brosisrelated diabetes; CGM, continuous
glucose monitoring; CHD, coronary heart disease; CHF, congestive heart failure; CCM, chronic care
model; CKD, chronic kidney disease; CMS, Centers for Medicare and Medicaid Services; CSII, continuous
subcutaneous insulin infusion; CVD, cardiovascular disease; DASH, Dietary Approaches to Stop Hyper-
tension; DCCT, Diabetes Control and Complications Trial; DKA, diabetic ketoacidosis; DMMP, diabetes
medical management plan; DPN, distal symmetric polyneuropathy; DPP, Diabetes Prevention Program;
DPS, Diabetes Prevention Study; DREAM, Diabetes Reduction Assessment with Ramipril and Rosiglita-
zone Medication; DRS, Diabetic Retinopathy Study; DSME, diabetes self-management education; DSMT,
diabetes self-management training; eAG, estimated average glucose; eGFR, estimated glomerular ltration
rate; ECG, electrocardiogram; EDIC, Epidemiology of Diabetes Interventions and Complications; ERP,
education recognition program; ESRD, end-stage renal disease; ETDRS, Early Treatment Diabetic Reti-
nopathy Study; FDA, Food and Drug Administration; FPG, fasting plasma glucose; GDM, gestational
diabetes mellitus; GFR, glomerular ltration rate; HAPO, Hyperglycemia and Adverse Pregnancy Out-
comes; ICU, intensive care unit; IFG, impaired fasting glucose; IGT, impaired glucose tolerance; Look
AHEAD, Action for Health in Diabetes; MDRD, Modication of Diet in Renal Disease; MNT, medical
nutrition therapy; NDEP, National Diabetes Education Program; NGSP, National Glycohemoglobin Stan-
dardization Program; NPDR, nonproliferative diabetic retinopathy; OGTT, oral glucose tolerance test;
PAD, peripheral arterial disease; PCOS, polycystic ovarian syndrome; PDR, proliferative diabetic retinop-
athy; PPG, postprandial plasma glucose; RAS, renin-angiotensin system; SMBG, self-monitoring of blood
glucose; STOP-NIDDM, Study to Prevent Non-Insulin Dependent Diabetes; SSI, sliding scale insulin;
TZD, thiazolidinedione; UKPDS, U.K. Prospective Diabetes Study; VADT, Veterans Affairs Diabetes Trial;
XENDOS, XENical in the prevention of Diabetes in Obese Subjects.
2010 by the American Diabetes Association. Readers may use this article as long as the work is properly
cited, the use is educational and not for prot, and the work is not altered. See http://creativecommons.
org/licenses/by-nc-nd/3.0/ for details.
P O S I T I O N S T A T E M E N T
care.diabetesjournals.org DIABETES CARE, VOLUME 33, SUPPLEMENT 1, JANUARY 2010 S11
glucose levels and presence of retinopa-
thy as the key factor with which to iden-
tify threshold FPG and 2-h PG levels. The
committee examined data from three
cross-sectional epidemiologic studies that
assessed retinopathy with fundus photog-
raphy or direct ophthalmoscopy and
measured glycemia as FPG, 2-h PG, and
HbA
1c
(A1C). The studies demonstrated
glycemic levels belowwhich there was lit-
tle prevalent retinopathy and above
which the prevalence of retinopathy in-
creased in an apparently linear fashion.
The deciles of FPG, 2-h PG, and A1C at
which retinopathy began to increase were
the same for each measure within each
population. The analyses helped to in-
form a then-new diagnostic cut point of
126 mg/dl (7.0 mmol/l) for FPG and
conrmed the long-standing diagnostic
2-h PG value of 200 mg/dl (11.1
mmol/l) (4).
ADA has not previously recom-
mended the use of A1C for diagnosing
diabetes, in part due to lack of standard-
ization of the assay. However, A1C assays
are nowhighly standardized, and their re-
sults can be uniformly applied both tem-
porally and across populations. In a
recent report (5), after an extensive review
of both established and emerging epide-
miological evidence, an international ex-
pert committee recommended the use of
the A1C test to diagnose diabetes with a
threshold of 6.5%, and ADAafrms this
decision (6). The diagnostic test should
be performed using a method certied by
the National Glycohemoglobin Standard-
ization Program (NGSP) and standard-
ized or traceable to the Diabetes Control
and Complications Trial (DCCT) refer-
ence assay. Point-of-care A1C assays are
not sufciently accurate at this time to use
for diagnostic purposes.
Epidemiologic datasets show a rela-
tionship between A1C and the risk of ret-
inopathy similar to that which has been
shown for corresponding FPGand 2-h PG
thresholds. The A1C has several advan-
tages to the FPG, including greater conve-
nience, since fasting is not required;
evidence to suggest greater preanalytical
stability; and less day-to-day perturba-
tions during periods of stress and illness.
These advantages must be balanced by
greater cost, limited availability of A1C
testing in certain regions of the develop-
ing world, and incomplete correlation be-
tween A1C and average glucose in certain
individuals. In addition, the A1C can be
misleading in patients with certain forms
of anemia and hemoglobinopathies. For
patients with a hemoglobinopathy but
normal red cell turnover, such as sickle
cell trait, an A1C assay without interfer-
ence from abnormal hemoglobins should
be used (an updated list of A1Cassays and
whether abnormal hemoglobins impact
them is available at www.ngsp.org/prog/
index3.html). For conditions with abnor-
mal red cell turnover, such as pregnancy or
anemias from hemolysis and iron de-
ciency, the diagnosis of diabetes must use
glucose criteria exclusively.
The established glucose criteria for
the diagnosis of diabetes (FPG and 2-h
PG) remain valid. Patients with severe hy-
perglycemia such as those who present
with severe classic hyperglycemic symp-
toms or hyperglycemic crisis can continue
to be diagnosed when a random (or ca-
sual) PG of 200 mg/dl (11.1 mmol/l) is
found. It is likely that in such cases the
health care professional would also con-
duct an A1C test as part of the initial as-
sessment of the severity of the diabetes
and that it would be above the diagnostic
cut point. However, in rapidly evolving
diabetes such as the development of type
1 in some children, the A1C may not be
signicantly elevated despite frank
diabetes.
Just as there is 100% concordance
between the FPG and 2-h PG tests, there
is not perfect concordance between A1C
and either glucose-based test. Analyses of
National Health and Nutrition Examina-
tion Survey (NHANES) data indicate that,
assuming universal screening of the undi-
agnosed, the A1C cut point of 6.5%
identies one-third fewer cases of undiag-
nosed diabetes than a fasting glucose cut
point of 126 mg/dl (7.0 mmol/l) (E.
Gregg, personal communication). How-
ever, in practice, a large portion of the
diabetic population remains unaware of
their condition. Thus, the lower sensitiv-
ity of A1Cat the designated cut point may
well be offset by the tests greater practi-
cality, and wider application of a more
convenient test (A1C) may actually in-
crease the number of diagnoses made.
As with most diagnostic tests, a test
result diagnostic of diabetes should be re-
peated to rule out laboratory error, unless
the diagnosis is clear on clinical grounds,
such as a patient with classic symptoms of
hyperglycemia or hyperglycemic crisis. It
is preferable that the same test be repeated
for conrmation, since there will be a
greater likelihood of concurrence in this
case. For example, if the A1C is 7.0% and
a repeat result is 6.8%, the diagnosis of
diabetes is conrmed. However, there are
scenarios in which results of two different
tests (e.g., FPG and A1C) are available for
the same patient. In this situation, if the
two different tests are both above the di-
Table 1 ADA evidence grading system for clinical practice recommendations
Level of
evidence Description
A Clear evidence from well-conducted, generalizable, randomized controlled trials that
are adequately powered, including:
Evidence from a well-conducted multicenter trial
Evidence from a meta-analysis that incorporated quality ratings in the analysis
Compelling nonexperimental evidence, i.e., all or none rule developed by Center
for Evidence Based Medicine at Oxford
Supportive evidence from well-conducted randomized controlled trials that are
adequately powered, including:
Evidence from a well-conducted trial at one or more institutions
Evidence from a meta-analysis that incorporated quality ratings in the analysis
B Supportive evidence from well-conducted cohort studies:
Evidence from a well-conducted prospective cohort study or registry
Evidence from a well-conducted meta-analysis of cohort studies
Supportive evidence from a well-conducted case-control study
C Supportive evidence from poorly controlled or uncontrolled studies
Evidence from randomized clinical trials with one or more major or three or
more minor methodological aws that could invalidate the results
Evidence from observational studies with high potential for bias (such as case
series with comparison to historical controls)
Evidence from case series or case reports
Conicting evidence with the weight of evidence supporting the recommendation
E Expert consensus or clinical experience
Standards of Medical Care
S12 DIABETES CARE, VOLUME 33, SUPPLEMENT 1, JANUARY 2010 care.diabetesjournals.org
agnostic threshold, the diagnosis of dia-
betes is conrmed.
On the other hand, if two different
tests are available in an individual and the
results are discordant, the test whose re-
sult is above the diagnostic cut point
should be repeated, and the diagnosis is
made on the basis of the conrmed test.
That is, if a patient meets the diabetes cri-
terion of the A1C(two results 6.5%) but
not the FPG(126 mg/dl or 7.0 mmol/l),
or vice versa, that person should be con-
sidered to have diabetes. Admittedly, in
most circumstance the nondiabetic test
is likely to be in a range very close to the
threshold that denes diabetes.
Since there is preanalytic and analytic
variability of all the tests, it is also possible
that when a test whose result was above
the diagnostic threshold is repeated, the
second value will be below the diagnostic
cut point. This is least likely for A1C,
somewhat more likely for FPG, and most
likely for the 2-h PG. Barring a laboratory
error, such patients are likely to have test
results near the margins of the threshold
for a diagnosis. The healthcare profes-
sional might opt to follow the patient
closely and repeat the testing in 36
months.
The current diagnostic criteria for di-
abetes are summarized in Table 2.
C. Categories of increased risk for
diabetes
In 1997 and 2003, The Expert Committee
on the Diagnosis and Classication of Di-
abetes Mellitus (4,7) recognized an inter-
mediate group of individuals whose
glucose levels, although not meeting cri-
teria for diabetes, are nevertheless too
high to be considered normal. This group
was dened as having impaired fasting
glucose (IFG) (FPG levels of 100 mg/dl
[5.6 mmol/l] to 125 mg/dl [6.9 mmol/l])
or impaired glucose tolerance (IGT) (2-h
OGTT values of 140 mg/dl [7.8 mmol/l]
to 199 mg/dl [11.0 mmol/l]).
Individuals with IFGand/or IGT have
been referred to as having pre-diabetes,
indicating the relatively high risk for the
future development of diabetes. IFG and
IGT should not be viewed as clinical en-
tities in their own right but rather risk
factors for diabetes as well as cardiovas-
cular disease (CVD). IFG and IGT are
associated with obesity (especially
abdominal or visceral obesity), dyslipide-
mia with high triglycerides and/or low
HDL cholesterol, and hypertension.
Structured lifestyle intervention, aimed at
increasing physical activity and produc-
ing 510% loss of body weight, and cer-
tain pharmacological agents have been
demonstrated to prevent or delay the de-
velopment of diabetes in people with IGT
(see Table 7). It should be noted that the
2003 ADA Expert Committee report re-
duced the lower FPG cut point to dene
IFG from 110 mg/dl (6.1 mmol/l) to 100
mg/dl (5.6 mmol/l), in part to make the
prevalence of IFG more similar to that of
IGT. However, the World Health Organi-
zation (WHO) and many other diabetes
organizations did not adopt this change.
As the A1C becomes increasingly
used to diagnose diabetes in individuals
with risk factors, it will also identify those
at high risk for developing diabetes in the
future. As was the case with the glucose
measures, dening a lower limit of an in-
termediate category of A1C is somewhat
arbitrary, since risk of diabetes with any
measure or surrogate of glycemia is a con-
tinuum extending well into the normal
ranges. To maximize equity and efciency
of preventive interventions, such an A1C
cut point, should balance the costs of false
negatives (failing to identify those who are
going to develop diabetes) against the
costs of false positives (falsely identifying
and then spending intervention resources
on those who were not going to develop
diabetes anyway).
Linear regression analyses of nation-
ally representative U.S. data (NHANES
20052006) indicate that among the
nondiabetic adult population, an FPG of
110 mg/dl corresponds to an A1C of
5.6%, while an FPG of 100 mg/dl corre-
sponds to an A1C of 5.4%. Receiver op-
erating curve analyses of these data
indicate that an A1C value of 5.7%, com-
pared with other cut points, has the best
combination of sensitivity (39%) and
specicity (91%) to identify cases of IFG
(FPG 100 mg/dl [5.6 mmol/l]) (R.T.
Ackerman, Personal Communication).
Other analyses suggest that an A1C of
5.7% is associated with diabetes risk sim-
ilar to that of the high-risk participants in
the Diabetes Prevention Program (DPP)
(R.T. Ackerman, personal communica-
tion). Hence, it is reasonable to consider
an A1C range of 5.76.4% as identifying
individuals with high risk for future dia-
betes and to whom the term pre-diabetes
may be applied (6).
As is the case for individuals found to
have IFG and IGT, individuals with an
A1C of 5.76.4% should be informed of
their increased risk for diabetes as well
as CVD and counseled about effective
strategies to lower their risks (see IV. PRE-
VENTION/DELAYOFTYPE2DIABETES).
As with glucose measurements, the contin-
uum of risk is curvilinear, so that as A1C
rises, the risk of diabetes rises dispropor-
tionately. Accordingly, interventions
should be most intensive and follow-up
should be particularly vigilant for those
with an A1C 6.0%, who should be con-
sidered to be at very high risk. However,
just as anindividual witha fastingglucose of
98 mg/dl (5.4 mmol/l) may not be at negli-
gible risk for diabetes, individuals with an
A1C 5.7%may still be at risk, depending
on the level of A1C and presence of other
risk factors, such as obesity and family
history.
Table 2Criteria for the diagnosis of diabetes
1. A1C 6.5%. The test should be performed in a laboratory using a method
that is NGSP certied and standardized to the DCCT assay.*
OR
2. FPG 126 mg/dl (7.0 mmol/l). Fasting is dened as no caloric intake for at
least 8 h.*
OR
3. Two-hour plasma glucose 200 mg/dl (11.1 mmol/l) during an OGTT.
The test should be performed as described by the World Health
Organization, using a glucose load containing the equivalent of 75 g
anhydrous glucose dissolved in water.*
OR
4. In a patient with classic symptoms of hyperglycemia or hyperglycemic
crisis, a random plasma glucose 200 mg/dl (11.1 mmol/l).
*In the absence of unequivocal hyperglycemia, criteria 13 should be conrmed by repeat testing.
Table 3Categories of increased risk for
diabetes*
FPG 100125 mg/dl (5.66.9 mmol/l)
IFG
2-h PG on the 75-g OGTT 140199 mg/dl
(7.811.0 mmol/l) IGT
A1C 5.76.4%
*For all three tests, risk is continuous, extending
below the lower limit of the range and becoming
disproportionately greater at higher ends of the
range.
Position Statement
Table 3 summarizes the categories of
increased risk for diabetes.
II. TESTING FOR DIABETES
IN ASYMPTOMATIC
PATIENTS
Recommendations
Testing to detect type 2 diabetes and

assess risk for future diabetes in asymp-
tomatic people should be considered in
adults of any age who are overweight or
obese (BMI 25 kg/m
2
) and who have
one or more additional risk factors for
diabetes (Table 4). In those without
these risk factors, testing should begin
at age 45 years. (B)
If tests are normal, repeat testing should

be carried out at least at 3-year inter-
vals. (E)
To test for diabetes or to assess risk of

future diabetes, either A1C, FPG , or
2-h 75-g OGTT are appropriate. (B)
In those identied with increased risk

for future diabetes, identify and, if ap-
propriate, treat other CVD risk factors.
(B)
For many illnesses there is a major dis-
tinction between screening and diagnos-
tic testing. However, for diabetes the same
tests would be used for screening as for
diagnosis. Type 2 diabetes has a long
asymptomatic phase and signicant clin-
ical risk markers. Diabetes may be identi-
ed anywhere along a spectrumof clinical
scenarios ranging from a seemingly low-
risk individual who happens to have glu-
cose testing, to a higher-risk individual
who the provider tests because of high
suspicion of diabetes, to the symptomatic
patient. The discussion herein is primar-
ily framed as testing for diabetes in indi-
viduals without symptoms. Testing for
diabetes will also detect individuals at in-
creased future risk for diabetes, herein re-
ferred to as pre-diabetic.
A. Testing for type 2 diabetes and
risk of future diabetes in adults
Type 2 diabetes is frequently not diag-
nosed until complications appear, and
approximately one-fourth of all people
with diabetes in the U.S. may be undiag-
nosed. Although the effectiveness of early
identication of pre-diabetes and diabetes
through mass testing of asymptomatic in-
dividuals has not been proven denitively
(and rigorous trials to provide such proof
are unlikely to occur), pre-diabetes and
diabetes meet established criteria for con-
ditions in which early detection is appro-
priate. Both conditions are common, are
increasing in prevalence, and impose sig-
nicant public health burdens. There is a
long presymptomatic phase before the di-
agnosis of type 2 diabetes is usually made.
Relatively simple tests are available to de-
tect preclinical disease (9). Additionally,
the duration of glycemic burden is a
strong predictor of adverse outcomes,
and effective interventions exist to pre-
vent progression of pre-diabetes to diabe-
tes (see IV. PREVENTION/DELAY OF
TYPE 2 DIABETES) and to reduce risk of
complications of diabetes (see VI. PRE-
VENTION AND MANAGEMENT OF DI-
ABETES COMPLICATIONS).
Recommendations for testing for dia-
betes in asymptomatic undiagnosed
adults are listed in Table 4. Testing should
be considered in adults of any age with
BMI 25 kg/m
2
and one or more risk fac-
tors for diabetes. Because age is a major
risk factor for diabetes, testing of those
without other risk factors should begin no
later than at age 45 years.
Either A1C, FPG, or 2-h OGTT is ap-
propriate for testing. The 2-h OGTT identi-
es people with either IFGor IGT and thus
more people at increased risk for the devel-
opment of diabetes and CVD. It should be
noted that the two tests do not necessarily
detect the same individuals (10). The ef-
cacy of interventions for primary preven-
tion of type 2 diabetes (1117) has
primarily been demonstrated among indi-
viduals with IGT, but not for individuals
with IFG (who do not also have IGT) or
those with specic A1C levels.
The appropriate interval between
tests is not known (18). The rationale for
the 3-year interval is that false negatives
will be repeated before substantial time
elapses, and there is little likelihood that
an individual will develop signicant
complications of diabetes within 3 years
of a negative test result.
Because of the need for follow-up and
discussion of abnormal results, testing
should be carried out within the health
care setting. Community screening out-
side a health care setting is not recom-
mended because people with positive
tests may not seek, or have access to, ap-
propriate follow-up testing and care.
Conversely, there may be failure to ensure
appropriate repeat testing for individuals
who test negative. Community screening
may also be poorly targeted, i.e., it may
fail to reach the groups most at risk and
inappropriately test those at low risk (the
worried well) or even those already diag-
nosed (19,20).
B. Testing for type 2 diabetes in
children
The incidence of type 2 diabetes in ado-
lescents has increased dramatically in the
last decade, especially in minority popu-
lations (21), although the disease remains
rare in the general pediatric population
(22). Consistent with recommendations
for adults, children and youth at in-
creased risk for the presence or the devel-
opment of type 2 diabetes should be
tested within the health care setting (23).
The recommendations of the ADA con-
sensus statement on type 2 diabetes in
Table 4Criteria for testing for diabetes in asymptomatic adult individuals
1. Testing should be considered in all adults who are overweight (BMI 25 kg/m
2
*) and
have additional risk factors:
physical inactivity
rst-degree relative with diabetes
members of a high-risk ethnic population (e.g., African American, Latino, Native
American, Asian American, Pacic Islander)
women who delivered a baby weighing 9 lb or were diagnosed with GDM
hypertension (140/90 mmHg or on therapy for hypertension)
HDL cholesterol level 35 mg/dl (0.90 mmol/l) and/or a triglyceride level 250
mg/dl (2.82 mmol/l)
women with polycystic ovary syndrome
A1C 5.7%, IGT, or IFG on previous testing
other clinical conditions associated with insulin resistance (e.g., severe obesity,
acanthosis nigricans)
history of CVD
2. In the absence of the above criteria, testing diabetes should begin at age 45 years
3. If results are normal, testing should be repeated at least at 3-year intervals, with
consideration of more frequent testing depending on initial results and risk
status.
*At-risk BMI may be lower in some ethnic groups.
children and youth, with some modica-
tions, are summarized in Table 5.
C. Screening for type 1 diabetes
Generally, people with type 1 diabetes
present with acute symptoms of diabetes
and markedly elevated blood glucose lev-
els, and most cases are diagnosed soon
after the onset of hyperglycemia. How-
ever, evidence from type 1 diabetes pre-
vention studies suggests that measurement
of islet autoantibodies identies individ-
uals who are at risk for developing type 1
diabetes. Such testing may be appropriate
in high-risk individuals, such as those
with prior transient hyperglycemia or
those who have relatives with type 1 dia-
betes, in the context of clinical research
studies (see, for example, http://www2.
diabetestrialnet.org). Widespread clini-
cal testing of asymptomatic low-risk
individuals cannot currently be recom-
mended, as it would identify very few in-
dividuals in the general population who
are at risk. Individuals who screen posi-
tive should be counseled about their risk
of developing diabetes. Clinical studies
are being conducted to test various meth-
ods of preventing type 1 diabetes or re-
versing early type 1 diabetes in those with
evidence of autoimmunity.
III. DETECTION AND
DIAGNOSIS OF GDM
Recommendations
Screen for GDM using risk factor anal-

ysis and, if appropriate, an OGTT. (C)
Women with GDM should be screened

for diabetes 612 weeks postpartum
and should be followed up with subse-
quent screening for the development of
diabetes or pre-diabetes. (E)
For many years, GDMhas been dened as
any degree of glucose intolerance with on-
set or rst recognition during pregnancy
(4). Although most cases resolve with de-
livery, the denition applied whether the
condition persisted after pregnancy and
did not exclude the possibility that unrec-
ognized glucose intolerance may have an-
tedated or begun concomitantly with the
pregnancy. This denition facilitated a
uniform strategy for detection and classi-
cation of GDM, but its limitations were
recognized for many years. As the ongo-
ing epidemic of obesity and diabetes has
led to more type 2 diabetes in women of
childbearing age, the number of pregnant
women with undiagnosed type 2 diabetes
has increased (24). After deliberations in
20082009, the International Associa-
tion of Diabetes and Pregnancy Study
Groups (IADPSG), an international con-
sensus group with representatives from
multiple obstetrical and diabetes organi-
zations, including ADA, recommended
that high-risk women found to have dia-
betes at their initial prenatal visit using
standard criteria (Table 2) receive a diag-
nosis of overt, not gestational, diabetes.
Approximately 7% of all pregnancies
(ranging from1 to 14%depending on the
population studied and the diagnostic
tests used) are complicated by GDM, re-
sulting in more than 200,000 cases
annually.
Because of the risks of GDM to the
mother and neonate, screening and diag-
nosis are warranted. Current screening
and diagnostic strategies, based on the
2004 ADA position statement on GDM
(25), are outlined in Table 6.
Results of the Hyperglycemia and Ad-
verse Pregnancy Outcomes (HAPO) study
(26), a large-scale (25,000 pregnant
women) multinational epidemiologic
study, demonstrated that risk of adverse
maternal, fetal, and neonatal outcomes
continuously increased as a function of
maternal glycemia at 2428 weeks, even
within ranges previously considered nor-
mal for pregnancy. For most complica-
tions there was no threshold for risk.
These results have led to careful reconsid-
eration of the diagnostic criteria for GDM.
The IADPSG recommended that all
women not known to have prior diabetes
undergo a 75-g OGTT at 2428 weeks of
gestation. The group developed diagnos-
tic cut points for the fasting, 1-h, and 2-h
PG measurements that conveyed an odds
ratio for adverse outcomes of at least 1.75
compared with women with the mean
glucose levels in the HAPO study.
At the time of this update to the Stan-
dards of Medical Care in Diabetes, ADA is
planning to work with U.S. obstetrical or-
ganizations to consider adoption of the
IADPSG diagnostic criteria and to discuss
the implications of this change. While this
change will signicantly increase the
prevalence of GDM, there is mounting ev-
idence that treating even mild GDM re-
duces morbidity for both mother and
baby (27).
Because women with a history of
GDMhave a greatly increased subsequent
risk for diabetes (28), they should be
screened for diabetes 612 weeks post-
partum, using nonpregnant OGTT crite-
ria, and should be followed up with
subsequent screening for the develop-
ment of diabetes or pre-diabetes, as out-
lined in II. TESTING FOR DIABETES IN
ASYMPTOMATIC PATIENTS. Informa-
tion on the National Diabetes Education
Program (NDEP) campaign to prevent
type 2 diabetes in women with GDM can
be found at http://ndep.nih.gov/media/
NeverTooEarly_Tipsheet.pdf.
IV. PREVENTION/DELAY
OF TYPE 2 DIABETES
Recommendations
Patients with IGT (A), IFG (E), or an

A1C of 5.76.4% (E) should be re-
ferred to an effective ongoing support
program for weight loss of 510% of
body weight and an increase in physical
activity of at least 150 min/week of
moderate activity such as walking.
Follow-up counseling appears to be im-

portant for success. (B)
Based on potential cost savings of dia-

betes prevention, such counseling
should be covered by third-party pay-
ors. (E)
In addition to lifestyle counseling, met-

formin may be considered in those who
are at very high risk for developing di-
abetes (combined IFG and IGT plus
Table 5Testing for type 2 diabetes in asymptomatic children
Criteria: Overweight (BMI 85th percentile for age and sex, weight for height
85th percentile, or weight 120% of ideal for height)
Plus any two of
the following
risk factors:
Family history of type 2 diabetes in rst- or second-degree relative
Race/ethnicity (Native American, African American, Latino, Asian
American, Pacic Islander)
Signs of insulin resistance or conditions associated with insulin
resistance (acanthosis nigricans, hypertension, dyslipidemia,
polycystic ovary syndrome, or small for gestational age
birthweight)
Maternal history of diabetes or GDM during the childs gestation
Age of
initiation:
Age 10 years or at onset of puberty, if puberty occurs at a younger
age
Frequency: Every 3 years
Position Statement
other risk factors such as A1C 6%,
hypertension, low HDL cholesterol, el-
evated triglycerides, or family history of
diabetes in a rst-degree relative) and
who are obese and under 60 years of
age. (E)
Monitoring for the development of di-

abetes in those with pre-diabetes
should be performed every year. (E)
Randomized controlled trials have shown
that individuals at high risk for develop-
ing diabetes (those with IFG, IGT, or
both) can be given interventions that sig-
nicantly decrease the rate of onset of di-
abetes (1117). These interventions
include intensive lifestyle modication
programs that have been shown to be very
effective (58% reduction after 3 years)
and use of the pharmacologic agents met-
formin, -glucosidase inhibitors, orlistat,
and thiazolidinediones, each of which has
been shown to decrease incident diabetes
to various degrees. A summary of major
diabetes prevention trials is shown in Ta-
ble 7.
Two studies of lifestyle intervention
have shown persistent reduction in the
role of conversion to type 2 diabetes with
3 years (29) to 14 years (30) of postinter-
vention follow-up.
Based on the results of clinical trials
and the known risks of progression of
pre-diabetes to diabetes, an ADA Consen-
sus Development Panel (36) concluded
that people with IGT and/or IFG should
be counseled on lifestyle changes with
goals similar to those of the DPP (510%
weight loss and moderate physical activ-
ity of 30 min/day). Regarding the more
difcult issue of drug therapy for diabetes
prevention, the consensus panel felt that
metformin should be the only drug con-
sidered for use in diabetes prevention. For
other drugs, the issues of cost, side effects,
and lack of persistence of effect in some
studies led the panel to not recommend
use for diabetes prevention. Metformin
use was recommended only for very-
high-risk individuals (those with com-
bined IGT and IFG who are obese and
have at least one other risk factor for dia-
betes) who are under 60 years of age. In
addition, the panel highlighted the evi-
dence that in the DPP, metformin was
most effective compared with lifestyle in
individuals with BMI 35 kg/m
2
and
those under age 60 years.
V. DIABETES CARE
A. Initial evaluation
A complete medical evaluation should be
performed to classify the diabetes, detect
the presence of diabetes complications,
review previous treatment and glycemic
control in patients with established diabe-
tes, assist in formulating a management
plan, and provide a basis for continuing
care. Laboratory tests appropriate to the
evaluation of each patients medical con-
dition should be performed. A focus on
the components of comprehensive care
(Table 8) will assist the health care teamto
ensure optimal management of the pa-
tient with diabetes.
B. Management
People with diabetes should receive med-
ical care from a physician-coordinated
team. Such teams may include, but are
not limited to, physicians, nurse practitio-
ners, physicians assistants, nurses, dieti-
tians, pharmacists, and mental health
professionals with expertise and a special
interest in diabetes. It is essential in this
collaborative and integrated team ap-
proach that individuals with diabetes as-
sume an active role in their care.
The management plan should be for-
mulated as a collaborative therapeutic al-
liance among the patient and family, the
physician, and other members of the
health care team. A variety of strategies
and techniques should be used to provide
adequate education and development of
problem-solving skills in the various as-
pects of diabetes management. Imple-
mentation of the management plan
requires that each aspect is understood
and agreed to by the patient and the care
providers and that the goals and treat-
ment plan are reasonable. Any plan
should recognize diabetes self-manage-
ment education (DSME) and on-going di-
abetes support as an integral component
Table 6Screening for and diagnosis of GDM
Carry out diabetes risk assessment at the rst prenatal visit.
Women at very high risk should be screened for diabetes as soon as possible after the
conrmation of pregnancy. Criteria for very high risk are:
Severe obesity
Prior history of GDM or delivery of large-for-gestational-age infant
Presence of glycosuria
Diagnosis of PCOS
Strong family history of type 2 diabetes
Screening/diagnosis at this stage of pregnancy should use standard diagnostic testing (Table
2).
All women of greater than low risk of GDM, including those above not found to have diabetes
early in pregnancy, should undergo GDM testing at 2428 weeks of gestation. Low-
risk status, which does not require GDM screening, is dened as women with ALL of
the following characteristics:
Age 25 years
Weight normal before pregnancy
Member of an ethnic group with a low prevalence of diabetes
No known diabetes in rst-degree relatives
No history of abnormal glucose tolerance
No history of poor obstetrical outcome
Two approaches may be followed for GDM screening at 2428 weeks:
1. Two-step approach:
A. Perform initial screening by measuring plasma or serum glucose 1 h after a 50-g load
of 140 mg/dl identies 80% of women with GDM, while the sensitivity is further
increased to 90% by a threshold of 130 mg/dl.
B. Perform a diagnostic 100-g OGTT on a separate day in women who exceed the chosen
threshold on 50-g screening.
2. One-step approach (may be preferred in clinics with high prevalence of GDM): Perform
a diagnostic 100-g OGTT in all women to be tested at 2428 weeks.
The 100-g OGTT should be performed in the morning after an overnight fast of at least 8
h.
To make a diagnosis of GDM, at least two of the following plasma glucose values must be
found:
Fasting 95 mg/dl
1-h 180 mg/dl
2-h 155 mg/dl
3-h 140 mg/dl
of care. In developing the plan, consider-
ation should be given to the patients age,
school or work schedule and conditions,
physical activity, eating patterns, social
situation and cultural factors, and pres-
ence of complications of diabetes or other
medical conditions.
C. Glycemic control
1. Assessment of glycemic control
Two primary techniques are available for
health providers and patients to assess the
effectiveness of the management plan on
glycemic control: patient self-monitoring
of blood glucose (SMBG) or interstitial
glucose and A1C.
a. Glucose monitoring
Recommendations
SMBG should be carried out three or

more times daily for patients using mul-
tiple insulin injections or insulin pump
therapy. (A)
For patients using less frequent insulin

injections, noninsulin therapies, or
medical nutrition therapy (MNT)
alone, SMBGmay be useful as a guide to
the success of therapy. (E)
To achieve postprandial glucose tar-

gets, postprandial SMBGmay be appro-
priate. (E)
When prescribing SMBG, ensure that

patients receive initial instruction in,
and routine follow-up evaluation of,
SMBG technique and using data to ad-
just therapy. (E)
Continuous glucose monitoring (CGM)

in conjunction with intensive insulin
regimens can be a useful tool to lower
A1C in selected adults (age 25 years)
with type 1 diabetes (A).
Although the evidence for A1C lower-

ing is less strong in children, teens, and
younger adults, CGMmay be helpful in
these groups. Success correlates with
adherence to ongoing use of the device.
(C)
CGM may be a supplemental tool to

SMBG in those with hypoglycemia un-
awareness and/or frequent hypoglyce-
mic episodes. (E)
The ADA consensus and position state-
ments on SMBGprovide a comprehensive
review of the subject (37,38). Major clin-
ical trials of insulin-treated patients that
demonstrated the benets of intensive
glycemic control on diabetes complica-
tions have included SMBG as part of
multifactorial interventions, suggesting
that SMBG is a component of effective
therapy. SMBG allows patients to eval-
uate their individual response to ther-
apy and assess whether glycemic targets
are being achieved. Results of SMBGcan
be useful in preventing hypoglycemia
and adjusting medications (particularly
prandial insulin doses), MNT, and
physical activity.
Table 7Therapies proven effective in diabetes prevention trials
Study (ref.) n Population
Mean
age
(years)
Duration
(years)
Intervention
(daily dose)
Incidence in
control
subjects
(%/year)
Relative risk
reduction (%)
(95% CI)
3-Year
number
needed to
treat*
Lifestyle
Finnish DPS (12) 522 IGT, BMI 25 kg/m
2
55 3.2 I-D&E 6 58 (3070) 8.5
DPP (11) 2,161 IGT, BMI 24 kg/m
2
,
FPG 5.3 mmol/l
51 3 I-D&E 10.4 58 (4866) 6.9
Da Qing (13) 259 IGT (randomized
groups)
45 6 G-D&E 14.5 38 (1456) 7.9
Toranomon Study (31) 458 IGT (men), BMI 24
kg/m
2
55 4 I-D&E 2.4 67 (P 0.043) 20.6
Indian DPP (17) 269 IGT 46 2.5 I-D&E 23 29 (2137) 6.4
Medications
DPP (11) 2,155 IGT, BMI 24 kg/m
2
,
FPG 5.3 mmol/l
51 2.8 Metformin
(1,700
mg)
10.4 31 (1743) 13.9
Indian DPP (17) 269 IGT 46 2.5 Metformin
(500 mg)
23 26 (1935) 6.9
STOP NIDDM (15) 1,419 IGT, FPG 5.6
mmol/l
54 3.2 Acarbose
(300 mg)
12.4 25 (1037) 9.6
XENDOS (32) 3,277 BMI 30 kg/m
2
43 4 Orlistat (360
mg)
2.4 37 (1454) 45.5
DREAM (16) 5,269 IGT or IFG 55 3.0 Rosiglitazone
(8 mg)
9.1 60 (5465) 6.9
Voglibose Ph-3 (33) 1,780 IGT 56 3.0 (1-year Rx) Vogliobose
(0.2 mg)
12.0 40 (1857) 21 (1-year
Rx)
ACT-NOW (34) 602 IGT or IFG 52 2.6 Pioglitizone
(45 mg)
6.8 81 (6191) 6.3
Modied and reprinted with permission (35). Percentage points: *Number needed to treat to prevent 1 case of diabetes, standardized for a 3-year period to improve
comparisons across studies. Number of participants in the indicated comparisons, not necessarily in entire study. Calculated from information in the article.
ACT-NOW, ACTos Now Study for the Prevention of Diabetes; DPP, Diabetes Prevention Program; DPS, Diabetes Prevention Study; DREAM, Diabetes Reduction
Assessment with Ramipril and Rosiglitazone Medication; STOP NIDDM, Study to Prevent Non-Insulin Dependent Diabetes; XENDOS, Xenical in the prevention of
Diabetes in Obese Subjects. I, individual; G, group; D&E, diet and exercise.
Position Statement
The frequency and timing of SMBG
should be dictated by the particular needs
and goals of the patient. SMBG is espe-
cially important for patients treated with
insulin in order to monitor for and pre-
vent asymptomatic hypoglycemia and hy-
perglycemia. For most patients with type
1 diabetes and pregnant women taking
insulin, SMBG is recommended three or
more times daily. For these populations,
signicantly more frequent testing may be
required to reach A1C targets safely with-
out hypoglycemia. The optimal frequency
and timing of SMBGfor patients with type
2 diabetes on noninsulin therapy is un-
clear. A meta-analysis of SMBG in non
insulin-treated patients with type 2
diabetes concluded that some regimen of
SMBG was associated with a reduction in
A1Cof 0.4%. However, many of the stud-
ies in this analysis also included patient
education with diet and exercise counsel-
ing and, in some cases, pharmacologic in-
tervention, making it difcult to assess the
contribution of SMBG alone to improved
control (39). Several recent trials have
called into question the clinical utility
and cost-effectiveness of routine SMBGin
noninsulin-treated patients (4042).
Because the accuracy of SMBG is in-
strument and user dependent (43), it is
important to evaluate each patients mon-
itoring technique, both initially and at
regular intervals thereafter. In addition,
optimal use of SMBG requires proper in-
terpretation of the data. Patients should
be taught how to use the data to adjust
food intake, exercise, or pharmacological
therapy to achieve specic glycemic goals,
and these skills should be reevaluated
periodically.
CGMthrough the measurement of in-
terstitial glucose (which correlates well
with PG) is available. These sensors re-
quire calibration with SMBG, and the lat-
ter are still recommended for making
acute treatment decisions. CGM devices
also have alarms for hypo- and hypergly-
cemic excursions. Small studies in se-
lected patients with type 1 diabetes have
suggested that CGM use reduces the time
spent in hypo- and hyperglycemic ranges
and may modestly improve glycemic con-
trol. A larger 26-week randomized trial of
322 type 1 diabetic patients showed that
adults age 25 years and older using inten-
sive insulin therapy and CGM experi-
enced a 0.5% reduction in A1C (from
7.6 to 7.1%) compared with usual in-
tensive insulin therapy with SMBG (44).
Sensor use in children, teens, and adults
to age 24 years did not result in signicant
A1C lowering, and there was no signi-
cant difference in hypoglycemia in any
group. Importantly, the greatest predictor
of A1C lowering in this study for all age-
groups was frequency of sensor use,
which was lower in younger age-groups.
In a smaller randomized controlled trial of
129 adults and children with baseline
A1C 7.0%, outcomes combining A1C
and hypoglycemia favored the group us-
ing CGM, suggesting that CGM is also
benecial for individuals with type 1 dia-
betes who have already achieved excellent
control with A1C 7.0% (45). Although
CGMis an evolving technology, emerging
data suggest that it may offer benet in
appropriately selected patients who are
motivated to wear it most of the time.
CGM may be particularly useful in those
with hypoglycemia unawareness and/or
frequent episodes of hypoglycemia, and
studies in this area are ongoing.
b. A1C
Recommendations
Perform the A1C test at least two times

a year in patients who are meeting treat-
ment goals (and who have stable glyce-
mic control). (E)
Table 8Components of the comprehensive diabetes evaluation
Medical history
Age and characteristics of onset of diabetes (e.g., DKA, asymptomatic laboratory nding)
Eating patterns, physical activity habits, nutritional status, and weight history; growth
and development in children and adolescents
Diabetes education history
Review of previous treatment regimens and response to therapy (A1C records)
Current treatment of diabetes, including medications, meal plan, physical activity patterns,
and results of glucose monitoring and patients use of data
DKA frequency, severity, and cause
Hypoglycemic episodes
Hypoglycemia awareness
Any severe hypoglycemia: frequency and cause
History of diabetes-related complications
Microvascular: retinopathy, nephropathy, neuropathy (sensory, including history of
foot lesions; autonomic, including sexual dysfunction and gastroparesis)
Macrovascular: CHD, cerebrovascular disease, PAD
Other: psychosocial problems*, dental disease*
Physical examination
Height, weight, BMI
Blood pressure determination, including orthostatic measurements when indicated
Fundoscopic examination*
Thyroid palpation
Skin examination (for acanthosis nigricans and insulin injection sites)
Comprehensive foot examination:
Inspection
Palpation of dorsalis pedis and posterior tibial pulses
Presence/absence of patellar and Achilles reexes
Determination of proprioception, vibration, and monolament sensation
Laboratory evaluation
A1C, if results not available within past 23 months
If not performed/available within past year:
Fasting lipid prole, including total, LDL- and HDL cholesterol and triglycerides
Liver function tests
Test for urine albumin excretion with spot urine albumin/creatinine ratio
Serum creatinine and calculated GFR
TSH in type 1 diabetes, dyslipidemia, or women over age 50 years
Referrals
Annual dilated eye exam
Family planning for women of reproductive age
Registered dietitian for MNT
DSME
Dental examination
Mental health professional, if needed
* See appropriate referrals for these categories.
Perform the A1C test quarterly in pa-

tients whose therapy has changed or
who are not meeting glycemic goals. (E)
Use of point-of-care testing for A1C al-

lows for timely decisions on therapy
changes, when needed. (E)
Because A1C is thought to reect average
glycemia over several months (43) and
has strong predictive value for diabetes
complications (11,46), A1C testing
should be performed routinely in all pa-
tients with diabetes, at initial assessment
and then as part of continuing care. Mea-
surement approximately every 3 months
determines whether a patients glycemic
targets have been reached and main-
tained. For any individual patient, the fre-
quency of A1C testi ng shoul d be
dependent on the clinical situation, the
treatment regimen used, and the judg-
ment of the clinician. Some patients with
stable glycemia well within target may do
well with testing only twice per year,
while unstable or highly intensively man-
aged patients (e.g., pregnant type 1 dia-
betic women) may be tested more
frequently than every 3 months. The
availability of the A1C result at the time
that the patient is seen (point-of-care test-
ing) has been reported to result in in-
creased intensication of therapy and
i mprovement i n gl ycemi c control
(47,48).
The A1C test is subject to certain lim-
itations. Conditions that affect erythro-
cyte turnover (hemolysis, blood loss) and
hemoglobin variants must be considered,
particularly when the A1Cresult does not
correlate with the patients clinical situa-
tion (43). In addition, A1C does not pro-
vide a measure of glycemic variability or
hypoglycemia. For patients prone to gly-
cemic variability (especially type 1 dia-
betic patients, or type 2 diabetic patients
with severe insulin deciency), glycemic
control is best judged by the combination
of results of SMBG testing and the A1C.
The A1C may also serve as a check on the
accuracy of the patients meter (or the pa-
tients reported SMBGresults) and the ad-
equacy of the SMBG testing schedule.
Table 9 contains the correlation be-
tween A1C levels and mean PG levels
based on data fromthe international A1C-
Derived Average Glucose (ADAG) trial
using frequent SMBG and CGM in 507
adults (83% Caucasian) with type 1, type
2, and no diabetes (49). ADA and the
American Association of Clinical Chem-
ists have determined that the correlation
(r 0.92) is strong enough to justify re-
porting both an A1C result and an esti-
mated average glucose (eAG) result when
a clinician orders the A1C test. In previ-
ous versions of the Standards of Medical
Care in Diabetes, the table describing the
correlation between A1C and mean glu-
cose was derived from relatively sparse
data (one seven-point prole over 1 day
per A1C reading) in the primarily Cauca-
sian type 1 participants in the DCCT (50).
Clinicians should note that the numbers
in the table are now different, as they are
based on 2,800 readings per A1C in the
ADAG trial.
In the ADAG trial, there were no sig-
nicant differences among racial and eth-
nic groups in the regression lines between
A1C and mean glucose, although there
was a trend toward a difference between
Africans/African Americans participants
and Caucasians that might have been sig-
nicant had more Africans/African Amer-
icans been studied. A recent study
comparing A1C to CGMdata in 48 type 1
diabetic children found a highly statisti-
cally signicant correlation between A1C
and mean blood glucose, although the
correlation (r 0.7) was signicantly
lower than in the ADAG trial (51).
Whether there are signicant differences
in how A1C relates to average glucose in
children or in African American patients
is an area for further study. For the time
being, the question has not led to different
recommendations about testing A1C or
different interpretations of the clinical
meaning of given levels of A1C in those
populations.
For patients in whom A1C/eAG and
measured blood glucose appear discrep-
ant, clinicians should consider the possi-
bilities of hemoglobinopathy or altered
red cell turnover and the options of more
frequent and/or different timing of SMBG
or use of CGM. Other measures of chronic
glycemia such as fructosamine are avail-
able, but their linkage to average glucose
and their prognostic signicance are not
as clear as is the case for A1C.
2. Glycemic goals in adults
Lowering A1C to below or around 7%

has been shown to reduce microvascu-
lar and neuropathic complications of
type 1 and type 2 diabetes. Therefore,
for microvascular disease prevention,
the A1C goal for nonpregnant adults in
general is 7%. (A)
In type 1 and type 2 diabetes, random-

ized controlled trials of intensive versus
standard glycemic control have not
shown a signicant reduction in CVD
outcomes during the randomized por-
tion of the trials. Long-term follow-up
of the DCCT and UK Prospective Dia-
betes Study (UKPDS) cohorts suggests
that treatment to A1C targets below or
around 7% in the years soon after the
diagnosis of diabetes is associated with
long-term reduction in risk of macro-
vascular disease. Until more evidence
becomes available, the general goal of
7% appears reasonable for many
adults for macrovascular risk reduc-
tion. (B)
Subgroup analyses of clinical trials such

as the DCCT and UKPDS, and evidence
for reduced proteinuria in the Action in
Diabetes and Vascular Disease: Preterax
and Diamicron Modied Release Con-
trolled Evaluation (ADVANCE) trial
suggest a small but incremental benet
in microvascular outcomes with A1C
values closer to normal. Therefore, for
selected individual patients, providers
might reasonably suggest even lower
A1C goals than the general goal of
7%, if this can be achieved without
signicant hypoglycemia or other ad-
verse effects of treatment. Such patients
might include those with short dura-
tion of diabetes, long life expectancy,
and no signicant CVD. (B)
Conversely, less-stringent A1C goals

than the general goal of 7% may be
appropriate for patients with a history
of severe hypoglycemia, limited life ex-
pectancy, advanced microvascular or
macrovascular complications, and ex-
tensive comorbid conditions and those
with longstanding diabetes in whom
the general goal is difcult to attain de-
Table 9Correlation of A1C with average
glucose
A1C (%)
Mean plasma glucose
mg/dl mmol/l
6 126 7.0
7 154 8.6
8 183 10.2
9 212 11.8
10 240 13.4
11 269 14.9
12 298 16.5
These estimates are based on ADAG data of 2,700
glucose measurements over 3 months per A1C mea-
surement in 507 adults with type 1, type 2, and no
diabetes. The correlation between A1C and average
glucose was 0.92 (49). A calculator for converting
A1C results into estimated average glucose (eAG),
in either mg/dl or mmol/l, is available at
http://professional.diabetes.org/eAG.
Position Statement
spite diabetes self-management educa-
tion, appropriate glucose monitoring,
and effective doses of multiple glucose-
lowering agents including insulin. (C)
Glycemic control is fundamental to the
management of diabetes. The DCCT, a
prospective, randomized, controlled trial
of intensive versus standard glycemic
control in patients with relatively recently
diagnosed type 1 diabetes, showed den-
itively that improved glycemic control is
associated with signicantly decreased
rates of microvascular (retinopathy and
nephropathy) as well as neuropathic
complications (53). Follow-up of the
DCCT cohorts in the Epidemiology of Di-
abetes Interventions and Complications
(EDIC) study has shown persistence of
this effect in previously intensively
treated subjects, even though their glyce-
mic control has been equivalent to that of
previous standard arm subjects during
follow-up (54,55).
In type 2 diabetes, the Kumamoto
study (56) and the UKPDS (57,58) dem-
onstrated signicant reductions in micro-
vascular and neuropathic complications
with intensive therapy. Similar to the
DCCT-EDIC ndings, long-term fol-
low-up of the UKPDS cohort has recently
demonstrated a legacy effect of early in-
tensive glycemic control on long-term
rates of microvascular complications,
even with loss of glycemic separation be-
tween the intensive and standard cohorts
after the end of the randomized con-
trolled trial (59). The more recent Veter-
ans Affairs Diabetes Trial (VADT) in type
2 diabetes also showed signicant reduc-
tions in albuminuria with intensive
(achieved median A1C 6.9%) compared
with standard glycemic control but no
difference in retinopathy and neuropathy
(60,61).
In each of these large randomized
prospective clinical trials, treatment regi-
mens that reduced average A1C to 7%
(1% above the upper limits of normal)
were associated with fewer markers of
long-term microvascular complications;
however, intensive control was found to
increase the risk of severe hypoglycemia
and led to weight gain (46,60,62).
Epidemiological analyses of the
DCCT and UKPDS (46,53) demonstrate a
curvilinear relationship between A1Cand
microvascular complications. Such anal-
yses suggest that, on a population level,
the greatest number of complications will
be averted by taking patients from very
poor control to fair or good control. These
analyses also suggest that further lowering
of A1C from 7 to 6% is associated with
further reduction in the risk of microvas-
cular complications, albeit the absolute
risk reductions become much smaller.
The ADVANCE study of intensive versus
standard glycemic control in type 2 dia-
betes found a statistically signicant re-
duction in albuminuria with an A1C
target of 6.5% (achieved median A1C
6.3%) compared with standard therapy
achieving a median A1C of 7.0% (63).
Given the substantially increased risk of
hypoglycemia (particularly in those with
type 1 diabetes, but also in the recent type
2 diabetes trials described below), the
concerning mortality ndings in the Ac-
tion to Control Cardiovascular Risk in Di-
abetes (ACCORD) trial described below
and the relatively much greater effort re-
quired to achieve near-normoglycemia,
the risks of lower targets may outweigh
the potential benets on microvascular
complications on a population level.
However, selected individual patients, es-
pecially those with little comorbidity and
long life expectancy (who may reap the
benets of further lowering glycemia be-
low 7%) may, at patient and provider
judgment, adopt glycemic targets as close
to normal as possible as long as signicant
hypoglycemia does not become a barrier.
Whereas many epidemiologic studies
and meta-analyses (64,65) have clearly
shown a direct relationship between A1C
and CVD, the potential of intensive glyce-
mic control to reduce CVD has been less
clearly dened. In the DCCT, there was a
trend toward lower risk of CVD events
with intensive control (risk reduction
41%, 95% CI 1068%), but the number
of events was small. However, 9-year
post-DCCT follow-up of the cohort has
shown that participants previously ran-
domized to the intensive arm had a 42%
reduction (P 0.02) in CVD outcomes
and a 57% reduction (P 0.02) in the
risk of nonfatal myocardial infarction
(MI), stroke, or CVD death compared
with participants previously in the stan-
dard arm (66). The benet of intensive
glycemic control in this type 1 diabetic
cohort has recently been shown to persist
for up to 30 years (67).
The UKPDS trial of type 2 diabetes
observed a 16%reduction in cardiovascu-
lar complications (combined fatal or non-
fatal MI and sudden death) in the
intensive glycemic control arm, although
this difference was not statistically signif-
icant (P 0.052), and there was no sug-
gestion of benet on other CVDoutcomes
such as stroke. In an epidemiologic anal-
ysis of the study cohort, a continuous as-
sociation was observed such that for every
percentage point lower median on-study
A1C (e.g., 87%), there was a statistically
signicant 18% reduction in CVD events,
again with no glycemic threshold. A re-
cent report of 10 years of follow-up of the
UKPDS cohort described, for the partici-
pants originally randomized to intensive
glycemic control compared with those
randomized to conventional glycemic
control, long-termreductions in MI (15%
with sulfonylurea or insulin as initial
pharmacotherapy, 33% with metformin
as initial pharmacotherapy, both statisti-
cally signicant) and in all-cause mortal-
ity (13 and 27%, respectively, both
statistically signicant) (59).
Because of ongoing uncertainty re-
garding whether intensive glycemic con-
trol can reduce the increased risk of CVD
events in people with type 2 diabetes, sev-
eral large long-term trials were launched
in the past decade to compare the effects
of intensive versus standard glycemic
control on CVD outcomes in relatively
high-risk participants with established
type 2 diabetes. In 2008, results of three
large trials (ACCORD, ADVANCE, and
VADT) suggested no signicant reduction
in CVDoutcomes with intensive glycemic
control in these populations. Details of
these three studies are shown in Table 10,
and their results and implications are re-
viewed more extensively in a recent ADA
position statement (52).
The ACCORD study randomized
10,251 participants with either history of
a CVD event or signicant CVD risk to a
strategy of intensive glycemic control (tar-
get A1C 6.0%) or standard glycemic
control (A1Ctarget 7.07.9%). Investiga-
tors used multiple glycemic medications
in both arms. From a baseline median
A1C of 8.1%, the intensive arm reached a
median A1Cof 6.4%within 12 months of
randomization, while the standard group
reached a median A1C of 7.5%. Other
risk factors were treated aggressively and
equally in both groups. The intensive gly-
cemic control group had more use of in-
sulin in combination with multiple oral
agents, signicantly more weight gain,
and more episodes of severe hypoglyce-
mia than the standard group.
In early 2008, the glycemic control
arm of ACCORD was halted on the rec-
ommendation of the studys data safety
monitoring board due to the nding of an
increased rate of mortality in the intensive
arm compared with the standard arm
(1.41 vs. 1.14%/year, hazard ratio 1.22,
95% CI 1.011.46), with a similar in-
crease in cardiovascular deaths. The pri-
mary outcome of ACCORD (MI, stroke,
or cardiovascular death) was lower in the
intensive glycemic control group due to a
reduction in nonfatal MI, although this
nding was not statistically signicant
when the study was terminated (68). Of
note, prespecied subset analyses showed
that participants with no previous CVD
event and those who had a baseline A1C
8% had a statistically signicant reduc-
tion in the primary CVD outcome, al-
though overall mortality was not reduced
in these groups.
The cause of excess deaths in the in-
tensive group of the ACCORD has been
difcult to pinpoint (and is discussed in
some detail in a 2009 ADA position state-
ment [52]). However, exploratory analy-
ses of the mortality ndings of ACCORD
(evaluating variables including weight
gain, use of any specic drug or drug
combination, and hypoglycemia) were re-
portedly unable to identify a clear expla-
nation for the excess mortality in the
intensive arm. At the 69th Scientic Ses-
sions of the American Diabetes Associa-
t i on, t he ACCORD i nvest i gat or s
presented additional analyses showing no
increase in mortality in participants who
achieved A1Clevels 7%or in those who
lowered their A1C quickly after trial en-
rollment. In fact, the converse was ob-
served: those at highest risk for mortality
were participants in the intensive arm
with the highest A1C levels.
The ADVANCE study randomized
participants to a strategy of intensive gly-
cemic control (with primary therapy be-
ing the sulfonylurea gliclizide and
additional medications as needed to
achieve a target A1Cof 6.5%) or to stan-
dard therapy (in which any medication
but gliclizide could be used and the gly-
cemic target was according to local
guidelines). ADVANCE participants
Table 10Comparison of the three trials of intensive glycemic control and CVD outcomes
ACCORD ADVANCE VADT
Participant characteristics
n 10,251 11,140 1,791
Mean age (years) 62 66 60
Duration of diabetes (years) 10 8 11.5
History of CVD (%) 35 32 40
Median baseline A1C (%) 8.1 7.2 9.4
On insulin at baseline (%) 35 1.5 52
Protocol characteristics
A1C goals (%) (I vs. S)* 6.0 vs. 7.07.9 6.5 vs. based on local guidelines 6.0 (action if 6.5) vs.
planned separation of 1.5
Protocol for glycemic control
(I vs. S)* Multiple drugs in both
arms
Multiple drugs added to gliclizide vs.
multiple drugs with no gliclizide
Multiple drugs in both arms
Management of other risk
factors Embedded blood pressure
and lipid trials
Embedded blood pressure trial Protocol for intensive
treatment in both arms
On-study characteristics
Achieved median A1C (%)
(I vs. S) 6.4 vs. 7.5 6.3 vs. 7.0 6.9 vs. 8.5
On insulin at study end (%)
(I vs. S)* 77 vs. 55* 40 vs. 24 89 vs. 0.74
Weight changes (kg)
Intensive glycemic control arm 3.5 0.1 7.8
Standard glycemic control arm 0.4 1.0 3.4
Severe hypoglycemia
(participants with one or more
episodes during study) (%)
Intensive glycemic control arm 16.2 2.7 21.2
Standard glycemic control arm 5.1 1.5 9.9
Outcomes
Denition of primary outcome Nonfatal MI, nonfatal
stroke, CVD death
Microvascular plus macrovascular
(nonfatal MI, nonfatal stroke, CVD
death) outcomes
Nonfatal MI, nonfatal stroke,
CVD death,
hospitalization for heart
failure, revascularization
HR for primary outcome
(95% CI) 0.90 (0.781.04) 0.9 (0.820.98);
macrovascular 0.94 (0.841.06)
0.88 (0.741.05)
HR for mortality ndings
(95% CI) 1.22 (1.011.46) 0.93 (0.831.06) 1.07 (0.811.42)
*Insulin rates for ACCORD are for any use during the study. I, intensive glycemic control; S, standard glycemic control. Abridged from ref. 52.
Position Statement
were slightly older than those in AC-
CORD and VADT and had similar high
CVD risk. However, they had an average
duration of diabetes that was 2 years
shorter, lower baseline A1C (median
7.2%), and almost no use of insulin at
enrollment. The median A1C levels
achieved in the intensive and standard
arms were 6.3 and 7.0%, respectively,
and maximal separation between the
arms took several years to achieve. Use of
other drugs that favorably impact CVD
risk (aspirin, statins, and angiotensin en-
zyme inhibitors) was lower in ADVANCE
than in ACCORD or VADT.
The primary outcome of ADVANCE
was a combination of microvascular
events (nephropathy and retinopathy)
and major adverse cardiovascular events
(MI, stroke, and cardiovascular death).
Intensive glycemic control signicantly
reduced the primary end point, although
this was due to a signicant reduction in
the microvascular outcome, primarily de-
velopment of macroalbuminuria, with no
signicant reduction in the macrovascu-
lar outcome. There was no difference in
overall or cardiovascular mortality be-
tween the intensive compared with the
standard glycemic control arms (63).
VADT randomized participants with
type 2 diabetes uncontrolled on insulin or
maximal dose oral agents (median entry
A1C 9.4%) to a strategy of intensive gly-
cemic control (goal A1C 6.0%) or stan-
dard glycemic control, with a planned
A1C separation of at least 1.5%. Medica-
tion treatment algorithms were used to
achieve the specied glycemic goals, with
a goal of using similar medications in both
groups. Median A1C levels of 6.9 and
8.4% were achieved in the intensive and
standard arms, respectively, within the
1st year of the study. Other CVD risk fac-
tors were treated aggressively and equally
in both groups.
The primary outcome of VADT was a
composite of CVDevents. The cumulative
primary outcome was nonsignicantly
lower in the intensive arm. There were
more CVD deaths in the intensive arm
than in the standard arm, but the differ-
ence was not statistically signicant (60).
Post hoc subgroup analyses suggested
that duration of diabetes interacted with
randomization such that participants
with duration of diabetes less than about
12 years appeared to have a CVD benet
of intensive glycemic control while those
with longer duration of disease prior to
study entry had a neutral or even adverse
effect of intensive glycemic control. Other
exploratory analyses suggested that se-
vere hypoglycemia within the past 90
days was a strong predictor of the primary
outcome and of CVD mortality (69).
All three of these trials were carried
out in participants with established diabe-
tes (mean duration 811 years) and either
known CVD or multiple risk factors sug-
gesting the presence of established ath-
erosclerosis. Subset analyses of the three
trials suggested a signicant benet of in-
tensive glycemic control on CVD in par-
ticipants with shorter duration of
diabetes, lower A1C at entry, and/or ab-
sence of known CVD. The DCCT-EDIC
study and the long-term follow-up of the
UKPDS cohort both suggest that intensive
glycemic control initiated soon after diag-
nosis of diabetes in patients with a lower
level of CVD risk may impart long-term
protection from CVD events. As is the
case with microvascular complications, it
may be that glycemic control plays a
greater role before macrovascular disease
is well developed and minimal or no role
when it is advanced. Consistent with this
concept, data from an ancillary study of
VADT demonstrated that intensive glyce-
mic control was quite effective in reduc-
ing CVD events in individuals with less
atherosclerosis at baseline (assessed by
coronary calcium) but not in people with
more extensive baseline atherosclerosis
(70).
The benets of intensive glycemic
control on microvascular and neuro-
pathic complications are well established
for both type 1 and type 2 diabetes. AD-
VANCE and VADT have added to that ev-
i dence base by demonst r at i ng a
signicant reduction in the risk of new or
worsening albuminuria with intensive
glycemic control. The lack of signicant
reduction in CVD events with intensive
glycemic control in ACCORD, AD-
VANCE, and VADT should not lead clini-
cians to abandon the general target of an
A1C 7.0% and thereby discount the
benet of good control on serious and de-
bilitating microvascular complications.
The evidence for a cardiovascular
benet of intensive glycemic control pri-
marily rests on long-term follow-up of
study cohorts treated early in the course
of type 1 and type 2 diabetes as well as
subset analyses of ACCORD, ADVANCE,
and VADT. A recent group-level meta-
analysis of the three trials suggests that
glucose lowering has a modest (9%) but
statistically signicant reduction in major
CVD outcomes, primarily nonfatal MI,
with no signicant increase in mortality.
A prespecied subgroup analysis sug-
gested that major CVD outcome reduc-
tion occurred in patients without known
CVD at baseline (HR 0.84 [95% CI 0.74
0.94]) (71). Conversely, the mortality
ndings in ACCORD and subgroup anal-
yses of VADT suggest that the potential
risks of very intensive glycemic control
may outweigh its benets in some pa-
tients, such as those with very long dura-
tion of diabetes, known history of severe
hypoglycemia, advanced atherosclerosis,
and advanced age/frailty. Certainly, pro-
viders should be vigilant in preventing se-
vere hypoglycemia in patients with
advanced disease and should not aggres-
sively attempt to achieve near-normal
A1C levels in patients in whom such a
target cannot be reasonably easily and
safely achieved.
Recommended glycemic goals for
nonpregnant adults are shown in Table
11. The recommendations are based on
those for A1C values, with listed blood
glucose levels that appear to correlate
with achievement of an A1Cof 7%. The
issue of pre- versus postprandial SMBG
targets is complex (72). Elevated post-
challenge (2-h OGTT) glucose values
have been associated with increased car-
diovascular risk independent of FPG in
some epidemiological studies. In diabetic
subjects, some surrogate measures of vas-
cular pathology, such as endothelial dys-
function, are negatively affected by
postprandial hyperglycemia (73). It is
clear that postprandial hyperglycemia,
like preprandial hyperglycemia, contrib-
utes to elevated A1C levels, with its rela-
tive contribution being higher at A1C
levels that are closer to 7%. However, out-
come studies have clearly shown A1C to
be the primary predictor of complica-
tions, and landmark glycemic control tri-
als such as the DCCT and UKPDS relied
overwhelmingly on preprandial SMBG.
Additionally, a randomized controlled
trial in patients with known CVD found
no CVD benet of insulin regimens tar-
geting postprandial glucose compared
with those targeting preprandial glucose
(74). For individuals who have premeal
glucose values within target but A1C val-
ues above target, a reasonable recommen-
dation for postprandial testing and targets
is monitoring postprandial plasma glu-
cose (PPG) 12 h after the start of the meal
and treatment aimed at reducing PPGval-
ues to 180 mg/dl to help lower A1C.
As noted above, less stringent treat-
ment goals may be appropriate for adults
with limited life expectancies or advanced
vascular disease. Glycemic goals for chil-
dren are provided in VII.A.1.a. Glycemic
control. Severe or frequent hypoglycemia
is an absolute indication for the modica-
tion of treatment regimens, including set-
ting higher glycemic goals.
Regarding goals for glycemic control
for women with GDM, recommendations
from the Fifth International Workshop-
Conference on Gestational Diabetes (75)
are to target maternal capillary glucose
concentrations of:
Preprandial 95 mg/dl (5.3 mmol/l)

and either
1-h postmeal 140 mg/dl (7.8

mmol/l)
or
2-h postmeal 120 mg/dl (6.7

mmol/l)
For women with preexisting type 1 or
type 2 diabetes who become pregnant, a
recent consensus statement (76) recom-
mends the following as optimal glycemic
goals, if they can be achieved without ex-
cessive hypoglycemia:
premeal, bedtime, and overnight glu-

cose 6099 mg/dl (3.35.4 mmol/l)
peak postprandial glucose 100129

mg/dl (5.47.1 mmol/l)
A1C 6.0%
3. Approach to treatment
a. Therapy for type 1 diabetes. The
DCCT clearly showed that intensive insu-
lin therapy (three or more injections per
day of insulin or continuous subcutane-
ous insulin infusion [CSII] or insulin
pump therapy) was a key part of im-
proved glycemia and better outcomes
(53,66). At the time of the study, therapy
was carried out with short- and interme-
diate-acting human insulins. Despite bet-
ter microvascular outcomes, intensive
insulin therapy was associated with a high
rate in severe hypoglycemia (62 episodes
per 100 patient-years of therapy). Since
the time of the DCCT, a number of rapid-
acting and long-acting insulin analogs
have been developed. These analogs are
associated with less hypoglycemia with
equal A1C lowering in type 1 diabetes
(77,78).
Recommended therapy for type 1 di-
abetes therefore consists of the following
components: 1) use of multiple dose in-
sulin injections (34 injections per day of
basal and prandial insulin) or CSII ther-
apy; 2) matching of prandial insulin to
carbohydrate intake, premeal blood glu-
cose, and anticipated activity; and 3) for
many patients (especially if hypoglycemia
is a problem), use of insulin analogs.
There are excellent reviews available that
guide the initiation and management of
insulin therapy to achieve desired glyce-
mic goals (3,77,79).
Because of the increased frequency of
other autoimmune diseases in type 1 dia-
betes, screening for thyroid dysfunction,
vitamin B12 deciency, or celiac disease
should be considered based on signs and
symptoms. Periodic screening in the ab-
sence of symptoms has been recom-
mended, but the effectiveness and
optimal frequency are unclear.
b. Therapy for type 2 diabetes. The ADA
and the European Association for the
Study of Diabetes (EASD) published a
consensus statement on the approach to
management of hyperglycemia in individ-
uals with type 2 diabetes (80) and a sub-
sequent update (81). Highlights of this
approach include: intervention at the
time of diagnosis with metformin in com-
bination with lifestyle changes (MNT and
exercise) and continuing timely augmen-
tation of therapy with additional agents
(including early initiation of insulin ther-
apy) as a means of achieving and main-
taining recommended levels of glycemic
control (i.e., A1C7%for most patients).
The overall objective is to achieve and
maintain glycemic control and to change
interventions when therapeutic goals are
not being met.
The algorithm took into account the
evidence for A1C lowering of the individ-
ual interventions, their additive effects,
and their expense. The precise drugs used
and their exact sequence may not be as
important as achieving and maintaining
glycemic targets safely. Medications not
included in the consensus algorithm, ow-
ing to less glucose-lowering effectiveness,
limited clinical data, and/or relative ex-
pense, still may be appropriate choices for
individual patients to achieve glycemic
goals. Initiation of insulin at the time of
diagnosis is recommended for individuals
presenting with weight loss or other se-
vere hyperglycemic symptoms or signs.
D. Medical nutrition therapy
General recommendations
Individuals who have pre-diabetes or

diabetes should receive individualized
MNT as needed to achieve treatment
goals, preferably provided by a regis-
tered dietitian familiar with the compo-
nents of diabetes MNT. (A)
Because it can result in cost savings and

improved outcomes (B), MNT should
be covered by insurance and other pay-
ors (E).
Energy balance, overweight, and
obesity
In overweight and obese insulin-

resistant individuals, modest weight
loss has been shown to reduce insulin
resistance. Thus, weight loss is recom-
mended for all overweight or obese in-
dividuals who have or are at risk for
diabetes. (A)
For weight loss, either low-carbohy-

drate or low-fat calorie-restricted diets
Table 11 Summary of glycemic recommendations for non-pregnant adults with diabetes
A1C 7.0%*
Preprandial capillary plasma glucose 70130 mg/dl (3.97.2 mmol/l)
Peak postprandial capillary plasma glucose 180 mg/dl (10.0 mmol/l)
Key concepts in setting glycemic goals:
A1C is the primary target for glycemic control
Goals should be individualized based on:
duration of diabetes
age/life expectancy
comorbid conditions
known CVD or advanced microvascular
complications
hypoglycemia unawareness
individual patient considerations
More or less stringent glycemic goals may be
appropriate for individual patients
Postprandial glucose may be targeted if A1C goals are not
met despite reaching preprandial glucose goals
*Referenced to a nondiabetic range of 4.06.0% using a DCCT-based assay. Postprandial glucose mea-
surements should be made 12 h after the beginning of the meal, generally peak levels in patients with
diabetes.
Position Statement
may be effective in the short-term (up
to 1 year). (A)
For patients on low-carbohydrate diets,

monitor lipid proles, renal function,
and protein intake (in those with ne-
phropathy) and adjust hypoglycemic
therapy as needed. (E)
Physical activity and behavior modi-

cation are important components of
weight loss programs and are most
helpful in maintenance of weight loss.
(B)
Primary prevention of diabetes
Among individuals at high risk for de-

veloping type 2 diabetes, structured
programs emphasi zi ng l i f est yl e
changes that include moderate weight
loss (7% body weight) and regular
physical activity (150 min/week) with
dietary strategies including reduced
calories and reduced intake of dietary
fat can reduce the risk for developing
diabetes and are therefore recom-
mended. (A)
Individuals at high risk for type 2 dia-

betes should be encouraged to achieve
the U.S. Department of Agriculture
(USDA) recommendation for dietary -
ber (14 g ber/1,000 kcal) and foods
containing whole grains (one-half of
grain intake). (B)
Dietary fat intake in diabetes
management
Saturated fat intake should be 7% of

total calories. (A)
Reducing intake of trans fat lowers LDL

cholesterol and increases HDL choles-
terol (A); therefore intake of trans fat
should be minimized (E).
Carbohydrate intake in diabetes
management
Monitoring carbohydrate intake,

whether by carbohydrate counting, ex-
changes, or experience-based estima-
tion, remains a key strategy in achieving
glycemic control. (A)
For individuals with diabetes, use of the

glycemic index and glycemic load may
provide a modest additional benet for
glycemic control over that observed
when total carbohydrate is considered
alone. (B)
Other nutrition recommendations
Sugar alcohols and nonnutritive sweet-

eners are safe when consumed within
the acceptable daily intake levels estab-
lished by the Food and Drug Adminis-
tration (FDA). (A)
If adults with diabetes choose to use

alcohol, daily intake should be limited
to a moderate amount (one drink per
day or less for adult women and two
drinks per day or less for adult men).
(E)
Routine supplementation with antioxi-

dants, such as vitamins E and C and
carotene, is not advised because of lack
of evidence of efcacy and concern re-
lated to long-term safety. (A)
Benet from chromium supplementa-

tion in people with diabetes or obesity
has not been conclusively demon-
strated and therefore cannot be recom-
mended. (C)
Individualized meal planning should

include optimization of food choices to
meet recommended dietary allowances
(RDAs)/dietary reference intakes
(DRIs) for all micronutrients. (E)
MNT is an integral component of diabetes
prevention, management, and self-
management education. In addition to its
role in preventing and controlling diabe-
tes, ADA recognizes the importance of
nutrition as an essential component of an
overall healthy lifestyle. A full review of
the evidence regarding nutrition in pre-
venting and controlling diabetes and its
complications and additional nutrition-
related recommendations can be found in
the ADA position statement, Nutrition
Recommendations and Interventions for
Diabetes, published in 2006 and updated
for 2008 (82). Achieving nutrition-
related goals requires a coordinated team
effort that includes the active involvement
of the person with pre-diabetes or diabe-
tes. Because of the complexity of nutrition
issues, it is recommended that a registered
dietitian who is knowledgeable and
skilled in implementing nutrition therapy
into diabetes management and education
be the team member who provides MNT.
Clinical trials/outcome studies of
MNT have reported decreases in A1C at
36 months ranging from 0.25 to 2.9%
with higher reductions seen in type 2 di-
abetes of shorter duration. Multiple stud-
i es have demonst rat ed sust ai ned
improvements in A1C at 12 months and
longer when a registered dietitian pro-
vided follow-up visits ranging from
monthly to three sessions per year (83
90). Meta-analyses of studies in nondia-
betic, free-living subjects report that MNT
reduces LDL cholesterol by 1525 mg/dl
(91) or by up to 16% (92), while clinical
trials support a role for lifestyle modica-
tion in treating hypertension (92,93).
Because of the effects of obesity on
insulin resistance, weight loss is an im-
portant therapeutic objective for over-
weight or obese individuals with pre-
diabetes or diabetes (94). Short-term
studies have demonstrated that moderate
weight loss (5% of body weight) in sub-
jects with type 2 diabetes is associated
with decreased insulin resistance, im-
proved measures of glycemia and lipemia,
and reduced blood pressure (95); longer-
term studies (52 weeks) showed mixed
effects on A1C in adults with type 2 dia-
betes (9699), and results were con-
founded by pharmacologic weight loss
therapy. A systematic reviewof 80 weight
loss studies of 1 year duration demon-
strated that moderate weight loss
achieved through diet alone, diet and ex-
ercise, and meal replacements can be
achieved and maintained over the long
term (4.88% weight loss at 12 months
[100]). The multifactorial intensive life-
style intervention used in the DPP, which
included reduced intake of fat and calo-
ries, led to weight loss averaging 7% at 6
months and maintenance of 5% weight
loss at 3 years, associated with a 58% re-
duction in incidence of type 2 diabetes
(11). Look AHEAD (Action for Health in
Diabetes) is a large clinical trial designed
to determine whether long-term weight
loss will improve glycemia and prevent
cardiovascular events in subjects with
type 2 diabetes. One-year results of the
intensive lifestyle intervention in this trial
show an average of 8.6% weight loss, sig-
nicant reduction of A1C, and reduction
in several CVD risk factors (101). When
completed, the Look AHEAD study
should provide insight into the effects of
long-term weight loss on important clin-
ical outcomes.
The optimal macronutrient distribu-
tion of weight loss diets has not been es-
tablished. Although low-fat diets have
traditionally been promoted for weight
loss, several randomized controlled trials
found that subjects on low-carbohydrate
diets (130 g/day of carbohydrate) lost
more weight at 6 months than subjects on
low-fat diets (102,103); however, at 1
year, the difference in weight loss be-
tween the low-carbohydrate and low-fat
diets was not signicant and weight loss
was modest with both diets. Another
study of overweight women randomized
to one of four diets showed signicantly
more weight loss at 12 months with the
Atkins low-carbohydrate diet than with
hi gher-carbohydrat e di et s (104).
Changes in serum triglyceride and HDL
cholesterol were more favorable with the
low-carbohydrate diets. In one study,
those subjects with type 2 diabetes dem-
onstrated a greater decrease in A1Cwith a
low-carbohydrate diet than with a low-fat
diet (103). Arecent meta-analysis showed
that at 6 months, low-carbohydrate diets
were associated with greater improve-
ments in triglyceride and HDL cholesterol
concentrations than low-fat diets; how-
ever, LDL cholesterol was signicantly
higher with the low-carbohydrate diets
(105). In a 2-year dietary intervention
study, Mediterranean and low-carbohy-
drate diets were found to be effective and
safe alternatives to a low-fat diet for
weight reduction in moderately obese
participants (99).
The RDA for digestible carbohydrate
is 130 g/day and is based on providing
adequate glucose as the required fuel for
the central nervous system without reli-
ance on glucose production fromingested
protein or fat. Although brain fuel needs
can be met on lower-carbohydrate diets,
long-term metabolic effects of very-low-
carbohydrate diets are unclear, and such
diets eliminate many foods that are im-
portant sources of energy, ber, vitamins,
and minerals that are important in dietary
palatability (106).
Although numerous studies have at-
tempted to identify the optimal mix of
macronutrients for meal plans of people
with diabetes, it is unlikely that one such
combination of macronutrients exists.
The best mix of carbohydrate, protein,
and fat appears to vary depending on
individual circumstances. For those
individuals seeking guidance as to macro-
nutrient distribution in healthy adults,
DRIs may be helpful (106). It must be
clearly recognized that regardless of the
macronutrient mix, the total caloric in-
take must be appropriate to the weight
management goal. Further, individualiza-
tion of the macronutrient composition
will depend on the metabolic status of the
patient (e.g., lipid prole and renal func-
tion) and/or food preferences. Plant-
based diets (vegan or vegetarian) that are
well planned and nutritionally adequate
have also been shown to improve meta-
bolic control (107,108).
The primary goal with respect to di-
etary fat in individuals with diabetes is to
limit saturated fatty acids, trans fatty ac-
ids, and cholesterol intake so as to reduce
risk for CVD. Saturated and trans fatty ac-
ids are the principal dietary determinants
of plasma LDL cholesterol. There is a lack
of evidence on the effects of specic fatty
acids on people with diabetes; therefore,
the recommended goals are consistent
with those for individuals with CVD
(92,109).
The FDA has approved ve nonnutri-
tive sweeteners for use in the U.S.: acesul-
fame potassium, aspartame, neotame,
saccharin, and sucralose. Before being al-
lowed on the market, all underwent rig-
orous scrutiny and were shown to be safe
when consumed by the public, including
people with diabetes and women during
pregnancy. Reduced calorie sweeteners
approved by the FDA include sugar alco-
hols (polyols) such as erythritol, isomalt,
lactitol, maltitol, mannitol, sorbitol, xyli-
tol, tagatose, and hydrogenated starch hy-
drolysates. The use of sugar alcohols
appears to be safe; however, they may
cause diarrhea, especially in children. Ste-
via (Rebaudioside A) has been designated
by the FDA as being generally recognized
as safe (GRAS).
Reimbursement for MNT
MNT, when delivered by a registered dieti-
tian according to nutrition practice guide-
lines, is reimbursed as part of the Medicare
program as overseen by the Centers for
Medicare and Medicaid Services (www.
cms.hhs.gov/ medicalnutritiontherapy).
E. Bariatric surgery
Recommendations
Bariatric surgery should be considered

for adults with BMI 35 kg/m
2
and
type 2 diabetes, especially if the diabe-
tes or associated comorbidities are dif-
cult to control with lifestyle and
pharmacologic therapy. (B)
Patients with type 2 diabetes who have

undergone bariatric surgery need life-
long lifestyle support and medical moni-
toring. (E)
Although small trials have shown glyce-

mic benet of bariatric surgery inpatients
with type 2 diabetes and BMI of 3035
kg/m
2
, there is currently insufcient evi-
dence togenerally recommendsurgery in
patients withBMI 35kg/m
2
outside of a
research protocol. (E)
The long-term benets, cost-effectiveness,

and risks of bariatric surgery in individ-
uals with type 2 diabetes should be
studied in well-designed, randomized
controlled trials with optimal medical
and lifestyle therapy as the comparator.
(E)
Gastric reduction surgery, either gastric
banding or procedures that involve by-
passing or transposing sections of the
small intestine, when part of a compre-
hensive team approach, can be an effec-
tive weight loss treatment for severe
obesity, and national guidelines support
its consideration for people with type 2
diabetes who have BMI 35 kg/m
2
. Bari-
atric surgery has been shown to lead to
near or complete normalization of glyce-
mia in 5595% of patients with type 2
diabetes, depending on the surgical pro-
cedure. A meta-analysis of studies of bari-
atric surgery reported that 78% of
individuals with type 2 diabetes had com-
plete resolution of diabetes (normaliza-
tion of blood glucose levels in the absence
of medications) and that the resolution
rates were sustained in studies that had
follow-up exceeding 2 years (110). Reso-
lution rates are lower with procedures
that only constrict the stomach and
higher with those that bypass portions of
the small intestine. Additionally, there is a
suggestion that intestinal bypass proce-
dures may have glycemic effects that are
independent of their effects on weight.
A recent randomized controlled trial
compared adjustable gastric banding to
the best available medical and lifestyle
therapy in subjects with type 2 diabetes
diagnosed 2 years before randomiza-
tion and with BMI 3040 kg/m
2
(111). In
this trial, 73% of surgically treated pa-
tients achieved remission of their diabe-
tes, compared with 13% of those treated
medically. The latter group lost only 1.7%
of body weight, suggesting that their ther-
apy was not optimal. Overall the trial had
60 subjects, and only 13 had a BMI 35
kg/m
2
, making it difcult to generalize
these results to diabetic patients who are
less severely obese or with longer dura-
tion of diabetes.
Bariatric surgery is costly in the short
termand has some risks. Rates of morbidity
and mortality directly related to the surgery
have been reduced considerably in recent
years, with 30-day mortality rates now
0.28%, similar to those of laparoscopic cho-
lecystectomy (112). Longer-term concerns
include vitamin and mineral deciencies,
osteoporosis, and rare but often severe hy-
poglycemia from insulin hypersecretion.
Cohort studies attempting to match sub-
jects suggest that the procedure may reduce
longer-term mortality rates (113), and it is
reasonable to postulate that there may be
recouping of costs over the long term. How-
ever, studies of the mechanisms of glycemic
improvement, long-termbenets and risks,
and cost-effectiveness of bariatric surgery in
individuals withtype 2 diabetes will require
Position Statement
well-designed, randomized clinical trials
with optimal medical and lifestyle therapy
of diabetes andcardiovascular riskfactors as
the comparators.
F. Diabetes self-management
education
Recommendations
People with diabetes should receive

DSME according to national standards
when their diabetes is diagnosed and as
needed thereafter. (B)
Effective self-management and quality

of life are the key outcomes of DSME
and should be measured and moni-
tored as part of care. (C)
DSME should address psychosocial is-

sues, since emotional well-being is as-
soci at ed wi t h posi t i ve di abet es
outcomes. (C)
Because DSME can result in cost-

savings and improved outcomes (B),
DSME should be reimbursed by third-
party payors. (E)
DSME is an essential element of dia-
betes care (114120), and national stan-
dards for DSME (121) are based on
evidence for its benets. Education helps
people with diabetes initiate effective self-
management and cope with diabetes
when they are rst diagnosed. Ongoing
DSME and support also help people with
di abet es mai nt ai n ef f ect i ve sel f -
management throughout a lifetime of di-
abetes as they face new challenges and as
treatment advances become available.
DSME helps patients optimize metabolic
control, prevent and manage complica-
tions, and maximize quality of life in a
cost-effective manner (122).
DSME is the on-going process of fa-
cilitating the knowledge, skill, and ability
necessary for diabetes self-care (121).
This process incorporates the needs,
goals, and life experiences of the person
with diabetes. The overall objectives of
DSME are to support informed decision-
making, self-care behaviors, problem-
solving, and active collaboration with the
health care team and to improve clinical
outcomes, health status, and quality of life
in a cost-effective manner (121).
Current best practice of DSME is a
skills-based approach that focuses on
helping those with diabetes make in-
formed self-management choices. DSME
has changed from a didactic approach fo-
cusing on providing information, to a
more theoretically based empowerment
model that focuses on helping those with
diabetes make informed self-management
decisions. Care of diabetes has shifted to
an approach that is more patient centered
and places the person with diabetes at the
center of the care model working in col-
laboration with health care professionals.
Patient-centered care is respectful of and
responsive to individual patient prefer-
ences, needs, and values and ensures that
patient values guide all decision making
(123).
1. Evidence for the benets of DSME
Multiple studies have found that DSME is
associated with improved diabetes
knowledge and self-care behavior (115);
improved clinical outcomes such as lower
A1C (116,117,119,120,124), lower self-
reported weight (115), improved quality
of life (118,125), and healthy coping
(126); and lower costs (127). Better out-
comes were reported for DSME interven-
tions that were longer and included
follow-up support (115,128131), that
were culturally (132) and age appropriate
(133,134) and tailored to individual
needs and preferences (114), and that ad-
dressed psychosocial issues (114,115,
119,135). Both individual and group ap-
proaches have been found effective (136
138). There is growing evidence for the
role of community health workers and
peer (139) and lay leaders (140) in deliv-
ering DSME and support in addition to
the core team (141).
Diabetes education is associated with
increased use of primary and preventive
services and lower use of acute, inpatient
hospital services (127). Patients who par-
ticipate in diabetes education are more
likely to follow best practice treatment
recommendations, particularly among
the medicare population, and to have
lower Medicare and commercial claim
costs (142).
2. National Standards for DSME
The National Standards for DSME are de-
signed to dene quality diabetes self-
management education and to assist
diabetes educators in a variety of settings
to provide evidence-based education
(121). The standards, most recently re-
vised in 2007, are reviewed and updated
every 5 years by a task force representing
key organizations involved in the eld of
diabetes education and care.
3. Reimbursement for DSME
DSME, when provided by a program that
meets ADA recognition standards, is re-
imbursed as part of the Medicare program
overseen by the Centers for Medicare and
Medicaid Services (www.cms.hhs.gov/
DiabetesSelfManagement).
G. Physical activity
Recommendations
People with diabetes should be advised

to perform at least 150 min/week of
moderate-intensity aerobic physical ac-
tivity (5070% of maximum heart
rate). (A)
In the absence of contraindications,

people with type 2 diabetes should be
encouraged to performresistance train-
ing three times per week. (A)
ADA technical reviews on exercise in pa-
tients with diabetes, currently being up-
dated, have summarized the value of
exercise in the diabetes management plan
(143,144). Regular exercise has been
shown to improve blood glucose control,
reduce cardiovascular risk factors, con-
tribute to weight loss, and improve well
being. Furthermore, regular exercise may
prevent type 2 diabetes in high-risk indi-
viduals (1113). Structured exercise in-
terventions of at least 8 weeks duration
have been shown to lower A1C by an av-
erage of 0.66% in people with type 2 di-
abetes, even with no signicant change in
BMI (145). Higher levels of exercise in-
tensity are associated with greater im-
provements in A1C and tness (146).
1. Frequency and type of exercise
The U.S. Department of Health and Hu-
man Services Physical Activity Guide-
lines for Americans (147) suggest that
adults over age 18 years perform150 min/
week of moderate-intensity or 75 min/
week of vigorous aerobic physical activity
or an equivalent combination of the two.
In addition, the guidelines suggest that
adults also do muscle-strengthening ac-
tivities that involve all major muscle
groups two or more days per week. The
guidelines suggest that adults over age 65
years, or those with disabilities, followthe
adult guidelines if possible or (if this is not
possible) be as physically active as they
are able. Studies included in the meta-
analysis of effects of exercise interventions
on glycemic control (145) had a mean
number of sessions per week of 3.4, with
a mean of 49 min/session. The DPP life-
style intervention, which included 150
min/week of moderate intensity exercise,
had a benecial effect on glycemia in
those with pre-diabetes. Therefore, it
seems reasonable to recommend that peo-
ple with diabetes try to followthe physical
activity guidelines for the general
population.
Progressive resistance exercise im-
proves insulin sensitivity in older men
with type 2 diabetes to the same or even to
a greater extent as aerobic exercise (148).
Clinical trials have provided strong evi-
dence for the A1C-lowering value of re-
sistance training in older adults with type
2 diabetes (149,150) and for an additive
benet of combined aerobic and resis-
tance exercise in adults with type 2 diabe-
tes (151).
2. Evaluation of the diabetic patient
before recommending an exercise
program
Prior guidelines have suggested that be-
fore recommending a programof physical
activity, the provider should assess pa-
tients with multiple cardiovascular risk
factors for coronary artery disease (CAD).
As further discussed in VI.A.5. Coronary
heart disease screening and treatment, the
area of screening asymptomatic diabetic
patients for CAD remains unclear, and a
recent ADA consensus statement on this
issue concluded that routine screening is
not recommended (152). Providers
should use clinical judgment in this area.
Certainly, high-risk patients should be
encouraged to start with short periods of
low-intensity exercise and to increase the
intensity and duration slowly.
Providers should assess patients for
conditions that might contraindicate cer-
tain types of exercise or predispose to in-
jury, such as uncontrolled hypertension,
severe autonomic neuropathy, severe pe-
ripheral neuropathy or history of foot le-
si ons, and unst abl e prol i f erat i ve
retinopathy. The patients age and previ-
ous physical activity level should be
considered.
3. Exercise in the presence of
nonoptimal glycemic control
a. Hyperglycemia. When people with
type 1 diabetes are deprived of insulin for
1248 h and are ketotic, exercise can
worsen hyperglycemia and ketosis (153);
therefore, vigorous activity should be
avoided in the presence of ketosis. How-
ever, it is not necessary to postpone exer-
cise simply based on hyperglycemia,
provided the patient feels well and urine
and/or blood ketones are negative.
b. Hypoglycemia. In individuals taking
insulin and/or insulin secretagogues,
physical activity can cause hypoglycemia
if medication dose or carbohydrate con-
sumption is not altered. For individuals
on these therapies, added carbohydrate
should be ingested if pre-exercise glucose
levels are 100 mg/dl (5.6 mmol/l)
(154,155). Hypoglycemia is rare in dia-
betic individuals who are not treated with
insulin or insulin secretagogues, and no
preventive measures for hypoglycemia
are usually advised in these cases.
4. Exercise in the presence of specic
long-term complications of diabetes
a. Retinopathy. In the presence of pro-
liferative diabetic retinopathy (PDR) or
severe non-proliferative diabetic retinop-
athy (NPDR), vigorous aerobic or resis-
tance exercise may be contraindicated
because of the risk of triggering vitreous
hemorrhage or retinal detachment (156).
b. Peripheral neuropathy. Decreased
pain sensation in the extremities results in
increased risk of skin breakdown and in-
fection and of Charcot joint destruction.
Prior recommendations have advised
nonweight-bearing exercise for patients
with severe peripheral neuropathy. Stud-
ies have shown that moderate-intensity
walking may not lead to increased risk of
foot ulcers or reulceration in those with
peripheral neuropathy (157). All individ-
uals with peripheral neuropathy should
wear proper footwear and examine their
feet daily for early detection of lesions.
Anyone with a foot injury or open sore
should be restricted to nonweight-
bearing activities.
c. Autonomic neuropathy. Autonomic
neuropathy can increase the risk of exer-
cise-induced injury or adverse events
through decreased cardiac responsive-
ness to exercise, postural hypotension,
impaired thermoregulation, impaired
night vision due to impaired papillary re-
action, and unpredictable carbohydrate
delivery from gastroparesis predisposing
to hypoglycemia (158). Autonomic neu-
ropathy is also strongly associated with
CVD in people with diabetes (159,160).
People with diabetic autonomic neuropa-
thy should undergo cardiac investigation
before beginning physical activity more
intense than that to which they are
accustomed.
d. Albuminuria and nephropathy. Phys-
ical activity can acutely increase urinary
protein excretion. However, there is no
evidence that vigorous exercise increases
the rate of progression of diabetic kidney
disease and likely no need for any specic
exercise restrictions for people with dia-
betic kidney disease (161).
H. Psychosocial assessment and care
Recommendations
Assessment of psychological and social

situation should be included as an on-
going part of the medical management
of diabetes. (E)
Psychosocial screening and follow-up

should include, but is not limited to,
attitudes about the illness, expectations
for medical management and out-
comes, affect/mood, general and diabe-
tes-related quality of life, resources
(nancial, social, and emotional), and
psychiatric history. (E)
Screen for psychosocial problems such

as depression and diabetes-related dis-
tress, anxiety, eating disorders, and
cognitive impairment when self-
management is poor. (C)
Psychological and social problems can
impair the ability of the individual (162
164) or the family to carry out diabetes
care tasks and therefore compromise
health status. There are opportunities for
the clinician to assess psychosocial status
in a timely and efcient manner so that
referral for appropriate services can be
accomplished.
Key opportunities for screening of
psychosocial status occur at diagnosis,
during regularly scheduled management
visits, during hospitalizations, at discov-
ery of complications, or when problems
with glucose control, quality of life, or ad-
herence are identied. Patients are likely
to exhibit psychological vulnerability at
diagnosis and when their medical status
changes, i.e., the end of the honeymoon
period, when the need for intensied
treatment is evident, and when complica-
tions are discovered (164).
I ssues known t o i mpact sel f -
management and health outcomes in-
clude but are not limited to: attitudes
about the illness, expectations for medical
management and outcomes, affect/mood,
general and diabetes-related quality of
life, diabetes-related distress (165), re-
sources (nancial, social, and emotional)
(166), and psychiatric history (167,168).
Screening tools are available for a number
of these areas (135). Indications for refer-
ral to a mental health specialist familiar
with diabetes management may include
gross noncompliance with medical regi-
men (by self or others) (168), depression
wi t h t he possi bi l i t y of sel f -harm
(169,170), debilitating anxiety (alone or
with depression), indications of an eating
disorder, or cognitive functioning that
Position Statement
signicantly impairs judgment. It is pref-
erable to incorporate psychological as-
sessment and treatment into routine care
rather than waiting for identication of a
specic problem or deterioration in psy-
chological status (135). Although the cli-
nician may not feel qualied to treat
psychological problems, using the pa-
tient-provider relationship as a founda-
tion for further treatment can increase the
likelihood that the patient will accept re-
ferral for other services. It is important to
establish that emotional well-being is part
of diabetes management.
I. When treatment goals are not met
For a variety of reasons, some people with
diabetes and their health care providers
do not achieve the desired goals of treat-
ment (Table 11). Rethinking the treat-
ment regimen may require assessment of
barriers including income, health literacy,
diabetes distress, depression, and com-
peting demands, including those related
to family responsibilities and dynamics.
Other strategies may include culturally
appropriate and enhanced DSME, co-
management with a diabetes team, refer-
ral to a medical social worker for
assistance with insurance coverage, or
change in pharmacological therapy. Initi-
ation of or increase in SMBG, utilization
of CGM, frequent contact with the pa-
tient, or referral to a mental health profes-
sional or physician with special expertise
in diabetes may be useful. Providing pa-
tients with an algorithm for self-titration
of insulin doses based on SMBG results
may be helpful for type 2 patients who
take insulin (171).
J. Intercurrent illness
The stress of illness, trauma, and/or sur-
gery frequently aggravates glycemic con-
trol and may preci pi tate di abeti c
ketoacidosis (DKA) or nonketotic hyper-
osmolar state, life-threatening conditions
that require immediate medical care to
prevent complications and death (172).
Any condition leading to deterioration in
glycemic control necessitates more fre-
quent monitoring of blood glucose and
(in ketosis-prone patients) urine or blood
ketones. Marked hyperglycemia requires
temporary adjustment of the treatment
program and, if accompanied by ketosis,
vomiting, or alteration in level of con-
sciousness, immediate interaction with
the diabetes care team. The patient treated
with noninsulin therapies or MNT alone
may temporarily require insulin. Ade-
quate uid and caloric intake must be as-
sured. Infection or dehydration are more
likely to necessitate hospitalization of the
person with diabetes than the person
without diabetes.
The hospitalized patient should be
treated by a physician with expertise in
the management of diabetes. For further
information on management of patients
with hyperglycemia in the hospital, see
VIII.A. Diabetes care in the hospital. For
further information on management of
DKA or nonketotic hyperosmolar state,
refer to the ADA consensus statement on
hyperglycemic crises (173).
K. Hypoglycemia
Recommendations
Glucose (1520 g) is the preferred

treatment for the conscious individual
with hypoglycemia, although any form
of carbohydrate that contains glucose
may be used. If SMBG 15 min after
treatment shows continued hypoglyce-
mia, the treatment should be repeated.
Once SMBG glucose returns to normal,
the individual should consume a meal
or snack to prevent recurrence of hypo-
glycemia. (E)
Glucagon should be prescribed for all

individuals at signicant risk of severe
hypoglycemia, and caregivers or family
members of these individuals should be
instructed in its administration. Gluca-
gon administration is not limited to
health care professionals. (E)
Individuals with hypoglycemia un-

awareness or one or more episodes of
severe hypoglycemia should be advised
to raise their glycemic targets to strictly
avoid further hypoglycemia for at least
several weeks to partially reverse hypo-
glycemia unawareness and reduce risk
of future episodes. (B)
Hypoglycemia is the leading limiting fac-
tor in the glycemic management of type 1
and insulin-treated type 2 diabetes (174).
Treatment of hypoglycemia (PG70 mg/
dl) requires ingestion of glucose- or car-
bohydrate-containing foods. The acute
glycemic response correlates better with
the glucose content than with the carbo-
hydrate content of the food. Although
pure glucose is the preferred treatment,
any form of carbohydrate that contains
glucose will raise blood glucose. Added
fat may retard and then prolong the acute
glycemic response (175). Ongoing activ-
ity of insulin or insulin secretagogues may
lead to recurrence of hypoglycemia unless
further food is ingested after recovery.
Severe hypoglycemia (where the indi-
vidual requires the assistance of another
person and cannot be treated with oral
carbohydrate due to confusion or uncon-
sciousness) should be treated using emer-
gency glucagon kits, which require a
prescription. Those in close contact with
or who have custodial care of people with
hypoglycemia-prone diabetes (family
members, roommates, school personnel,
child care providers, correctional institu-
tion staff, or coworkers) should be in-
structed in use of such kits. An individual
does not need to be a health care profes-
sional to safely administer glucagon. Care
should be taken to ensure that unexpired
glucagon kits are available.
Prevention of hypoglycemia is a crit-
ical component of diabetes management.
Teaching people with diabetes to balance
insulin use, carbohydrate intake, and ex-
ercise is a necessary but not always suf-
cient strategy. In type 1 diabetes and
severely insulin-decient type 2 diabetes,
the syndrome of hypoglycemia unaware-
ness, or hypoglycemia-associated auto-
nomic failure, can severely compromise
stringent diabetes control and quality of
life. The decient counter-regulatory hor-
mone release and autonomic responses in
this syndrome are both risk factors for
and are caused by hypoglycemia. A corol-
lary to this vicious cycle is that several
weeks of avoidance of hypoglycemia has
been demonstrated to improve counter-
regulation and awareness to some extent
in many patients (174,176,177). Hence,
patients with one or more episodes of se-
vere hypoglycemia may benet from at
least short-term relaxation of glycemic
targets.
L. Immunization
Recommendations
Annually provide an inuenza vaccine

to all diabetic patients 6 months of
age. (C)
Administer pneumococcal polysaccha-

ride vaccine to all diabetic patients 2
years of age. Aone-time revaccination is
recommended for individuals 64
years of age previously immunized
when they were 65 years of age if the
vaccine was administered 5 years
ago. Other indications for repeat vacci-
nation include nephrotic syndrome,
chronic renal disease, and other immu-
nocompromised states, such as after
transplantation. (C)
Inuenza and pneumonia are common,
preventable infectious diseases associated
with high mortality and morbidity in the
elderly and in people with chronic dis-
eases. Though there are limited studies
reporting the morbidity and mortality of
inuenza and pneumococcal pneumonia
specically in people with diabetes, ob-
servational studies of patients with a vari-
ety of chronic illnesses, including
diabetes, show that these conditions are
associated with an increase in hospitaliza-
tions for inuenza and its complications.
People with diabetes may be at increased
risk of the bacteremic form of pneumo-
coccal infection and have been reported
to have a high risk of nosocomial bactere-
mia, which has a mortality rate as high as
50% (178).
Safe and effective vaccines are avail-
able that can greatly reduce the risk of
serious complications from these diseases
(179,180). In a case-control series, inu-
enza vaccine was shown to reduce diabe-
tes-related hospital admission by as much
as 79%during u epidemics (179). There
is sufcient evidence to support that peo-
ple with diabetes have appropriate sero-
logic and clinical responses to these
vaccinations. The Centers for Disease
Control and Preventions Advisory Com-
mittee on Immunization Practices recom-
mends inuenza and pneumococcal
vaccines for all individuals with diabetes
(http://www.cdc.gov/vaccines/recs/). For
a complete discussion on the prevention
of inuenza and pneumococcal disease in
people with diabetes, consult the techni-
cal review and position statement on this
subject (178,181).
VI. PREVENTION AND
MANAGEMENT OF
DIABETES COMPLICATIONS
A. Cardiovascular disease
CVD is the major cause of morbidity and
mortality for individuals with diabetes and
the largest contributor to the direct and in-
direct costs of diabetes. The common con-
ditions coexisting with type 2 diabetes (e.g.,
hypertension and dyslipidemia) are clear
riskfactors for CVD, anddiabetes itself con-
fers independent risk. Numerous studies
have shown the efcacy of controlling indi-
vidual cardiovascular risk factors in pre-
venting or slowing CVD in people with
diabetes. Large benets are seen when mul-
tiple risk factors are addressed globally
(182,183). Risk for coronary heart disease
and CVD in general can be estimated using
multivariable risk factor approaches, and
such a strategy may be desirable to under-
take in adult patients prior to instituting
preventive therapy.
1. Hypertension/blood pressure
control
Recommendations
Screening and diagnosis
Blood pressure should be measured at

every routine diabetes visit. Patients
found to have systolic blood pressure
130 mmHg or diastolic blood pres-
sure 80 mmHg should have blood
pressure conrmed on a separate day.
Repeat systolic blood pressure 130
mmHg or diastolic blood pressure 80
mmHg conrms a diagnosis of hyper-
tension. (C)
Goals
Patients with diabetes should be treated

to a systolic blood pressure 130
mmHg. (C)
Patients with diabetes should be treated

to a diastolic blood pressure 80
mmHg. (B)
Treatment
Patients with a systolic blood pressure

130139 mmHg or a diastolic blood
pressure 8089 mmHg may be given
lifestyle therapy alone for a maximum
of 3 months, and then if targets are not
achieved, patients should be treated
with the addition of pharmacological
agents. (E)
Patients with more severe hypertension

(systolic blood pressure 140 mmHg
or diastolic blood pressure 90
mmHg) at diagnosis or follow-up
should receive pharmacologic therapy
in addition to lifestyle therapy. (A)
Lifestyle therapy for hypertension con-

sists of weight loss if overweight,
DASH-style dietary pattern including
reducing sodium and increasing potas-
sium intake, moderation of alcohol in-
take, and increased physical activity.
(B)
Pharmacologic therapy for patients

with diabetes and hypertension should
be paired with a regimen that includes
either an ACE inhibitor or an angioten-
sin II receptor blocker (ARB). If one
class is not tolerated, the other should
be substituted. If needed to achieve
blood pressure targets, a thiazide di-
uretic should be added to those with an
estimated glomerular ltration rate
(GFR) (see below) 30 ml min/1.73
m
2
and a loop diuretic for those with an
estimated GFR 30 ml min/1.73 m
2
.
(C)
Multiple drug therapy (two or more

agents at maximal doses) is generally
required to achieve blood pressure tar-
gets. (B)
If ACE inhibitors, ARBs, or diuretics are

used, kidney function and serumpotas-
sium levels should be closely moni-
tored. (E)
In pregnant patients with diabetes and

chronic hypertension, blood pressure
target goals of 110129/6579 mmHg
are suggested in the interest of long-
term maternal health and minimizing
impaired fetal growth. ACE inhibitors
and ARBs are contraindicated during
pregnancy. (E)
Hypertension is a common comorbidity
of diabetes that affects the majority of pa-
tients, with prevalence depending on type
of diabetes, age, obesity, and ethnicity.
Hypertension is a major risk factor for
both CVD and microvascular complica-
tions. In type 1 diabetes, hypertension is
often the result of underlying nephropa-
thy, while in type 2 diabetes it usually
coexists with other cardiometabolic risk
factors.
a. Screening and diagnosis. Measure-
ment of blood pressure in the ofce
should be done by a trained individual
and should follow the guidelines estab-
lished for nondiabetic individuals: mea-
surement in the seated position, with feet
on the oor and arm supported at heart
level, after 5 min of rest. Cuff size should
be appropriate for the upper arm circum-
ference. Elevated values should be con-
rmed on a separate day. Because of the
clear synergistic risks of hypertension and
diabetes, the diagnostic cutoff for a diag-
nosis of hypertension is lower in people
with diabetes (blood pressure 130/80
mmHg) than in those without diabetes
(blood pressure 140/90 mmHg) (184).
Home blood pressure self-monitoring
and 24-h ambulatory blood pressure
monitoring may provide additional evi-
dence of white coat and masked hyper-
tension and other discrepancies between
ofce and true blood pressure, and
studies in nondiabetic populations show
that home measurements may correlate
better with CVDrisk than ofce measure-
ments (185,186). However, the prepon-
derance of the clear evidence of benets of
treatment of hypertension in people with
diabetes is based on ofce measurements.
Position Statement
b. Treatment goals. Randomized clinical
trials have demonstrated the benet (re-
duction of coronary heart disease [CHD]
events, stroke, and nephropathy) of low-
ering blood pressure to 140 mmHg sys-
tolic and 80 mmHg diastolic in
individuals with diabetes (184,187189).
Epidemiologic analyses show that blood
pressure 115/75 mmHg is associated
with increased cardiovascular event rates
and mortality in individuals with diabetes
(184,190,191). Therefore, a target blood
pressure goal of 130/80 mmHg is rea-
sonable if it can be achieved safely. The
ongoing ACCORD trial is designed to de-
termine whether blood pressure lowering
to systolic blood pressure 120 mmHg
provides greater cardiovascular protec-
tion than a systolic blood pressure level of
140 mmHg in patients with type 2 dia-
betes (192).
c. Treatment strategies. Although there
are no well-controlled studies of diet and
exercise in the treatment of hypertension
in individuals with diabetes, the Dietary
Approaches to Stop Hypertensi on
(DASH) study in nondiabetic individuals
has shown antihypertensive effects simi-
lar to those of pharmacologic mono-
therapy. Lifestyle therapy consists of
reducing sodium intake (to 1,500 mg/
day) and excess body weight; increasing
consumption of fruits, vegetables (810
servings/day), and low-fat dairy products
(23 servings/day); avoiding excessive al-
cohol consumption (no more than two
servings per day in men and no more than
one serving per day in women); and in-
creasing activity levels (184,193). These
nonpharmacological strategies may also
positively affect glycemia and lipid con-
trol. Their effects on cardiovascular
events have not been established. An ini-
tial trial of nonpharmacologic therapy
may be reasonable in diabetic individu-
als with mild hypertension (systolic
130 139 mmHg or diastolic 80 89
mmHg). If the blood pressure is 140
mmHg systolic and/or 90 mmHg dia-
stolic at the time of diagnosis, pharma-
cologic therapy should be initiated
along with nonpharmacologic therapy
(184).
Lowering of blood pressure with reg-
imens based on a variety of antihyperten-
sive drugs, including ACE inhibitors,
ARBs, -blockers, diuretics, and calcium
channel blockers, has been shown to be
effective in reducing cardiovascular
events. Several studies suggested that
ACE inhibitors may be superior to dihy-
dropyridine calcium channel blockers in
reducing cardiovascular events (194
196). However, a variety of other studies
have shown no specic advantage to ACE
inhibitors as initial treatment of hyperten-
sion in the general hypertensive popula-
ti on, but rather an advantage on
cardiovascular outcomes of initial therapy
wi t h l ow-dose t hi azi de di uret i cs
(184,197,198).
In people with diabetes, inhibitors of
the renin-angiotensin system (RAS) may
have unique advantages for initial or early
therapy of hypertension. In a nonhyper-
tension trial of high-risk individuals in-
cluding a large subset with diabetes, an
ACE inhibitor reduced CVD outcomes
(199). In patients with congestive heart
failure (CHF), including diabetic sub-
groups, ARBs have been shown to reduce
major CVD outcomes (200203), and in
type 2 patients with signicant nephrop-
athy, ARBs were superior to calcium
channel blockers for reducing heart fail-
ure (204206). Though evidence for dis-
tinct advantages of RAS inhibitors on
CVD outcomes in diabetes remains con-
icting (187,207), the high CVD risks as-
sociated with diabetes, and the high
prevalence of undiagnosed CVD, may still
favor recommendations for their use as
rst-line hypertension therapy in people
with diabetes (184). Recently, the blood
pressure arm of the ADVANCE trial dem-
onstrated that routine administration of a
xed combination of the ACE inhibitor
perindopril and the diuretic indapamide
signicantly reduced combined micro-
vascular and macrovascular outcomes, as
well as CVD and total mortality. The im-
proved outcomes also could have been
due to lower achieved blood pressure in
the perindopril-indapamide arm (208).
In addition, the ACCOMPLISH(Avoiding
Cardiovascular Events in Combination
Therapy in Patients Living with Systolic
Hypertension) trial showed a decrease in
morbidity and mortality in those receiv-
ing benazapril and amlodipine versus
benazapril and hydrochlorothiazide. The
compelling benets of RAS inhibitors in
diabetic patients with albuminuria or re-
nal insufciency provide additional ratio-
nale for use of these agents (see below,
VI. B. Nephropathy screeni ng and
treatment).
An important caveat is that most pa-
tients with hypertension require multi-
drug therapy to reach treatment goals,
especially diabetic patients whose targets
are lower. Many patients will require
three or more drugs to reach target goals
(184). If blood pressure is refractory to
optimal doses of at least three antihyper-
tensive agents of different classications,
one of which should be a diuretic, clini-
cians should consider an evaluation for
secondary forms of hypertension.
During pregnancy in diabetic women
with chronic hypertension, target blood
pressure goals of 110129 mmHg sys-
tolic and 6579 mmHg diastolic are rea-
sonable, as they contribute to long-term
maternal health. Lower blood pressure
levels may be associated with impaired
fetal growth. During pregnancy, treat-
ment with ACE inhibitors and ARBs is
contraindicated, since they can cause fetal
damage. Antihypertensive drugs known
to be effective and safe in pregnancy in-
clude methyldopa, labetalol, diltiazem,
clonidine, and prazosin. Chronic diuretic
use during pregnancy has been associated
with restricted maternal plasma volume,
which might reduce uteroplacental perfu-
sion (209).
2. Dyslipidemia/lipid management
Recommendations
Screening
In most adult patients, measure fasting

lipid prole at least annually. In adults
with low-risk lipid values (LDL choles-
terol 100 mg/dl, HDL cholesterol
50 mg/dl, and triglycerides 150
mg/dl), lipid assessments may be re-
peated every 2 years. (E)
Treatment recommendations and goals
Lifestyle modication focusing on the

reduction of saturated fat, trans fat,
and cholesterol intake; increase of n-3
fatty acids, viscous ber, and plant
stanols/sterols; weight loss (if indi-
cated); and increased physical activity
should be recommended to improve
the lipid prole in patients with dia-
betes. (A)
Statin therapy should be added to life-

style therapy, regardless of baseline
lipid levels, for diabetic patients:
with overt CVD. (A)
without CVD who are over the age of

40 years and have one or more other
CVD risk factors. (A)
For patients at lower risk than de-

scribed above (e.g., without overt CVD
and under the age of 40 years), statin
therapy should be considered in addi-
tion to lifestyle therapy if LDL choles-
terol remains 100 mg/dl or in those
with multiple CVD risk factors. (E)
In individuals without overt CVD, the

primary goal is an LDL cholesterol
100 mg/dl (2.6 mmol/l). (A)
In individuals with overt CVD, a lower

LDL cholesterol goal of 70 mg/dl (1.8
mmol/l), using a high dose of a statin, is
an option. (B)
If drug-treated patients do not reach the

above targets on maximal tolerated sta-
tin therapy, a reduction in LDL choles-
terol of 3040% from baseline is an
alternative therapeutic goal. (A)
Triglycerides levels 150 mg/dl (1.7

mmol/l) and HDL cholesterol 40
mg/dl (1.0 mmol/l) in men and 50
mg/dl (1.3 mmol/l) in women, are de-
sirable. However, LDL cholesterol
targeted statin therapy remains the
preferred strategy. (C)
If targets are not reached on maximally

tolerated doses of statins, combination
therapy using statins and other lipid-
lowering agents may be considered to
achieve lipid targets but has not been
evaluated in outcome studies for either
CVD outcomes or safety. (E)
Statin therapy is contraindicated in

pregnancy. (E)
a. Evidence for benets of lipid-lowering
therapy. Patients with type 2 diabetes
have an increased prevalence of lipid ab-
normalities, contributing to their high
risk of CVD. Over the past decade or
more, multiple clinical trials have demon-
strated signicant effects of pharmaco-
logic (primarily statin) therapy on CVD
outcomes in subjects with CHD and for
primary CVD prevention (210). Analyses
of diabetic subgroups of larger trials
(211215) and trials specically in sub-
jects with diabetes (216,217) showed sig-
ni cant pr i mar y and s econdar y
prevention of CVD events with and with-
out CHD deaths in diabetic populations.
As shown in Table 12, and similar to nd-
ings in nondiabetic subjects, reduction in
hard CVD outcomes (CHD death and
nonfatal MI) can be more clearly seen in
diabetic subjects with high baseline CVD
risk (known CVD and/or very high LDL
cholesterol levels), but overall the benets
of statin therapy in people with diabetes at
moderate or high risk for CVD are
convincing.
Low levels of HDL cholesterol, often
associated with elevated triglyceride lev-
els, are the most prevalent pattern of dys-
lipidemia in people with type 2 diabetes.
However, the evidence base for drugs that
target these lipid fractions is signicantly
less robust than that for statin therapy
(217). Nicotinic acid has been shown to
reduce CVD outcomes (218), although
the study was done in a nondiabetic co-
hort. Gembrozil has been shown to de-
crease rates of CVD events in subjects
without diabetes (219,220) and in a di-
abetic subgroup of a larger trial (219).
However, in a large trial specic to dia-
betic patients, fenobrate failed to re-
duce overall cardiovascular outcomes
(221).
b. Dyslipidemia treatment and target
lipid levels. For most patients with dia-
betes, the rst priority of dyslipidemia
therapy (unless severe hypertriglyceride-
mia is the immediate issue) is to lower
LDL cholesterol to a target goal of 100
mg/dl (2.60 mmol/l) (222). Lifestyle in-
tervention, including MNT, increased
physical activity, weight loss, and smok-
ing cessation, may allow some patients to
reach lipid goals. Nutrition intervention
should be tailored according to each pa-
tients age, type of diabetes, pharmacolog-
ical treatment, lipid levels, and other
medical conditions and should focus on
the reduction of saturated fat, cholesterol,
and trans unsaturated fat intake and in-
creases in n-3 fatty acids, viscous ber
(such as in oats, legumes, citrus), and
plant stanols/sterols. Glycemic control
can also benecially modify plasma lipid
levels, particularly in patients with very
high triglycerides and poor glycemic
control.
In those with clinical CVDor who are
over age 40 years and have CVD risk fac-
tors, pharmacological treatment should
be added to lifestyle therapy regardless of
baseline lipid levels. Statins are the drugs
of choice for lowering LDL cholesterol.
In patients other than those described
above, statin treatment should be consid-
ered if there is an inadequate LDL choles-
terol response to lifestyle modications
and improved glucose control or if the
patient has increased cardiovascular risk
Table 12Reduction in 10-year risk of major CVD endpoints (CHD death/non-fatal MI) in major statin trials, or sub-studies of major trials,
in diabetic subjects (N 16,032)
Study (ref.)
CVD
prevention Statin dose and comparator Risk reduction
Relative risk
reduction
Absolute risk
reduction
LDL
cholesterol
reduction (%)
4S-DM (211) 2 Simvastatin 2040 mg vs. placebo 85.7 to 43.2% 50% 42.5% 186 to 119 mg/dl (36%)
ASPEN 2 (216) 2 Atorvastatin 10 mg vs. placebo 39.5 to 24.5% 34% 12.7% 112 to 79 mg/dl (29%)
HPS-DM (212) 2 Simvastatin 40 mg vs. placebo 43.8 to 36.3% 17% 7.5% 123 to 84 mg/dl (31%)
CARE-DM (213) 2 Pravastatin 40 mg vs. placebo 40.8 to 35.4% 13% 5.4% 136 to 99 mg/dl (27%)
TNT-DM (214) 2 Atorvastatin 80 mg vs. 10 mg 26.3 to 21.6% 18% 4.7% 99 to 77 mg/dl (22%)
HPS-DM (212) 1 Simvastatin 40 mg vs. placebo 17.5 to 11.5% 34% 6.0% 124 to 86 mg/dl (31%)
CARDS (234) 1 Atorvastatin 10 mg vs. placebo 11.5 to 7.5% 35% 4.0% 118 to 71 mg/dl (40%)
ASPEN 1 (216) 1 Atorvastatin 10 mg vs. placebo 9.8 to 7.9% 19% 1.9% 114 to 80 mg/dl (30%)
ASCOT-DM (215) 1 Atorvastatin 10 mg vs. placebo 11.1 to 10.2% 8% 0.9% 125 to 82 mg/dl (34%)
Studies were of differing lengths (3.35.4 years) and used somewhat different outcomes, but all reported rates of CVD death and non-fatal MI. In this tabulation,
results of the statin on 10-year risk of major CVDendpoints (CHDdeath/non-fatal MI) are listed for comparison between studies. Correlation between 10-year CVD
risk of the control group and the absolute risk reduction with statin therapy is highly signicant (P 0.0007). Analyses provided by Craig Williams, PharmD, Oregon
Health & Science University, 2007.
Table 13Summary of recommendations
for glycemic, blood pressure, and lipid control
for adults with diabetes
A1C 7.0%*
Blood pressure 130/80 mmHg
Lipids
LDL cholesterol 100 mg/dl (2.6
mmol/l)
*Referenced to a nondiabetic range of 4.06.0%
using a DCCT-based assay. In individuals with
overt CVD, a lower LDL cholesterol goal of 70
mg/dl (1.8 mmol/l), using a high dose of a statin, is
an option.
Position Statement
(e.g., multiple cardiovascular risk factors
or long duration of diabetes). Very little
clinical trial evidence exists for type 2 di-
abetic patients under the age of 40 years
and for type 1 diabetic patients of any age.
In the Heart Protection Study (lower age
limit 40 years), the subgroup of 600 pa-
tients with type 1 diabetes had a propor-
tionately similar reduction in risk as
patients with type 2 diabetes although not
statistically signicant (212). Although
the data are not denitive, consideration
should be given to lipid-lowering goals
for type 1 diabetic patients similar to
those for type 2 diabetic patients, partic-
ularly if other cardiovascular risk factors
are present.
c. Alternative LDL cholesterol goals.
Virtually all trials of statins and CVD out-
come have tested specic doses of statins
against placebo, other doses of statin, or
other statins, rather than aiming for spe-
cic LDL cholesterol goals (223). As can
be seen in Table 10, placebo-controlled
trials generally achieved LDL cholesterol
reductions of 3040% from baseline.
Hence, LDL cholesterol lowering of this
magnitude is an acceptable outcome for
patients who cannot reach LDL choles-
terol goals due to severe baseline eleva-
t i ons i n LDL chol est er ol and/ or
intolerance of maximal, or any, statin
doses. Additionally, for those with base-
line LDL cholesterol minimally 100 mg/
dl, prescribing statin therapy to lower
LDL cholesterol to 3040% from base-
line is probably more effective than pre-
scri bi ng j ust enough t o get LDL
cholesterol slightly 100 mg/dl.
Recent clinical trials in high-risk pa-
tients, such as those with acute coronary
syndromes or previous cardiovascular
events (224226), have demonstrated
that more aggressive therapy with high
doses of statins to achieve an LDL choles-
terol of 70 mg/dl led to a signicant re-
duction in further events. Therefore, a
reduction in LDL cholesterol to a goal of
70 mg/dl is an option in very-high-risk
diabetic patients with overt CVD (227).
In individual patients, LDL choles-
terol lowering with statins is highly vari-
able, and this variable response is poorly
understood (228). Reduction of CVD
events with statins correlates very closely
with LDL cholesterol lowering (229).
When maximally tolerated doses of st-
atins fail to signicantly lower LDL cho-
lesterol (30% reduction from patients
baseline), the primary aimof combination
therapy should be to achieve additional
LDL cholesterol lowering. Niacin, feno-
brate, ezetimibe, and bile acid seques-
trants all offer additional LDL cholesterol
lowering. The evidence that combination
therapy provides a signicant increment
in CVD risk reduction over statin therapy
alone is still elusive.
d. Treatment of other lipoprotein frac-
tions or targets. Severe hypertriglyceri-
demia may warrant immediate therapy of
this abnormality with lifestyle and usually
pharmacologic therapy (bric acid deriv-
ative or niacin) to reduce the risk of acute
pancreatitis. In the absence of severe hy-
pertriglyceridemia, therapy targeting
HDL cholesterol or triglycerides has intu-
itive appeal but lacks the evidence base of
statin therapy (186). If the HDL choles-
terol is 40 mg/dl and the LDL choles-
terol is 100129 mg/dl, gembrozil or
niacin might be used, especially if a pa-
tient is intolerant to statins. Niacin is the
most effective drug for raising HDL cho-
lesterol. It can signicantly increase blood
glucose at high doses, but recent studies
demonstrate that at modest doses (750
2,000 mg/day), signicant improvements
in LDL cholesterol, HDL cholesterol, and
triglyceride levels are accompanied by
only modest changes in glucose that are
generally amenable to adjustment of dia-
betes therapy (230,231).
Combination therapy with a statin
and a brate or a statin and niacin may be
efcacious for treatment of all three lipid
fractions, but this combination is associ-
ated with an increased risk for abnormal
transaminase levels, myositis, or rhabdo-
myolysis. The risk of rhabdomyolysis is
higher with higher doses of statins and
with renal insufciency and seems to be
lower when statins are combined with fe-
nobrate than gembrozil (232). Several
ongoing trials may provide much-needed
evidence for the effects of combination
therapy on cardiovascular outcomes.
In 2008, a consensus panel convened
by ADA and the American College of Car-
diology (ACC) recommended a greater
focus on non-HDL cholesterol and apo
lipoprotein B (apo B) in patients who are
likely to have small LDL particles, such as
people with diabetes (233). The consen-
sus panel suggested that for statin-treated
patients in whom the LDL cholesterol
goal would be 70 mg/dl (non-HDL cho-
lesterol 100 mg/dl), apo B should be
measured and treated to 80 mg/dl. For
patients on statins with an LDL choles-
terol goal of 100 mg/dl (non-HDL cho-
lesterol 130 mg/dl), apo B should be
measured and treated to 90 mg/dl.
For a summary of recommendations
for glycemic, blood pressure, and lipid
control for adults with diabetes, see Table
13.
3. Antiplatelet agents
Recommendations
Consider aspirin therapy (75162 mg/

day) as a primary prevention strategy in
those with type 1 or type 2 diabetes at
increased cardiovascular risk (10-year
risk 10%). This includes most men
50 years of age or women 60 years
of age who have at least one additional
major risk factor (family history of
CVD, hypertension, smoking, dyslipi-
demia, or albuminuria). (C)
There is not sufcient evidence to rec-

ommend aspirin for primary preven-
tion in lower risk individuals, such as
men 50 years of age or women 60
years of age without other major risk
factors. For patients in these age-groups
with multiple other risk factors, clinical
judgment is required. (C)
Use aspirin therapy (75162 mg/day)

as a secondary prevention strategy in
those with diabetes with a history of
CVD. (A)
For patients with CVD and docu-

mented aspirin allergy, clopidogrel (75
mg/day) should be used. (B)
Combination therapy with ASA (75

162 mg/day) and clopidogrel (75 mg/
day) is reasonable for up to a year after
an acute coronary syndrome. (B)
ADA and the American Heart Association
(AHA) have, in the past, jointly recom-
mended that low-dose aspirin therapy be
used as a primary prevention strategy in
those with diabetes at increased cardio-
vascular risk, including those who are
over 40 years of age or those with addi-
tional risk factors (family history of CVD,
hypertension, smoking, dyslipidemia, or
albuminuria) (235). These recommenda-
tions were derived from several older tri-
als that included small numbers of
patients with diabetes.
Aspirin has been shown to be effec-
tive in reducing cardiovascular morbidity
and mortality in high-risk patients with
previous MI or stroke (secondary preven-
tion). Its net benet in primary preven-
tion among patients with no previous
cardiovascular events is more controver-
sial, both for patients with and without
a history of diabetes (236). The U.S.
Preventive Services Task Force recently
updated its evidence base and recommen-
dations about aspirin use for primary pre-
vention (237,238). The Task Force
recommended encouraging aspirin use in
men 4579 and women 5579 years of
age and not encouraging aspirin use in
younger adults and did not differentiate
based on the presence or absence of
diabetes.
Two recent randomized controlled
trials of aspirin specically in patients
with diabetes failed to show a signicant
reduction in CVD end points, raising fur-
ther questions about the efcacy of aspi-
rin for primary prevention in people with
diabetes (239,240). In 2009, ADA AHA,
and ACC convened a group of experts to
review and synthesize the available evi-
dence and use this information to create
an updated recommendation. Their re-
port, including analyses in addition to
those described below, will be published
in early 2010.
The ATT (Anti-Thrombotic Trialists)
collaborators recently published an indi-
vidual patient-level meta-analysis of the
six large trials of aspirin for primary pre-
vention in the general population (236).
These trials collectively enrolled over
95,000 participants, including almost
4,000 with diabetes. Overall, they found
that aspirin reduced the risk of vascular
events by 12% (RR 0.88 [95% CI 0.82
0.94]). The largest reduction was for non-
fatal MI (0.77 [0.670.89]). Aspirin had
little effect on CHD death (0.95 [0.78
1.15]) or total stroke (0.95 [0.851.06]).
The net effect on total stroke reected a
relative reduction in risk of ischemic
stroke (14%) and a relative increased
risk of hemorrhagic stroke (32%).
There was some evidence of a difference
in aspirin effect by sex. Aspirin reduced
CHD events in men (0.77 [0.670.89])
but not in women (0.95 [0.771.17]).
Conversely, aspirin had no effect on
stroke in men (1.01 [0.741.39]) but re-
duced stroke in women (0.77 [0.59
0.99]). These potential differences in
effect by sex were of borderline statistical
signicance, were affected strongly by the
results of one trial, and cannot be consid-
ered denitive. Notably, sex differences in
aspirins effects have not been observed in
studies of secondary prevention (236). In
the six trials examined by the ATT collab-
orators, the effect of aspirin on major vas-
cular events was similar for patients with
and without diabetes (0.88 [0.671.15]
and 0.87 [0.790.96], respectively). The
CI was wider for those with diabetes be-
cause of their smaller number.
Based on the currently available evi-
dence, aspirin appears to have a modest
effect on ischemic vascular events with
the absolute decrease in events depending
on the underlying CVD risk. The main
adverse effects appear to be an increased
risk of gastrointestinal bleeding. The ex-
cess risk may be as high as 15 per 1,000
per year in real-world settings. In adults
with CVD risk greater than 1% per year,
the number of CVD events prevented will
be similar to or greater than the number of
episodes of bleeding induced, although
these complications do not have equal ef-
fects on long-term health (241).
Average daily dosages used in most
clinical trials involving patients with dia-
betes ranged from 50650 mg but were
mostly in the range of 100325 mg/day.
There is little evidence to support any spe-
cic dose, but using the lowest possible
dosage may help reduce side effects
(242). Although platelets from patients
with diabetes have altered function, it is
unclear what, if any, impact that nding
has on the required dose of aspirin for
cardioprotective effects in the patient
with diabetes. Many alternate pathways
for platelet activation exist that are inde-
pendent of thromboxane A
2
and thus not
sensitive to the effects of aspirin (243).
Therefore, while aspirin resistance ap-
pears higher in diabetic patients when
measured by a variety of ex vivo and in
vitro methods (platelet aggrenometry,
measurement of thromboxane B
2
), these
observations alone are insufcient to em-
pirically recommend at this time that
higher doses of aspirin be used in the di-
abetic patient (244246).
Aspirin use for secondary prevention
continues to have a strong evidence base
and is recommended. Until further evi-
dence is available, low-dose (75162 mg/
day) aspirin use for primary prevention is
reasonable for adults with diabetes and no
previous history of vascular disease who
are at increased CVD risk (10-year risk of
CVD events 10%) and who are not at
increased risk for bleeding. This generally
includes most men over age 50 years and
women over age 60 years who also have
one or more of the following major risk
factors: smoking, hypertension, dyslipi-
demia, family history of premature CVD,
and albuminuria.
Aspirin should not be recommended
for those at low CVD risk (women under
age 60 years and men under age 50 years
with no major CVD risk factors; 10-year
CVD risk 5%), as the low benet is off-
set by the incidence of signicant bleed-
ing. Clinical judgment should be used for
those at intermediate risk (younger pa-
tients with one or risk factors or older pa-
tients with no risk factors; those with 10-
year CVD risk 510%) until further
research is available. Use of aspirin in pa-
tients under the age of 21 years is contra-
indicated due to the associated risk of
Reyes syndrome.
Clopidogrel has been demonstrated
to reduce CVD events in diabetic individ-
uals (247). It is recommended as adjunc-
tive therapy in the 1st year after an acute
coronary syndrome or as alternative ther-
apy in aspirin-intolerant patients.
4. Smoking cessation
Recommendations
Advise all patients not to smoke. (A)
Include smoking cessation counseling

and other forms of treatment as a rou-
tine component of diabetes care. (B)
Issues of smokinganddiabetes are reviewed
in detail in the ADA technical review (248)
and position statement (249) on this topic.
Alarge body of evidence fromepidemiolog-
ical, case-control, and cohort studies pro-
vides convincing documentation of the
causal link between cigarette smoking and
health risks. Cigarette smoking contributes
to one of every ve deaths in the U.S. and is
the most important modiable cause of pre-
mature death. Much of the prior work doc-
umenting the impact of smoking on health
did not separately discuss results on subsets
of individuals withdiabetes, suggesting that
the identied risks are at least equivalent to
those found in the general population.
Other studies of individuals with diabetes
consistently found a heightened risk of
CVDandpremature deathamong smokers.
Smoking is alsorelatedtothe premature de-
velopment of microvascular complications
of diabetes and may have a role in the de-
velopment of type 2 diabetes.
A number of large randomized clini-
cal trials have demonstrated the efcacy
and cost-effectiveness of smoking cessa-
tion counseling in changing smoking be-
havior and reducing tobacco use. The
routine and thorough assessment of to-
bacco use is important as a means of pre-
vent i ng smoki ng or encouragi ng
cessation. Special considerations should
include assessment of level of nicotine de-
pendence, which is associated with dif-
culty in quitting and relapse (250,251).
Position Statement
5. Coronary heart disease screening
and treatment
Recommendations
Screening
In asymptomatic patients, evaluate risk

factors to stratify patients by 10-year
risk, and treat risk factors accordingly.
(B)
Treatment
In patients with known CVD, ACE in-

hibitor (C), aspirin (A), and statin ther-
apy (A) (if not contraindicated) should
be used to reduce the risk of cardiovas-
cular events.
In patients with a prior MI, -blockers

should be continued for at least 2 years
after the event. (B)
Longer-term use of -blockers in the

absence of hypertension is reasonable if
well tolerated, but data are lacking. (E)
Avoid thiazolidinedione (TZD) treat-

ment in patients with symptomatic
heart failure. (C)
Metformin may be used in patients with

stable CHF if renal function is normal.
It should be avoided in unstable or hos-
pitalized patients with CHF. (C)
Screening for CAD is reviewed in a re-
cently updated consensus statement (93).
To identify the presence of CAD in dia-
betic patients without clear or suggestive
symptoms, a risk factorbased approach
to the initial diagnostic evaluation and
subsequent follow-up has intuitive ap-
peal. However, recent studies concluded
that using this approach fails to identify
which patients will have silent ischemia
on screening tests (159,252).
Candidates for cardiac testing include
those with 1) typical or atypical cardiac
symptoms and 2) an abnormal resting
electrocardiogram (ECG). The screening
of asymptomatic patients remains contro-
versial, especially since intensive medical
therapy, indicated in diabetic patients at
high risk for CVD, has an increasing evi-
dence base for providing equal outcomes
to invasive revascularization, including in
diabetic patients (253,254). There is also
recent preliminary evidence that silent
myocardial ischemia may reverse over
time, adding to the controversy concern-
ing aggressive screening strategies (255).
Finally, a recent randomized observa-
tional trial demonstrated no clinical ben-
et to routine screening of asymptomatic
patients with type 2 diabetes and normal
ECGs (256). Despite abnormal myocar-
dial perfusion imaging in more than one
in ve patients, cardiac outcomes were es-
sentially equal (and very low) in screened
versus unscreened patients. Accordingly,
the overall effectiveness, especially the
cost-effectiveness, of such an indiscrimi-
nate screening strategy is in question.
In all patients with diabetes, cardio-
vascular risk factors should be assessed at
least annually. These risk factors include
dyslipidemia, hypertension, smoking, a
positive family history of premature cor-
onary disease, and the presence of micro-
or macroalbuminuria. Abnormal risk
factors should be treated as described
elsewhere in these guidelines. Patients at
increased CHDrisk should receive aspirin
and a statin, and ACE inhibitor, or ARB
therapy if hypertensive, unless there are
contraindications to a particular drug
class. While clear benet exists for ACE
inhibitor and ARB therapy in patients
with nephropathy or hypertension, the
benets in patients with CVD in the ab-
sence of these conditions is less clear,
especially when LDL cholesterol is con-
comitantly controlled (257,258).
B. Nephropathy screening and
treatment
Recommendations
To reduce the risk or slow the progres-

sion of nephropathy, optimize glucose
control. (A)

sion of nephropathy, optimize blood
pressure control. (A)
Screening
Perform an annual test to assess urine

albumin excretion in type 1 diabetic pa-
tients with diabetes duration of 5 years
and in all type 2 diabetic patients, start-
ing at diagnosis. (E)
Measure serumcreatinine at least annu-

ally in all adults with diabetes regard-
less of the degree of urine albumin
excretion. The serum creatinine should
be used to estimate GFR and stage the
level of chronic kidney disease (CKD),
if present. (E)
Treatment
In the treatment of the nonpregnant pa-

tient with micro- or macroalbuminuria,
either ACE inhibitors or ARBs should
be used. (A)
While there are no adequate head-to-

head comparisons of ACE inhibitors
and ARBs, there is clinical trial support
for each of the following statements:
In patients with type 1 diabetes, hy-

pertension, and any degree of albu-
minuria, ACE inhibitors have been
shown to delay the progression of ne-
phropathy. (A)

pertension, and microalbuminuria,
both ACE inhibitors and ARBs have
been shown to delay the progression
to macroalbuminuria. (A)

pertension, macroalbuminuria, and
renal insufciency (serum creatinine
1.5 mg/dl), ARBs have been shown
to delay the progression of nephrop-
athy. (A)
If one class is not tolerated, the other

should be substituted. (E)
Reduction of protein intake to 0.81.0

g kg body wt
1
day
1
in individuals
with diabetes and the earlier stages of
CKD and to 0.8 g kg body wt
1
day
1
in the later stages of CKD may improve
measures of renal function (urine albu-
min excretion rate and GFR) and is rec-
ommended. (B)
When ACE inhibitors, ARBs, or diuret-

ics are used, monitor serum creatinine
and potassium levels for the develop-
ment of acute kidney disease and hy-
perkalemia. (E)
Continued monitoring of urine albu-

min excretion to assess both response
to therapy and progression of disease is
recommended. (E)
Consider referral to a physician experi-

enced in the care of kidney disease
when there is uncertainty about the eti-
ology of kidney disease (active urine
sediment, absence of retinopathy, or
rapid decline in GFR), difcult manage-
ment issues, or advanced kidney dis-
ease. (B)
Diabetic nephropathy occurs in 2040%
of patients with diabetes and is the single
leading cause of end-stage renal disease
(ESRD). Persistent albuminuria in the
range of 30299 mg/24 h (microalbu-
minuria) has been shown to be the earliest
stage of diabetic nephropathy in type 1
diabetes and a marker for development of
nephropathy in type 2 diabetes. Mi-
croalbuminuria is also a well-established
marker of increased CVD risk (259,260).
Patients with microalbuminuria who
progress to macroalbuminuria (300
mg/24 h) are likely to progress to ESRD
(261,262). However, a number of inter-
ventions have been demonstrated to re-
duce the risk and slow the progression of
renal disease.
Intensive diabetes management
wi t h t he goal of achi evi ng near-
normoglycemia has been shown in large
prospective randomized studies to de-
lay the onset of microalbuminuria and
the progression of micro- to macroalbu-
mi nuri a i n pat i ent s wi t h t ype 1
(263,264) and type 2 (57,58) diabetes.
The UKPDS provided strong evidence
that control of blood pressure can re-
duce the development of nephropathy
(187). In addition, large prospective
randomized studies in patients with
type 1 diabetes have demonstrated that
achievement of lower levels of systolic
blood pressure (140 mmHg) resulting
from treatment using ACE inhibitors
provides a selective benet over other
antihypertensive drug classes in delay-
ing the progression from micro- to mac-
roalbuminuria and can slow the decline
in GFR in patients with macroalbumin-
uria (205,206,265). In type 2 diabetes
with hypertension and normoalbuminuria,
RAS inhibition has been demonstrated to
delay onset of microalbuminuria (266).
In addition, ACE inhibitors have been
shown to reduce major CVD outcomes
(i.e., MI, stroke, and death) in patients
with diabetes (199), thus further support-
ing the use of these agents in patients with
microalbuminuria, a CVD risk factor.
ARBs do not prevent microalbuminuria in
normotensive patients with type 1 or type
2 diabetes (267,268); however, ARBs
have been shown to reduce the rate of
progression from micro- to macroalbu-
minuria as well as ESRD in patients with
type 2 diabetes (269271). Some evi-
dence suggests that ARBs have a smaller
magnitude of rise in potassium compared
with ACE inhibitors in people with ne-
phropathy (272,273). It is important to
note that both ACE inhibitors and ARBs
reduce loss of kidney function in people
with diabetic nephropathy, above and be-
yond any such effect attributable to a re-
duction in systemic blood pressure.
Combinations of drugs that block the ren-
nin-angiotensin-aldosterone system (e.g.,
an ACE inhibitor plus an ARB, a miner-
alocorticoid antagonist, or a direct renin
inhibitor) have been shown to provide ad-
ditional lowering of albuminuria (274
277). However, the long-term effects of
such combinations on renal or cardiovas-
cular outcomes have not yet been evalu-
ated in clinical trials.
Other drugs, such as diuretics, cal-
cium channel blockers, and -blockers,
should be used as additional therapy to
further lower blood pressure in patients
already treated with ACE inhibitors or
ARBs (204) or as alternate therapy in the
rare individual unable to tolerate ACE in-
hibitors or ARBs.
Studies in patients with varying stages
of nephropathy have shown that protein
restriction helps slow the progression of
albuminuria, GFR decline, and occur-
rence of ESRD (278281). Protein re-
s t r i ct i on s houl d be cons i der ed
particularly in patients whose nephropa-
thy seems to be progressing despite opti-
mal glucose and blood pressure control
and use of ACE inhibitor and/or ARBs
(281).
Assessment of albuminuria status
and renal function
Screening for microalbuminuria can be
performed by measurement of the albu-
min-to-creatinine ratio in a random spot
collection (preferred method); 24-h or
timed collections are more burdensome
and add little to prediction or accuracy
(282,283). Measurement of a spot urine
for albumin only, whether by immunoas-
say or by using a dipstick test specic for
microalbumin, without simultaneously
measuring urine creatinine, is somewhat
less expensive but susceptible to false-
negative and -positive determinations as a
result of variation in urine concentration
due to hydration and other factors.
Abnormalities of albumin excretion
are dened in Table 14. Because of vari-
ability in urinary albumin excretion, two
of three specimens collected within a 3- to
6-month period should be abnormal be-
fore considering a patient to have crossed
one of these diagnostic thresholds. Exer-
cise within 24 h, infection, fever, CHF,
marked hyperglycemia, and marked hy-
pertension may elevate urinary albumin
excretion over baseline values.
Information on presence of abnormal
urine albumin excretion in addition to
level of GFR may be used to stage CKD.
The National Kidney Foundation classi-
cation (Table 15) is primarily based on
GFR levels and therefore differs from
other systems, in which staging is based
primarily on urinary albumin excretion
(284). Studies have found decreased GFR
in the absence of increased urine albumin
excretion in a substantial percentage of
adults with diabetes (285,286). Epidemi-
ologic evidence suggests that a substantial
fraction of those with CKD in the setting
of diabetes have little or no detectable al-
buminuria (285). Serum creatinine
should therefore be measured at least an-
nually in all adults with diabetes, regard-
less of the degree of urine albumin
excretion.
Serum creatinine should be used to
estimate GFR and to stage the level of
CKD, if present. Estimated GFR (eGFR) is
commonly co-reported by laboratories or
can be estimated using formulae such as
the Modication of Diet in Renal Disease
(MDRD) study equation (287). Recent re-
ports have indicated that the MDRD is
more accurate for the diagnosis and strat-
ication of CKD in patients with diabetes
than the Cockcroft-Gault formula (288).
GFR calculators are available at http://
www.nkdep.nih.gov.
The role of continued annual quanti-
tative assessment of albumin excretion af-
ter diagnosis of microalbuminuria and
institution of ACE inhibitor or ARB ther-
apy and blood pressure control is unclear.
Continued surveillance can assess both
response to therapy and progression of
disease. Some suggest that reducing ab-
normal albuminuria (30 mg/g) to the
normal or near-normal range may im-
prove renal and cardiovascular prognosis,
but this approach has not been formally
evaluated in prospective trials.
Complications of kidney disease cor-
relate with level of kidney function. When
the eGFR is less than 60 ml min/1.73 m
2
,
screening for anemia, malnutrition, and
metabolic bone disease is indicated. Early
vaccination against Hepatitis B is indi-
cated in patients likely to progress to end-
stage kidney disease.
Consider referral to a physician expe-
rienced in the care of kidney disease when
there is uncertainty about the etiology of
kidney disease (active urine sediment, ab-
sence of retinopathy, or rapid decline in
GFR), difcult management issues, or ad-
vanced kidney disease. The threshold for
referral may vary depending on the fre-
quency with which a provider encounters
diabetic patients with signicant kidney
disease. Consultation with a nephrologist
when stage 4 CKD develops has been
Table 14Denitions of abnormalities in al-
bumin excretion
Category
Spot collection
(g/mg
creatinine)
Normal 30
Microalbuminuria 30299
Macroalbuminuria (clinical) 300
Position Statement
found to reduce cost, improve quality of
care, and keep people off dialysis longer
(289,290). However, nonrenal specialists
should not delay educating their patients
about the progressive nature of diabetic
kidney disease, the renal preservation
benets of aggressive treatment of blood
pressure, blood glucose, and hyperlipid-
emia, and the potential need for renal re-
placement therapy.
C. Retinopathy screening and
treatment
Recommendations

sion of retinopathy, optimize glycemic
control. (A)

sion of retinopathy, optimize blood
pressure control. (A)
Screening
Adults and children aged 10 years or

older with type 1 diabetes should have
an initial dilated and comprehensive
eye examination by an ophthalmologist
or optometrist within 5 years after the
onset of diabetes. (B)
Patients with type 2 diabetes should

have an initial dilated and comprehen-
sive eye examination by an ophthalmol-
ogist or optometrist shortly after the
diagnosis of diabetes. (B)
Subsequent examinations for type 1

and type 2 diabetic patients should be
repeated annually by an ophthalmolo-
gist or optometrist. Less frequent exams
(every 23 years) may be considered
following one or more normal eye ex-
ams. Examinations will be required
more frequently if retinopathy is pro-
gressing. (B)
High-quality fundus photographs can

detect most clinically signicant dia-
betic retinopathy. Interpretation of the
images should be performed by a
trained eye care provider. While retinal
photography may serve as a screening
tool for retinopathy, it is not a substi-
tute for a comprehensive eye exam,
which should be performed at least ini-
tially and at intervals thereafter as rec-
ommended by an eye care professional.
(E)
Women with preexisting diabetes who

are planning pregnancy or who have
become pregnant should have a com-
prehensive eye examination and be
counseled on the risk of development
and/or progression of diabetic retinop-
athy. Eye examination should occur in
the rst trimester with close follow-up
throughout pregnancy and for 1 year
postpartum. (B)
Treatment
Promptly refer patients with any level of

macular edema, severe NPDR, or any
PDR to an ophthalmologist who is
knowledgeable and experienced in the
management and treatment of diabetic
retinopathy. (A)
Laser photocoagulation therapy is indi-

cated to reduce the risk of vision loss in
patients with high-risk PDR, clinically
signicant macular edema, and in some
cases of severe NPDR. (A)
The presence of retinopathy is not a

contraindication to aspirin therapy for
cardioprotection, as this therapy does
not increase the risk of retinal hemor-
rhage. (A)
Diabetic retinopathy is a highly specic
vascular complication of both type 1 and
type 2 diabetes, with prevalence strongly
related to duration of diabetes. Diabetic
retinopathy is the most frequent cause of
newcases of blindness among adults aged
2074 years. Glaucoma, cataracts, and
other disorders of the eye occur earlier
and more frequently in people with
diabetes.
In addition to duration of diabetes,
other factors that increase the risk of, or
are associated with, retinopathy include
chronic hyperglycemia (291), the pres-
ence of nephropathy (292), and hyper-
tensi on (293). Intensi ve di abetes
management with the goal of achieving
near normoglycemia has been shown in
large prospective randomized studies to
prevent and/or delay the onset and pro-
gr essi on of di abet i c r et i nopat hy
(53,57,58). Lowering blood pressure has
been shown to decrease the progression
of retinopathy (187). Several case series
and a controlled prospective study sug-
gest that pregnancy in type 1 diabetic pa-
t i ent s may aggravat e ret i nopat hy
(294,295); laser photocoagulation sur-
gery can minimize this risk (295).
One of the main motivations for
screening for diabetic retinopathy is the
established efcacy of laser photocoagu-
lation surgery in preventing vision loss.
Two large trials, the Diabetic Retinopathy
Study (DRS) and the Early Treatment Di-
abetic Retinopathy Study (ETDRS), pro-
vide the strongest support for the
therapeutic benets of photocoagulation
surgery.
The DRS (296) showed that panreti-
nal photocoagulation surgery reduced the
risk of severe vision loss from PDR from
15.9% in untreated eyes to 6.4% in
treated eyes. The benet was greatest
among patients whose baseline evalua-
tion revealed high-risk characteristics
(chiey disc neovascularization or vitre-
ous hemorrhage). Given the risks of mod-
est loss of visual acuity and contraction of
the visual eld from panretinal laser sur-
gery, such therapy is primarily recom-
mended for eyes with PDR approaching
or having high-risk characteristics.
The ETDRS (297) established the
benet of focal laser photocoagulation
surgery in eyes with macular edema,
particularly those with clinically signif-
icant macular edema, with reduction of
doubling of the visual angle (e.g., 20/
50 20/100) from 20% in untreated
eyes to 8% in treated eyes. The ETDRS
also veried the benets of panretinal
photocoagulation for high-risk PDR,
but not for mild or moderate NPDR. In
older-onset patients with severe NPDR
or less-than-high-risk PDR, the risk of
severe vision loss or vitrectomy was re-
duced 50% by early laser photocoagu-
lation surgery at these stages.
Table 15Stages of CKD
Stage Description
GFR (ml/min per
1.73 m
2
body
surface area)
1 Kidney damage* with normal or increased GFR 90
2 Kidney damage* with mildly decreased GFR 6089
3 Moderately decreased GFR 3059
4 Severely decreased GFR 1529
5 Kidney failure 15 or dialysis
*Kidney damage dened as abnormalities on pathologic, urine, blood, or imaging tests. Adapted from ref.
283.
Laser photocoagulation surgery in
both trials was benecial in reducing the
risk of further vision loss, but generally
not benecial in reversing already dimin-
ished acuity. This preventive effect and
the fact that patients with PDR or macular
edema may be asymptomatic provide
strong support for a screening programto
detect diabetic retinopathy.
As retinopathy is estimated to take at
least 5 years to develop after the onset of
hyperglycemia (298), patients with type 1
diabetes should have an initial dilated and
comprehensive eye examination within 5
years after the onset of diabetes. Patients
with type 2 diabetes who generally have
had years of undiagnosed diabetes (299)
and who have a signicant risk of preva-
lent diabetic retinopathy at the time of
diabetes diagnosis should have an initial
dilated and comprehensive eye examina-
tion soon after diagnosis. Examinations
should be performed by an ophthalmolo-
gist or optometrist who is knowledgeable
and experienced in diagnosing the pres-
ence of diabetic retinopathy and is aware
of its management. Subsequent examina-
tions for type 1 and type 2 diabetic pa-
tients are generally repeated annually.
Less frequent exams (every 23 years)
may be cost effective after one or more
normal eye exams (300302), while ex-
aminations will be required more fre-
quently if retinopathy is progressing.
Examinations can also be done with
retinal photographs (with or without di-
lation of the pupil) read by experienced
experts. In-person exams are still nec-
essary when the photos are unaccept-
able and for follow-up of abnormalities
detected. Photos are not a substitute for
a comprehensive eye exam, which
should be performed at least initially
and at intervals thereafter as recom-
mended by an eye care professional.
This technology has great potential in
areas where qualied eye care profes-
sionals are not available and may also
enhance efciency and reduce costs
when the expertise of ophthalmologists
can be used for more complex examina-
tions and for therapy (303).
Results of eye examinations should
be documented and transmitted to the
referring health care professional. For a
detailed review of the evidence and fur-
ther discussion of diabetic retinopathy,
see the ADA technical review and
position statement on this subject
(304,305).
D. Neuropathy screening and
treatment (306)
Recommendations
All patients should be screened for dis-

tal symmetric polyneuropathy (DPN) at
diagnosis and at least annually thereaf-
ter using simple clinical tests. (B)
Electrophysiological testing is rarely

needed, except in situations where the
clinical features are atypical. (E)
Screening for signs and symptoms of

cardiovascular autonomic neuropathy
should be instituted at diagnosis of type
2 diabetes and 5 years after the diagno-
sis of type 1 diabetes. Special testing is
rarely needed and may not affect man-
agement or outcomes. (E)
Medications for the relief of specic

symptoms related to DPN and auto-
nomic neuropathy are recommended,
as they improve the quality of life of the
patient. (E)
The diabetic neuropathies are heteroge-
neous with diverse clinical manifesta-
tions. They may be focal or diffuse. Most
common among the neuropathies are
chronic sensorimotor DPN and auto-
nomic neuropathy. Although DPN is a
diagnosis of exclusion, complex investi-
gations to exclude other conditions are
rarely needed.
The early recognition and appropri-
ate management of neuropathy in the pa-
tient with diabetes is important for a
number of reasons: 1) nondiabetic neu-
ropathies may be present in patients with
diabetes and may be treatable; 2) a num-
ber of treatment options exist for symp-
tomatic diabetic neuropathy; 3) up to
50% of DPN may be asymptomatic, and
patients are at risk of insensate injury to
their feet; 4) autonomic neuropathy may
involve every system in the body; and 5)
cardiovascular autonomic neuropathy
causes substantial morbidity and mortal-
ity. Specic treatment for the underlying
nerve damage is not currently available,
other than improved glycemic control,
which may slow progression but not re-
verse neuronal loss. Effective symptom-
atic treatments are available for some
manifestations of DPN and autonomic
neuropathy.
1. Diagnosis of neuropathy
a. Distal symmetric polyneuropathy.
Patients with diabetes should be screened
annually for DPN using tests such as pin-
prick sensation, vibration perception (us-
i ng a 128-Hz t uni ng f ork), 10-g
monolament pressure sensation at the
distal plantar aspect of both great toes and
metatarsal joints, and assessment of ankle
reexes. Combinations of more than one
test have 87% sensitivity in detecting
DPN. Loss of 10-g monolament percep-
tion and reduced vibration perception
predict foot ulcers (306).
b. Diabetic autonomic neuropathy (307).
The symptoms and signs of autonomic
dysfunction should be elicited carefully
during the history and physical examina-
tion. Major clinical manifestations of dia-
betic autonomic neuropathy include
resting tachycardia, exercise intolerance,
orthostatic hypotension, constipation,
gastroparesis, erectile dysfunction, sudo-
motor dysfunction, impaired neurovas-
cular function, brittle diabetes, and
hypoglycemic autonomic failure.
Cardiovascular autonomic neuropa-
thy, a CVD risk factor (93), is the most
studied and clinically important form of
diabetic autonomic neuropathy. Cardio-
vascular autonomic neuropathy may be
indicated by resting tachycardia (100
bpm), orthostasis (a fall in systolic blood
pressure 20 mmHg upon standing
without an appropriate heart rate re-
sponse), or other disturbances in auto-
nomic nervous system function involving
the skin, pupils, or gastrointestinal and
genitourinary systems.
Gastrointestinal neuropathies (e.g.,
esophageal enteropathy, gastroparesis,
constipation, diarrhea, and fecal incon-
tinence) are common, and any section
of the gastrointestinal tract may be af-
fected. Gastroparesis should be sus-
pected in individuals with erratic
glucose control or with upper gastroin-
testinal symptoms without other identi-
ed cause. Evaluation of solid-phase
gastric emptying using double-isotope
scintigraphy may be done if symptoms
are suggestive, but test results often cor-
relate poorly with symptoms. Constipa-
t i on i s t he most common l ower-
gastroi ntesti nal symptom but can
alternate with episodes of diarrhea.
Diabetic autonomic neuropathy is
also associated with genitourinary tract
disturbances. In men, diabetic autonomic
neuropathy may cause erectile dysfunc-
tion and/or retrograde ejaculation. Evalu-
ation of bladder dysfunction should be
performed for individuals with diabetes
who have recurrent urinary tract infec-
tions, pyelonephritis, incontinence, or a
palpable bladder.
Position Statement
2. Symptomatic treatments
a. Distal symmetric polyneuropathy.
The rst step in management of patients
with DPN should be to aim for stable and
optimal glycemic control. Although con-
trolled trial evidence is lacking, several
observational studies suggest that neuro-
pathic symptoms improve not only with
optimization of control, but also with the
avoidance of extreme blood glucose uc-
tuations. Patients with painful DPN may
benet from pharmacological treatment
of their symptoms: many agents have ef-
cacy conrmed in published random-
ized controlled trials, with several FDA-
approved for the management of painful
DPN. See Table 16 for examples of agents
to treat DPN pain.
b. Diabetic autonomic neuropathy. Gas-
troparesis symptoms may improve with
dietary changes and prokinetic agents
such as metoclopramide or erythromycin.
Treatments for erectile dysfunction may
include phosphodiesterase type 5 inhibi-
tors, intracorporeal or intraurethral pros-
taglandins, vacuum devices, or penile
prostheses. Interventions for other mani-
festations of autonomic neuropathy are
described in the ADA statement on neu-
ropathy (306). As with DPN treatments,
these interventions do not change the un-
derlying pathology and natural history of
the disease process but may have a posi-
tive impact on the quality of life of the
patient.
E. Foot care
Recommendations
For all patients with diabetes, perform

an annual comprehensive foot exami-
nation to identify risk factors predictive
of ulcers and amputations. The foot ex-
amination should include inspection,
assessment of foot pulses, and testing
for loss of protective sensation (LOPS)
(10-g monolament plus testing any
one of: vibration using 128-Hz tuning
fork, pinprick sensation, ankle reexes,
or vibration perception threshold). (B)
Provide general foot self-care education

to all patients with diabetes. (B)
A multidisciplinary approach is recom-

mended for individuals with foot ulcers
and high-risk feet, especially those with
a history of prior ulcer or amputation.
(B)
Refer patients who smoke, have LOPS

and structural abnormalities, or have
history of prior lower-extremity com-
plications to foot care specialists for on-
going preventive care and life-long
surveillance. (C)
Initial screening for peripheral arterial

disease (PAD) should include a history
for claudication and an assessment of
the pedal pulses. Consider obtaining an
ankle-brachial index (ABI), as many pa-
tients with PAD are asymptomatic. (C)
Refer patients with signicant claudica-

tion or a positive ABI for further vascu-
lar assessment and consider exercise,
medications, and surgical options. (C)
Amputation and foot ulceration, conse-
quences of diabetic neuropathy and/or
PAD, are common and major causes of
morbidity and disability in people with
diabetes. Early recognition and manage-
ment of risk factors can prevent or delay
adverse outcomes.
The risk of ulcers or amputations is
increased in people who have the follow-
ing risk factors:
previous amputation
past foot ulcer history
peripheral neuropathy
foot deformity
peripheral vascular disease
visual impairment
diabetic nephropathy (especially pa-

tients on dialysis)
poor glycemic control
cigarette smoking
Many studies have been published pro-
posing a range of tests that might usefully
identify patients at risk of foot ulceration,
creating confusion among practitioners as
to which screening tests should be
adopted in clinical practice. An ADA task
force was therefore assembled in 2008 to
concisely summarize recent literature in
this area and recommend what should be
included in the comprehensive foot exam
for adult patients with diabetes. Their rec-
ommendations are summarized below,
but clinicians should refer to the task
force report (308) for further details and
practical descriptions of how to perform
components of the comprehensive foot
examination.
At least annually, all adults with dia-
betes should undergo a comprehensive
foot examination to identify high-risk
conditions. Clinicians should ask about
history of previous foot ulceration or am-
putation, neuropathic or peripheral vas-
cular symptoms, impaired vision, tobacco
use, and foot care practices. A general in-
spection of skin integrity and musculo-
skeletal deformities should be done in a
well-lit room. Vascular assessment would
include inspection and assessment of
pedal pulses.
The neurologic exam recommended
is designed to identify LOPS rather than
early neuropathy. The clinical examina-
tion to identify LOPS is simple and re-
quires no expensive equipment. Five
simple clinical tests (use of a 10-g mono-
lament, vibration testing using a 128-Hz
tuning fork, tests of pinprick sensation,
ankle reex assessment, and testing vibra-
tion perception threshold with a biothesi-
ometer), each with evidence from well-
conducted prospective clinical cohort
studies, are considered useful in the diag-
nosis of LOPS in the diabetic foot. The
task force agrees that any of the ve tests
listed could be used by clinicians to iden-
tify LOPS, although ideally two of these
should be regularly performed during the
screening examnormally the 10-g
monolament and one other test. One or
more abnormal tests would suggest
LOPS, while at least two normal tests (and
no abnormal test) would rule out LOPS.
The last test listed, vibration assessment
using a biothesiometer or similar instru-
ment, is widely used in the U.S.; however,
Table 16Table of drugs to treat symptomatic DPN
Class Examples Typical doses*
Tricyclic drugs Amitriptyline 1075 mg at bedtime
Nortriptyline 2575 mg at bedtime
Imipramine 2575 mg at bedtime
Anticonvulsants Gabapentin 3001,200 mg t.i.d.
Carbamazepine 200400 mg t.i.d.
Pregabalin 100 mg t.i.d.
5-Hydroxytryptamine and
norepinephrine uptake
inhibitor
Duloxetine 60120 mg daily fs
Substance P inhibitor Capsaicin cream 0.0250.075% applied t.i.d.-q.i.d.
*Dose response may vary; initial doses need to be low and titrated up. Has FDA indication for treatment of
painful diabetic neuropathy.
identication of the patient with LOPS
can easily be carried out without this or
other expensive equipment.
Initial screening for PAD should in-
clude a history for claudication and an
assessment of the pedal pulses. Adiagnos-
tic ABI should be performed in any pa-
tient with symptoms of PAD. Due to the
high estimated prevalence of PAD in pa-
tients with diabetes and the fact that
many patients with PAD are asymptom-
atic, an ADA consensus statement on
PAD (309) suggested that a screening
of ABI be performed in patients over
50 years of age and considered in patients
under 50 years of age who have other
PADrisk factors (e.g., smoking, hyperten-
sion, hyperlipidemia, or duration of dia-
betes 10 years). Refer patients with
signicant symptoms or a positive ABI
for further vascular assessment and con-
sider exercise, medications, and surgical
options (309).
Patients with diabetes and high-risk
foot conditions should be educated re-
garding their risk factors and appropriate
management. Patients at risk should un-
derstand the implications of the LOPS,
the importance of foot monitoring on a
daily basis, the proper care of the foot in-
cluding nail and skin care, and the selec-
tion of appropriate footwear. Patients
with LOPS should be educated on ways to
substitute other sensory modalities (hand
palpation, visual inspection) for surveil-
lance of early foot problems. Patients un-
derstanding of these issues and their
physical ability to conduct proper foot
surveillance and care should be assessed.
Patients with visual difculties, physical
constraints preventing movement, or cog-
nitive problems that impair their ability to
assess the condition of the foot and to in-
stitute appropriate responses will need
other people, such as family members, to
assist in their care.
People with neuropathy or evidence
of increased plantar pressure (e.g., ery-
thema, warmth, callus, or measured pres-
sure) may be adequately managed with
well-tted walking shoes or athletic
shoes that cushion the feet and redis-
tribute pressure. Callus can be debrided
with a scalpel by a foot care specialist or
other health professional with experience
and training in foot care. People with
bony deformities (e.g., hammertoes,
prominent metatarsal heads, or bunions)
may need extra-wide or -depth shoes.
People with extreme bony deformities
(e.g., Charcot foot) who cannot be accom-
modated with commercial therapeutic
footwear may need custom-molded
shoes.
Foot ulcers and wound care may re-
quire care by a podiatrist, orthopedic
or vascular surgeon, or rehabilitation
specialist experienced in the manage-
ment of individuals with diabetes. For a
complete discussion, see the ADA con-
sensus statement on diabetic foot wound
care (310).
VII. DIABETES CARE IN
SPECIFIC POPULATIONS
A. Children and adolescents
1. Type 1 diabetes
Three-quarters of all cases of type 1 dia-
betes are diagnosed in individuals 18
years of age. Because children are not sim-
ply small adults, it is appropriate to con-
sider the unique aspects of care and
management of children and adolescents
with type 1 diabetes. Children with dia-
betes differ from adults in many respects,
including changes in insulin sensitivity
related to sexual maturity and physical
growth, ability to provide self-care, super-
vision in child care and school, and
unique neurologic vulnerability to hypo-
glycemia and DKA. Attention to such is-
sues as family dynamics, developmental
stages, and physiologic differences related
to sexual maturity are all essential in de-
veloping and implementing an optimal
diabetes regimen. Although recommen-
dations for children and adolescents are
less likely to be based on clinical trial ev-
idence, because of current and historical
restraints placed on conducting research
in children, expert opinion and a review
of available and relevant experimental
data are summarized in the ADA state-
ment on care of children and adolescents
with type 1 diabetes (311).
Ideally, the care of a child or adoles-
cent with type 1 diabetes should be pro-
vided by a multidisciplinary team of
specialists trained in the care of children
with pediatric diabetes. At the very least,
education of the child and family should
be provided by health care providers
trained and experienced in childhood di-
abetes and sensitive to the challenges
posed by diabetes in this age-group. At
the time of initial diagnosis, it is essential
that diabetes education be provided in a
timely fashion, with the expectation that
the balance between adult supervision
and self-care should be dened by, and
will evolve according to, physical, psy-
chological, and emotional maturity. MNT
should be provided at diagnosis, and at
least annually thereafter, by an individual
experienced with the nutritional needs of
the growing child and the behavioral is-
sues that have an impact on adolescent
diets, including risk for disordered eating.
a. Glycemic control
Recommendations
Consider age when setting glycemic

goals in children and adolescents with
type 1 diabetes, with less stringent goals
for younger children. (E)
While current standards for diabetes
management reect the need to maintain
glucose control as near to normal as safely
possible, special consideration must be
given to the unique risks of hypoglycemia
in young children. Glycemic goals need to
be modied to take into account the fact
that most children 6 or 7 years of age
have a form of hypoglycemic unaware-
ness. Their counterregulatory mecha-
nisms are immature and they may lack the
cognitive capacity to recognize and re-
spond to hypoglycemic symptoms, plac-
ing them at greater risk for severe
hypoglycemia and its sequelae. In addi-
tion, and unlike the case in adults, young
children under the age of 5 years are at
risk for permanent cognitive impairment
after episodes of severe hypoglycemia
(312314). Extensive evidence indicates
that near normalization of blood glucose
levels is seldomattainable in children and
adolescents after the honeymoon (remis-
sion) period. The A1C level achieved in
the intensive adolescent cohort of the
DCCT group was 1% higher than that
achieved by adult DCCT subjects and
above current ADA recommendations for
patients in general. However, the in-
creased frequency of use of basal bolus
regimens (including insulin pumps) in
youth from infancy through adolescence
has been associated with more children
reaching ADA blood glucose targets
(315,316) in those families in which both
parents and the child with diabetes are
motivated to perform the required diabe-
tes-related tasks.
In selecting glycemic goals, the bene-
ts on long-term health outcomes of
achieving a lower A1C must be weighed
against the unique risks of hypoglycemia
and the difculties achieving near-
normoglycemia in children and youth.
Age-specic glycemic and A1C goals are
presented in Table 17.
Position Statement
b. Screening and management of
chronic complications in children and
adolescents with type 1 diabetes
i. Nephropathy
Recommendations
Annual screening for microalbumin-

uria, with a random spot urine sample
for microalbumin-to-creatinine ratio,
should be initiated once the child is 10
years of age and has had diabetes for 5
years. (E)
Conrmed, persistently elevated mi-

croalbumin levels on two additional
urine specimens should be treated with
an ACE inhibitor, titrated to normaliza-
tion of microalbumin excretion if pos-
sible. (E)
ii. Hypertension
Recommendations
Treatment of high-normal blood pres-

sure (systolic or diastolic blood pres-
sure consistently above the 90th
percentile for age, sex, and height)
should include dietary intervention
and exercise aimed at weight control
and increased physical activity, if ap-
propriate. If target blood pressure is not
reached with 36 months of lifestyle
intervention, pharmacologic treatment
should be initiated. (E)
Pharmacologic treatment of hyperten-

sion (systolic or diastolic blood pres-
sure consistently above the 95th
percentile for age, sex, and height or
consistently 130/80 mmHg, if 95%
exceeds that value) should be initiated
as soon as the diagnosis is conrmed.
(E)
ACE inhibitors should be considered

for the initial treatment of hyperten-
sion. (E)
The goal of treatment is a blood pres-

sure consistently 130/80 or belowthe
90th percentile for age, sex, and height,
whichever is lower. (E)
Hypertension in childhood is dened as
an average systolic or diastolic blood pres-
sure 95th percentile for age, sex, and
height percentile measured on at least
three separate days. High-normal blood
pressure is dened as an average systolic
or diastolic blood pressure 90th but
95th percentile for age, sex, and height
percentile measured on at least 3 separate
days. Normal blood pressure levels for
age, sex, and height and appropriate
methods for determinations are available
online at www.nhlbi.nih.gov/health/
prof/heart/hbp/hbp_ped.pdf.
iii. Dyslipidemia
Recommendations
Screening
If there is a family history of hypercho-

lesterolemia (total cholesterol 240
mg/dl) or a cardiovascular event before
age 55 years, or if family history is un-
known, then a fasting lipid prole
should be performed on children 2
years of age soon after diagnosis (after
glucose control has been established).
If family history is not of concern, then
the rst lipid screening should be per-
formed at puberty (10 years). All chil-
dren diagnosed with diabetes at or after
puberty should have a fasting lipid
prole performed soon after diagnosis
(after glucose control has been estab-
lished). (E)
For both age-groups, if lipids are abnor-

mal, annual monitoring is recom-
mended. If LDL cholesterol values are
within the accepted risk levels (100
mg/dl [2.6 mmol/l]), a lipid prole
should be repeated every 5 years. (E)
Treatment
Initial therapy should consist of optimi-

zation of glucose control and MNT us-
ing a Step II AHA diet aimed at a
decrease in the amount of saturated fat
in the diet. (E)
After the age of 10 years, the addition of

a statin is recommended in patients
who, after MNT and lifestyle changes,
have LDL cholesterol 160 mg/dl (4.1
mmol/l) or LDL cholesterol 130
mg/dl (3.4 mmol/l) and one or more
CVD risk factors. (E)
The goal of therapy is an LDL choles-

terol value 100 mg/dl (2.6 mmol/l).
(E)
People diagnosed with type 1 diabetes in
childhood have a high risk of early sub-
clinical (317319) and clinical (320)
CVD. Although intervention data are
lacking, the AHA categorizes type 1 dia-
betic children in the highest tier for car-
diovascular risk and recommends both
lifestyle and pharmacologic treatment for
those with elevated LDL cholesterol levels
(321,322). Initial therapy should be with
a Step II AHA diet, which restricts satu-
rated fat to 7% of total calories and re-
stricts dietary cholesterol to 200 mg per
day. Data from randomized clinical trials
Table 17Plasma blood glucose and A1C goals for type 1 diabetes by age-group
Values by age (years)
Plasma blood glucose goal
range (mg/dl)
A1C Rationale Before meals
Bedtime/
overnight
Toddlers and preschoolers (06) 100180 110200 8.5% (but 7.5%) High risk and vulnerability to hypoglycemia
School age (612) 90180 100180 8% Risks of hypoglycemia and relatively low risk of
complications prior to puberty
Adolescents and young adults (1319) 90130 90150 7.5% Risk of severe hypoglycemia
Developmental and psychological issues
A lower goal (7.0%) is reasonable if it can be
achieved without excessive hypoglycemia
Key concepts in setting glycemic goals:
Goals should be individualized and lower goals may be reasonable based on benet-risk assessment.
Blood glucose goals should be higher than those listed above in children with frequent hypoglycemia or hypoglycemia unawareness.
Postprandial blood glucose values should be measured when there is a discrepancy between pre-prandial blood glucose values and A1C
levels and to help assess glycemia in those on basal/bolus regimens.
in children as young as 7 months of age
indicate that this diet is safe and does not
interfere with normal growth and devel-
opment (323,324).
For children over the age of 10 years
with persistent elevation of LDL choles-
terol despite lifestyle therapy, statins
should be considered. Neither long-term
safety nor cardiovascular outcome ef-
cacy has been established for children.
However, recent studies have shown
short-term safety equivalent to that seen
in adults and efcacy in lowering LDL
cholesterol levels, improving endothelial
function, and causing regression of ca-
rotid intimal thickening (325327). No
statin is approved for use under the age of
10 years, and statin treatment should gen-
erally not be used in type 1 diabetic chil-
dren prior to this age.
iv. Retinopathy
Recommendations
The rst ophthalmologic examination

should be obtained once the child is 10
years of age and has had diabetes for
35 years. (E)
After the initial examination, annual

routine follow-up is generally recom-
mended. Less frequent examinations
may be acceptable on the advice of an
eye care professional. (E)
Although retinopathy most commonly
occurs after the onset of puberty and after
510 years of diabetes duration, it has
been reported in prepubertal children
and with diabetes duration of only 12
years. Referrals should be made to eye
care professionals with expertise in dia-
betic retinopathy, an understanding of
the risk for retinopathy in the pediatric
population, and experience in counseling
the pediatric patient and family on the
importance of early prevention/inter-
vention.
v. Celiac disease
Recommendations
Children with type 1 diabetes should be

screened for celiac disease by measuring
ti ssue transgl utami nase or anti -
endomysial antibodies, with documenta-
tion of normal serum IgA levels, soon
after the diagnosis of diabetes. (E)
Testing should be repeated if growth

failure, failure to gain weight, weight
loss, or gastroenterologic symptoms oc-
cur. (E)
Consideration should be given to peri-

odic rescreening of asymptomatic indi-
viduals. (E)
Children with positive antibodies

should be referred to a gastroenterolo-
gist for evaluation. (E)
Children with conrmed celiac disease

should have consultation with a dieti-
tian and be placed on a gluten-free diet.
(E)
Celiac disease is an immune-mediated
disorder that occurs with increased fre-
quency in patients with type 1 diabetes
(116% of individuals compared with
0.31% in the general population)
(328,329). Symptoms of celiac disease in-
clude diarrhea, weight loss or poor weight
gain, growth failure, abdominal pain,
chronic fatigue, malnutrition due to mal-
absorption, other gastrointestinal prob-
lems, and unexplained hypoglycemia or
erratic blood glucose concentrations.
vi. Hypothyroidism
Recommendations
Children with type 1 diabetes should be

screened for thyroid peroxidase and
thyroglobulin antibodies at diagnosis.
(E)
Thyroid-stimulating hormone (TSH)

concentrations should be measured af-
ter metabolic control has been estab-
lished. If normal, they should be
rechecked every 12 years or if the pa-
tient develops symptoms of thyroid
dysfunction, thyromegaly, or an abnor-
mal growth rate. Free T4 should be
measured if TSH is abnormal. (E)
Autoimmune thyroid disease is the most
common autoimmune disorder associ-
ated with diabetes, occurring in 1730%
of patients with type 1 diabetes (330). The
presence of thyroid auto-antibodies is
predictive of thyroid dysfunction, gener-
ally hypothyroidism and less commonly
hyperthyroidism (331). Subclinical hy-
pothyroidism may be associated with in-
cr eas ed r i s k of s ympt omat i c
hypoglycemia (332) and with reduced
linear growth (333). Hyperthyroidism al-
ters glucose metabolism, potentially re-
sulting in deterioration of metabolic
control.
c. Self-management. No matter how
sound the medical regimen, it can only be
as good as the ability of the family and/or
individual to implement it. Family in-
volvement in diabetes remains an impor-
tant component of optimal diabetes
management throughout childhood and
into adolescence. Health care providers
who care for children and adolescents
therefore must be capable of evaluating
the behavioral, emotional, and psychoso-
cial factors that interfere with implemen-
tation and then must work with the
individual and family to resolve problems
that occur and/or to modify goals as
appropriate.
d. School and day care. Since a sizable
portion of a childs day is spent in school,
close communication with school or day
care personnel is essential for optimal di-
abetes management, safety, and maximal
academic opportunities. See VIII.B. Dia-
betes Care in the School and Day Care
Setting, for further discussion.
2. Type 2 diabetes
The incidence of type 2 diabetes in ado-
lescents is increasing, especially in ethnic
minority populations (21). Distinction
between type 1 and type 2 diabetes in
children can be difcult, since the preva-
lence of overweight in children continues
to rise and since autoantigens and ketosis
may be present in a substantial number of
patients with features of type 2 diabetes
(including obesity and acanthosis nigri-
cans). Such a distinction at the time of
diagnosis is critical because treatment
regimens, educational approaches, and
dietary counsel will differ markedly be-
tween the two diagnoses.
Type 2 diabetes has a signicant in-
ci dence of comorbi di t i es al ready
present at the time of diagnosis (334). It
is recommended that blood pressure
measurement, a fasting lipid prole,
microalbuminuria assessment, and di-
lated eye examination be performed at
the time of diagnosis. Thereafter,
screening guidelines and treatment rec-
ommendations for hypertension, dys-
l i pi demi a, mi croal bumi nuri a, and
retinopathy in youth with type 2 diabe-
tes are similar to those for youth with
type 1 diabetes. Additional problems
that may need to be addressed include
polycystic ovary disease and the various
comorbidities associated with pediatric
obesity such as sleep apnea, hepatic ste-
atosis, orthopedic complications, and
psychosocial concerns. The ADA con-
sensus statement on this subject (23)
provides guidance on the prevention,
screening, and treatment of type 2 dia-
betes and its comorbidities in young
people.
Position Statement
B. Preconception care
Recommendations
A1C levels should be as close to normal

as possible (7%) in an individual pa-
tient before conception is attempted.
(B)
Starting at puberty, preconception

counseling should be incorporated in
the routine diabetes clinic visit for all
women of child-bearing potential. (C)
Women with diabetes who are contem-

plating pregnancy should be evaluated
and, if indicated, treated for diabetic
retinopathy, nephropathy, neuropathy,
and CVD. (E)
Medications used by such women

should be evaluated prior to concep-
tion because drugs commonly used to
treat diabetes and its complications
may be contraindicated or not recom-
mended in pregnancy, including st-
atins, ACE inhibitors, ARBs, and most
noninsulin therapies. (E)
Major congenital malformations remain
the leading cause of mortality and serious
morbidity in infants of mothers with type
1 or type 2 diabetes. Observational stud-
ies indicate that the risk of malformations
increases continuously with increasing
maternal glycemia during the rst 68
weeks of gestation, as dened by rst-
trimester A1Cconcentrations. There is no
threshold for A1C values below which
risk disappears entirely. However, mal-
formation rates above the 12% back-
ground rate of nondiabetic pregnancies
appear to be limited to pregnancies in
which rst-trimester A1C concentrations
are 1% above the normal range for a
nondiabetic pregnant woman.
Preconception care of diabetes ap-
pears to reduce the risk of congenital mal-
formations. Five nonrandomized studies
compared rates of major malformations in
infants between women who participated
in preconception diabetes care programs
and women who initiated intensive diabe-
tes management after they were already
pregnant. The preconception care pro-
grams were multidisciplinary and de-
signed to train patients in diabetes self-
management with diet, intensied insulin
therapy, and SMBG. Goals were set to
achieve normal blood glucose concentra-
tions, and 80% of subjects achieved
normal A1C concentrations before they
became pregnant (335339). In all ve
studies, the incidence of major congenital
malformations in women who partici-
pated in preconception care (range 1.0
1.7%of infants) was much lower than the
incidence in women who did not partici-
pate (range 1.410.9% of infants). One
limitation of these studies is that partici-
pation in preconception care was self-
selected rather than randomized. Thus, it
is impossible to be certain that the lower
malformation rates resulted fully from
improved diabetes care. Nonetheless, the
evidence supports the concept that mal-
formations can be reduced or prevented
by careful management of diabetes before
pregnancy.
Planned pregnancies greatly facilitate
preconception diabetes care. Unfortu-
nately, nearly two-thirds of pregnancies
in women with diabetes are unplanned,
leading to a persistent excess of malfor-
mations in infants of diabetic mothers. To
minimize the occurrence of these devas-
tating malformations, standard care for all
women with diabetes who have child-
bearing potential, beginning at the onset
of puberty or at diagnosis, should include
1) education about the risk of malforma-
tions associated with unplanned pregnan-
cies and poor metabolic control; and 2)
use of effective contraception at all times,
unless the patient has good metabolic
control and is actively trying to conceive.
Women contemplating pregnancy
need to be seen frequently by a multidis-
ciplinary team experienced in the man-
agement of diabetes before and during
pregnancy. The goals of preconception
care are to 1) involve and empower the
patient in the management of her diabe-
tes, 2) achieve the lowest A1C test results
possible without excessive hypoglycemia,
3) assure effective contraception until sta-
ble and acceptable glycemia is achieved,
and 4) identify, evaluate, and treat long-
term diabetes complications such as reti-
nopathy, nephropathy, neuropathy,
hypertension, and CHD (76).
Among the drugs commonly used in
the treatment of patients with diabetes, a
number may be relatively or absolutely
contraindicated during pregnancy. St-
atins are category X (contraindicated for
use in pregnancy) and should be discon-
tinued before conception, as should ACE
inhibitors (340). ARBs are category C
(risk cannot be ruled out) in the rst tri-
mester but category D (positive evidence
of risk) in later pregnancy and should
generally be discontinued before preg-
nancy. Among the oral antidiabetic
agents, metformin and acarbose are clas-
sied as category B (no evidence of risk in
humans) and all others as category C. Po-
tential risks and benets of oral antidia-
betic agents in the preconception period
must be carefully weighed, recognizing
that data are insufcient to establish the
safety of these agents in pregnancy.
For further discussion of preconcep-
tion care, see the related ADA consensus
statement (76) and position statement
(341) on preexisting diabetes and
pregnancy.
C. Older adults
Recommendations
Older adults who are functional, are

cognitively intact, and have signicant
life expectancy should receive diabetes
care using goals developed for younger
adults. (E)
Glycemic goals for older adults not

meeting the above criteria may be re-
laxed using individual criteria, but hy-
perglycemia leading to symptoms or
risk of acute hyperglycemic complica-
tions should be avoided in all patients.
(E)
Other cardiovascular risk factors

should be treated in older adults with
consideration of the time frame of ben-
et and the individual patient. Treat-
ment of hypertension is indicated in
virtually all older adults, and lipid and
aspirin therapy may benet those with
life expectancy at least equal to the time
frame of primary or secondary preven-
tion trials. (E)
Screening for diabetes complications

should be individualized in older
adults, but particular attention should
be paid to complications that would
lead to functional impairment. (E)
Diabetes is an important health condition
for the aging population; at least 20% of
patients over the age of 65 years have di-
abetes, and this number can be expected
to grow rapidly in the coming decades.
Older individuals with diabetes have
higher rates of premature death, func-
tional disability, and coexisting illnesses
such as hypertension, CHD, and stroke
than those without diabetes. Older adults
with diabetes are also at greater risk than
other older adults for several common ge-
riatric syndromes, such as polypharmacy,
depression, cognitive impairment, uri-
nary incontinence, injurious falls, and
persistent pain.
The American Geriatric Societys
guidelines for improving the care of the
older person with diabetes (342) have in-
uenced the following discussion and
recommendations. The care of older
adults with diabetes is complicated by
their clinical and functional heterogene-
ity. Some older individuals developed di-
abetes years earlier and may have
signicant complications; others who are
newly diagnosed may have had years of
undiagnosed diabetes with resultant com-
plications or may have few complications
from the disease. Some older adults with
diabetes are frail and have other underly-
ing chronic conditions, substantial diabe-
tes-related comorbidity, or limited
physical or cognitive functioning. Other
older individuals with diabetes have little
comorbidity and are active. Life expectan-
cies are highly variable for this population
but often longer than clinicians realize.
Providers caring for older adults with di-
abetes must take this heterogeneity into
consideration when setting and prioritiz-
ing treatment goals.
There are few long-term studies in
older adults that demonstrate the benets
of intensive glycemic, blood pressure, and
lipid control. Patients who can be ex-
pected to live long enough to reap the
benets of long-term intensive diabetes
management and who are active, have
good cognitive function, and are willing
should be provided with the needed edu-
cation and skills to do so and be treated
using the goals for younger adults with
diabetes.
For patients with advanced diabetes
complications, life-limiting comorbid ill-
ness, or substantial cognitive or func-
tional impairment, it is reasonable to set
less-intensive glycemic target goals. These
patients are less likely to benet from re-
ducing the risk of microvascular compli-
cations and more likely to suffer serious
adverse effects from hypoglycemia. How-
ever, patients with poorly controlled
diabetes may be subject to acute compli-
cations of diabetes, including dehydra-
t i on, poor wound heal i ng, and
hyperglycemic hyperosmolar coma. Gly-
cemic goals at a minimum should avoid
these consequences.
Although control of hyperglycemia
may be important in older individuals
with diabetes, greater reductions in mor-
bidity and mortality may result from con-
trol of other cardiovascular risk factors
rather than from tight glycemic control
alone. There is strong evidence from clin-
ical trials of the value of treating hyper-
tension in the elderly (343,344). There is
less evidence for lipid-lowering and aspi-
rin therapy, although the benets of these
interventions for primary and secondary
prevention are likely to apply to older
adults whose life expectancies equal or
exceed the time frames seen in clinical
trials.
Special care is required in prescribing
and monitoring pharmacologic therapy in
older adults. Metformin is often contrain-
dicated because of renal insufciency or
signicant heart failure. TZDs can cause
uid retention, which may exacerbate or
lead to heart failure. They are contraindi-
cated in patients with CHF (New York
Heart Association class III and IV), and if
used at all should be used very cautiously
in those with, or at risk for, milder degrees
of CHF. Sulfonylureas, other insulin
secretagogues, and insulin can cause hy-
poglycemia. Insulin use requires that pa-
tients or caregivers have good visual and
motor skills and cognitive ability. Drugs
should be started at the lowest dose and
titrated up gradually until targets are
reached or side effects develop.
Screening for diabetes complications
in older adults also should be individual-
ized. Particular attention should be paid
to complications that can develop over
short periods of time and/or that would
signicantly impair functional status,
such as vision and lower-extremity
complications.
D. Cystic brosisrelated diabetes
Cystic brosis-related diabetes (CFRD) is
the most common comorbidity in people
with cystic brosis, occurring in 20%of
adolescents and 4050% of adults. The
additional diagnosis of diabetes in this
population is associated with worse nutri-
tional status, more severe inammatory
lung disease, and greater mortality from
respiratory failure. For reasons that are
not well understood, women with CFRD
are particularly vulnerable to excess mor-
bidity and mortality. Insulin insufciency
related to partial brotic destruction of
the islet mass is the primary defect in
CFRD. Genetically determined function
of the remaining -cells and insulin resis-
tance associated with infection and in-
ammati on may al so pl ay a rol e.
Encouraging new data suggest that early
detection and aggressive insulin therapy
have narrowed the gap in mortality be-
tween cystic brosis patients with and
without diabetes and have eliminated the
sex difference in mortality.
A consensus conference on CFRD
was cosponsored in 2009 by ADA, the
Cystic Fibrosis Foundation, and the Law-
son Wilkins Pediatric Endocrine Society.
Recommendations for the clinical man-
agement of CFRD will be found in the
consensus report to be published in 2010.
VIII. DIABETES CARE IN
SPECIFIC SETTINGS
Diabetes care in the hospital
Recommendations
All patients with diabetes admitted to

the hospital should have their diabetes
clearly identied in the medical record.
(E)
All patients with diabetes should have

an order for blood glucose monitoring,
with results available to all members of
the health care team. (E)
Goals for blood glucose levels
Critically ill patients: Insulin therapy

should be initiated for treatment of
persistent hyperglycemia starting at a
threshold of 180 mg/dl (10 mmol/
l). Once insulin therapy is started, a
glucose range of 140180 mg/dl
(7.810 mmol/l) is recommended
for the majority of critically ill pa-
tients. (A) These patients require an
intravenous insulin protocol that has
demonstrated efcacy and safety in
achieving the desired glucose range
without increasing risk for severe hy-
poglycemia. (E)
Noncritically ill patients: There is

no clear evidence for specic blood
glucose goals. If treated with insulin,
the premeal blood glucose target
should generally be 140 mg/dl (7.8
mmol/l) with random blood glucose
180 mg/dl (10.0 mmol/l), provided
these targets can be safely achieved.
More stringent targets may be appro-
priate in stable patients with previous
tight glycemic control. Less stringent
targets may be appropriate in those
with severe comorbidites. (E)
Scheduled subcutaneous insulin with

basal, nutritional, and correction com-
ponents is the preferred method for
achieving and maintaining glucose
control in noncritically ill patients. (C)
Using correction dose or supplemen-
tal insulin to correct premeal hyper-
glycemia in addition to scheduled
prandial and basal insulin is recom-
mended. (E)
Glucose monitoring should be initiated

in any patient not known to be diabetic
who receives therapy associated with
high risk for hyperglycemia, including
high-dose glucocorticoid therapy, initi-
ation of enteral or parenteral nutrition,
or other medications such as octreotide
Position Statement
or immunosuppressive medications.
(B) If hyperglycemia is documented
and persistent, treatment is necessary.
Such patients should be treated to the
same glycemic goals as patients with
known diabetes. (E)
A plan for treating hypoglycemia

should be established for each patient.
Episodes of hypoglycemia in the hospi-
tal should be tracked. (E)
All patients with diabetes admitted to

the hospital should have an A1C ob-
tained if the result of testing in the pre-
vious 23 months is not available. (E)
Patients with hyperglycemia in the hos-

pital who do not have a diagnosis of
diabetes should have appropriate plans
for follow-up testing and care docu-
mented at discharge. (E)
The subject of diabetes in the hospital is
extensively reviewed in an ADA technical
review(345). Arecent updated consensus
statement by the American Association of
Clinical Endocrinologists (AACE) and the
ADA (346) form the basis for the discus-
sion and guidelines in this section.
The literature on hospitalized pa-
tients with hyperglycemia typically de-
scribes three categories:
Medical history of diabetes: diabetes pre-

viously diagnosed and acknowledged by
the patients treating physician.
Unrecognized diabetes: hyperglycemia

(fasting blood glucose 126 mg/dl or
random blood glucose 200 mg/dl)
occurring during hospitalization and
conrmed as diabetes after hospitaliza-
tion by standard diagnostic criteria but
unrecognized as diabetes by the treat-
ing physician during hospitalization.
Hospital-related hyperglycemia: hyper-

glycemia (fasting blood glucose 126
mg/dl or random blood glucose 200
mg/dl) occurring during the hospital-
ization that reverts to normal after hos-
pital discharge.
The management of hyperglycemia in the
hospital has logically been considered
secondary in importance to the condition
that prompted admission (345). How-
ever, a body of literature now supports
targeted glucose control in the hospital
setting for potential improved clinical
outcomes. Hyperglycemia in the hospital
may result from stress; decompensation
of type 1, type 2, or other forms of dia-
betes; and/or may be iatrogenic due to
wi thhol di ng of anti hypergl ycemi c
medications or administration of hyper-
glycemia-provoking agents such as glu-
cocorticoids or vasopressors.
People with diabetes are more likely
to be hospitalized and to have longer
lengths of stay than those without diabe-
tes. A recent survey estimated that 22%of
all hospital inpatient days were incurred
by people with diabetes and that hospital
inpatient care accounted for one-half of
the $174 billion total U.S. medical expen-
ditures for this disease (347). This is due,
in part, to the continued expansion of the
worldwide epidemic of type 2 diabetes. In
the U.S. alone, there are 1.6 million new
cases of diabetes each year with an overall
prevalence of 23.6 million people (7.8%
of the population, with one-quarter of
cases remaining undiagnosed). An addi-
tional 57 million American adults are at
high risk for type 2 diabetes (348). While
the costs of illness-related stress hypergly-
cemia are not known, they are likely to be
signicant given the poor prognosis of
such patients (349352).
There is substantial observational ev-
idence linking hyperglycemia in hospital-
ized patients (with or without diabetes) to
poor outcomes. Cohort studies as well as
a few early randomized controlled trials
(RCTs) suggested that intensive treatment
of hyperglycemia improved hospital out-
comes (345,351,352). Interventions to
normalize glycemia, however, have had
inconsistent results. Indeed, recent trials
in critically ill patients have failed to show
a signicant improvement in mortality
wi t h i nt ens i ve gl ycemi c cont r ol
(353,354) or have even shown increased
mortality risk (355). Moreover, these re-
cent RCTs have highlighted the risk of se-
vere hypoglycemia resulting from such
efforts (353358).
The largest study to date, NICE-
SUGAR, a multicenter, multinational
RCT, tested the effect of tight glycemic
control (target 81108 mg/dl) on out-
comes among 6,104 critically ill partici-
pants, the majority of whom (95%)
required mechanical ventilation (355).
Ninety-day mortality was signicantly
higher in the intensive versus the conven-
tional group (target 144180 mg/dl) (78
more deaths; 27.5 vs. 24.9%, P 0.02) in
both surgical and medical patients. Mor-
tality from cardiovascular causes was
more common in the intensive group (76
more deaths; 41.6 vs. 35.8%; P 0.02).
Severe hypoglycemia was also more com-
mon in the intensively treated group (6.8
vs. 0.5%; P 0.001). The precise reason
for the increased mortality in the tightly
controlled group is unknown. The results
of this study lie in stark contrast to a fa-
mous 2001 single-center study that re-
ported a 42% relative reduction in
intensive care unit (ICU) mortality in crit-
ically ill surgical patients treated to a tar-
get blood glucose of 80110 mg/dl.
Importantly, the control group in NICE-
SUGAR had reasonably good blood glu-
cose management, maintained at a mean
glucose of 144 mg/dl, only 29 mg/dl
above the intensively managed patients.
Accordingly, this studys ndings do not
disprove the notion that glycemic control
in the ICUis important. However, they do
strongly suggest that it is not necessary to
target blood glucose values 140 mg/dl
and that a highly stringent target of 110
mg/dl actually may be dangerous.
In a recent meta-analysis of 26 trials
(N 13,567), which included the NICE-
SUGAR data, the pooled relative risk (RR)
of death with intensive insulin therapy
was 0.93 as compared with conventional
therapy (95% CI 0.831.04) (358). Ap-
proximately half of these trials reported
hypoglycemia, with a pooled RR of inten-
sive therapy of 6.0 (95%CI 4.58.0). The
specic ICU setting inuenced the nd-
ings, with patients in surgical ICUs ap-
pearing to benet from intensive insulin
therapy (RR 0.63 [95% CI 0.440.91]),
while those in other critical care settings
did not (medical ICU: 1.0 [0.781.28];
mixed ICU: 0.99 [0.861.12]). It was
concluded that overall, intensive insulin
therapy increased the risk of hypoglyce-
mia but provided no overall benet on
mortality in the critically ill, although a
benet to patients admitted to the surgical
ICU was suggested.
It is very clear that the management of
hyperglycemia in the hospital presents
unique challenges that stem from varia-
tions in a patients nutritional status and
level of consciousness, the practical limi-
tations of intermittent glycemic monitor-
ing, and the ultimate importance of
patient safety. Accordingly, reasonable
glucose targets in the hospital setting are
modestly higher than may be routinely
advised in patients with diabetes in the
outpatient setting. The following recom-
mendations represent a synthesis of the
evidence base over the past decade and
are somewhat less stringent than prior
recommendations of the ADA Standards
of Medical Care in Diabetes. For a com-
prehensive review of these data, the
reader is referred to the latest consensus
statement from AACE and ADA on inpa-
tient management of hyperglycemia
(346).
1. Glycemic targets in hospitalized
patients
a. Denition of glucose abnormalities in
the hospital setting. Hyperglycemia has
been dened as any blood glucose 140
mg/dl (7.8 mmol/l). Levels that are signif-
icantly and persistently above this may re-
quire treatment in hospitalized patients.
In patients without a previous diagnosis
of diabetes, elevated blood glucose may
be due to stress hyperglycemia, a condi-
tion that can be established by a review of
prior records or measurement of an A1C.
A1C values 6.5% suggest that diabetes
preceded hospitalization (359). Hypogly-
cemia has been dened as any blood glu-
cose 70 mg/dl (3.9 mmol/l). This is the
standard denition in outpatients and
correlates with the initial threshold for the
release of counterregulatory hormones
(177). Severe hypoglycemia in hospital-
ized patients has been dened by many
as 40 mg/dl (2.2 mmol/l), although
this is lower than the 50 mg/dl (2.8
mmol/l) level at which cognitive impair-
ment begins in normal individuals
(177,360,361). As with hyperglycemia,
hypoglycemia among inpatients is also as-
sociated with adverse short- and long-
term outcomes. Early recognition and
treatment of mild to moderate hypoglyce-
mia (40 and 69 mg/dl [2.2 and 3.8 mmol/
l]) can prevent deterioration to a more
severe episode with potential adverse se-
quelae (361,362).
i. Critically ill patients. Based on the
weight of the available evidence, for the
majority of critically ill patients in the ICU
setting, insulin infusion should be used to
control hyperglycemia, with a starting
threshold of 180 mg/dl (10.0 mmol/l).
Once intravenous insulin is started, the
glucose level should be maintained be-
tween 140 and 180 mg/dl (7.8 and 10.0
mmol/l). Greater benet may be realized
at the lower end of this range. Although
strong evidence is lacking, somewhat
lower glucose targets may be appropriate
in selected patients. However, targets
110 mg/dl (6.1 mmol/l) are not recom-
mended. Use of insulin infusion protocols
with demonstrated safety and efcacy, re-
sulting in low rates of hypoglycemia, are
highly recommended.
ii. Noncritically ill patients. With no pro-
spective, RCT data to inform specic gly-
cemic targets in noncritically ill patients,
recommendations are based on clinical
experience and judgment. For the major-
ity of noncritically ill patients treated with
insulin, premeal glucose targets should
generally be 140 mg/dl (7.8 mmol/l)
with random blood glucose 180 mg/dl
(10.0 mmol/l), as long as these targets can
be safely achieved. To avoid hypoglyce-
mia, consideration should be given to re-
assessing the insulin regimen if blood
glucose levels fall below 100 mg/dl (5.6
mmol/l). Modication of the regimen is
required when blood glucose values are
70 mg/dl (3.9 mmol/l), unless the event
is easily explained by other factors (such
as a missed meal, etc.).
Occasional patients with a prior his-
tory of successful tight glycemic control in
the outpatient setting who are clinically
stable may be maintained with a glucose
range below the above cut points. Con-
versely, higher glucose ranges may be ac-
ceptable in terminally ill patients or in
patients with severe comorbidities, as
well as in those in patient-care settings
where frequent glucose monitoring or
close nursing supervision is not feasible.
Clinical judgment, combined with
ongoing assessment of the patients clini-
cal status, including changes in the trajec-
tory of glucose measures, severity of
illness, nutritional status, or concurrent
use of medications that might affect glu-
cose levels (e.g., steroids, octreotide)
must be incorporated into the day-to-day
decisions regarding insulin dosing (363).
2. Treatment options in hospitalized
patients
In the hospital setting, insulin therapy is
the preferred method of glycemic control
in majority of clinical situations (346). In
the ICU, intravenous infusion is the pre-
ferred route of insulin administration.
Outside of critical care units, subcutane-
ous insulin is used much more frequently.
Oral agents have a limited role in the in-
patient setting.
a. Intravenous insulin infusions. In the
critical care setting, continuous intrave-
nous insulin infusion has been shown to
be the most effective method for achiev-
ing specic glycemic targets (346). Be-
cause of the very short half-life of
circulating insulin, intravenous delivery
allows rapid dosing adjustments to ad-
dress alterations in patients status.
Intravenous insulin is ideally admin-
istered via validated written or computer-
ized protocols that allow for predened
adjustments to the insulin infusion rate
according to glycemic uctuations and in-
sulin dose. An extensive review of the
merits and deciencies of published pro-
tocols is beyond the intent of this state-
ment, and the reader is referred to several
available reports and reviews (364366).
Continued education of staff with peri-
odic ongoing review of patient data are
critical for successful implementation of
any insulin protocol (364366).
Patients who receive intravenous in-
sulin infusion will usually require transi-
tion to subcutaneous insulin when they
begin eating regular meals or are trans-
ferred to lower intensity care. Typically, a
percentage (usually 7580%) of the total
daily intravenous infusion dose is propor-
tionately divided into basal and prandial
components (see below). Importantly,
subcutaneous insulin must be given 14
h prior to discontinuation of intravenous
insulin to prevent hyperglycemia (367).
b. Subcutaneous insulin. Scheduled
subcutaneous insulin is the preferred
method for achieving and maintaining
glucose control in non-ICU patients with
diabetes or stress hyperglycemia. The rec-
ommended components of inpatient sub-
cutaneous insulin regimens include a
basal, nutritional, and supplemental (cor-
rection) component (345,346,368). Each
component can be met by one of several
available insulin products, depending on
the particular hospital situation. The
reader is referred to several recent publi-
cations and reviews that describe cur-
rently available insulin preparations and
protocols (366370).
A topic that deserves particular atten-
tion is the persistent overuse of what has
been branded as sliding scale insulin (SSI)
for management of hyperglycemia. The
term correction insulin, which refers to
the use of additional short or rapid-acting
insulin with scheduled insulin doses to
treat blood glucose above desired targets,
is preferred (345). Prolonged therapy
with SSI as the sole regimen is ineffective
in the majority of patients (and potentially
dangerous in type 1 diabetes) (370375).
c. Noninsulin agents. These agents are
inappropriate in the majority of hospital-
ized patients because they are less titrat-
able than insulin in the short tem and are
meant to be used in patients eating on a
regular meal schedule. Continuation of
these agents may be appropriate in se-
lected stable patients who are expected to
consume meals at regular intervals. Spe-
cic caution is required with metformin,
due to the possibility that a contraindica-
tion may develop during the hospitaliza-
tion, such as renal insufciency, unstable
hemodynamic status, or need for an im-
aging study that requires a radio-contrast
dye (345,376). Injectable noninsulin
therapies such as exenatide and pramlint-
Position Statement
ide have limitations similar to those of
oral agents in the hospital setting.
d. Specic clinical situations
i. Insulin pumps. Patients who use CSII
pump therapy in the outpatient setting
can be candidates for diabetes self-
management in the hospital, provided
that they have the mental and physical
capacity to do so (346,368). It is impor-
tant that nursing personnel document
basal rates and bolus doses on a regular
basis (at least daily). The availability of
hospital personnel with expertise in CSII
therapy is essential.
ii. Enteral nutrition. Hyperglycemia is a
common side effect of inpatient enteral
nutrition therapy (377). A recent report
using a combination of basal insulin with
correction insulin achieved a mean glu-
cose value of 160 mg/dl (8.9 mmol/l).
Similar results were achieved in the group
randomized to receive SSI alone; how-
ever, 48% of patients required the addi-
tion of intermediate-acting insulin to
achieve glycemic targets (373).
iii. Parenteral nutrition. The high glu-
cose load in standard parenteral nutrition
frequently results in hyperglycemia,
which is associated with a higher inci-
dence of complications and mortality in
critically ill ICU patients (378). Insulin
therapy is highly recommended, with glu-
cose targets as dened previously by se-
verity of illness.
iv. Glucocorticoid therapy. Hyperglyce-
mia is a common complication of cortico-
steroid therapy (363). Several approaches
have been proposed for treatment of this
condition, but there are no published
protocols or studies that investigate the
efcacy of these approaches. A reasonable
approach is to institute glucose monitor-
ing for at least 48 h in all patients receiv-
ing high dose glucocorticoid therapy and
initiate insulin as appropriate. In patients
who are already being treated for hyper-
glycemia, early adjustment of insulin
doses is recommended. Importantly, dur-
ing steroid tapers, insulin dosing should
be proact i vel y adj ust ed t o avoi d
hypoglycemia.
v. Hypoglycemia prevention. Hypogly-
cemia, especially in insulin-treated pa-
tients, is the leading limiting factor in the
glycemic management of type 1 and type
2 diabetes (174). In the hospital, multiple
additional risk factors for hypoglycemia
are present, even among patients who are
neither brittle nor tightly controlled. Pa-
tients with or without diabetes may expe-
rience hypoglycemia in the hospital in
association with altered nutritional state,
heart failure, renal or liver disease, malig-
nancy, infection, or sepsis (379,379,380).
Additional triggering events leading to
iatrogenic hypoglycemia include sudden
reduction of corticosteroid dose, altered
ability of the patient to self-report symp-
toms, reduction of oral intake, emesis,
new NPO status, inappropriate timing of
short- or rapid-acting insulin in relation
to meals, reduction of rate of administra-
tion of intravenous dextrose, and unex-
pected interruption of enteral feedings or
parenteral nutrition.
Despite the preventable nature of
many inpatient episodes of hypoglyce-
mia, institutions are more likely to have
nursing protocols for the treatment of hy-
poglycemia than for its prevention.
Tracking such episodes and analyzing
their causes are important quality im-
provement activities.
3. Diabetes care providers in the
hospital
Inpatient diabetes management may be
effectively provided by primary care phy-
sicians, endocrinologists, or hospitalists.
Involvement of appropriately trained spe-
cialists or specialty teams may reduce
length of stay, improve glycemic control,
and improve outcomes (381384). In the
care of diabetes, implementation of stan-
dardized order sets for scheduled and cor-
rection-dose insulin may reduce reliance
on sliding-scale management. A team ap-
proach is needed to establish hospital
pathways. To achieve glycemic targets
associated with improved hospital out-
comes, hospitals will need multidisci-
plinary support to develop protocols for
subcutaneous insulin therapy that effec-
tively and safely achieve glycemic targets
(385).
4. Self-management in the hospital
Self-management of diabetes in the hos-
pital may be appropriate for competent
adult patients who have a stable level of
consciousness, have reasonably stable
daily insulin requirements, successfully
conduct self-management of diabetes at
home, have physical skills needed to suc-
cessfully self-administer insulin and per-
form SMBG, have adequate oral intake,
and are procient in carbohydrate count-
ing, use of multiple daily insulin injec-
tions, or insulin pump therapy and sick-
day management. The patient and
physician, in consultation with nursing
staff, must agree that patient self-
management is appropriate under the
conditions of hospitalization. For patients
conducting self-management in the hos-
pital, it is imperative that basal, prandial,
and correction doses of insulin and results
of bedside glucose monitoring be re-
corded as part of the patients hospital
medical record. While many institutions
allow patients on insulin pumps to con-
tinue these devices in the hospital, others
express concern regarding use of a device
unfamiliar to staff, particularly in patients
who are not able to manage their own
pump therapy. If a patient is too ill to
self-manage either multiple daily injec-
tions or CSII, then appropriate subcuta-
neous doses can be calculated on the basis
of their basal and bolus insulin needs dur-
ing hospitalization, with adjustments for
changes in nutritional or metabolic status.
5. DSME in the hospital
Teaching diabetes self-management to
patients in hospitals is a challenging task.
Patients are ill, under increased stress re-
lated to their hospitalization and diagno-
sis, and in an environment not conducive
to learning. Ideally, people with diabetes
should be taught at a time and place con-
ducive to learningas an outpatient in
a recognized program of diabetes
education.
For the hospitalized patient, diabetes
survival skills education is generally a
feasible approach. Patients and/or family
members receive sufcient information
and training to enable safe care at home.
Those newly diagnosed with diabetes or
who are new to insulin and/or blood glu-
cose monitoring need to be instructed
before discharge. Those patients hospital-
ized because of a crisis related to diabetes
management or poor care at home need
education to prevent subsequent episodes
of hospitalization. An assessment of the
need for a home health referral or referral
to an outpatient diabetes education pro-
gram should be part of discharge plan-
ning for all patients.
6. MNT in the hospital
Hospital diets continue to be ordered by
calorie levels based on the ADA diet.
However, since 1994 the ADA has not en-
dorsed any single meal plan or specied
percentages of macronutrients, and the
term ADA diet should no longer be
used. Current nutrition recommenda-
tions advise individualization based on
treatment goals, physiologic parameters,
and medication usage. Because of the
complexity of nutrition issues in the hos-
pital, a registered dietitian, knowledge-
able and skilled in MNT, should serve as
an inpatient team member. The dietitian
is responsible for integrating information
about the patients clinical condition, eat-
ing, and lifestyle habits and for establish-
ing treatment goals in order to determine
a realistic plan for nutrition therapy
(386,387).
7. Bedside blood glucose monitoring
Bedside blood glucose monitoring using
point-of-care glucose meters is performed
before meals and bedtime in the majority
of inpatients who are eating usual meals.
In patients who are receiving continuous
enteral or parenteral nutrition, glucose
monitoring is optimally performed every
46 h. In patients who are receiving cy-
cled enteral or parenteral nutrition, the
schedule for glucose monitoring can be
individualized but should be frequent
enough to detect hyperglycemia during
feedings and risk of hypoglycemia when
feedings are interrupted (374,376). More
frequent bloodglucose testing ranging from
every 30 min to every 2 h is required for
patients on intravenous insulin infusions.
Safe and rational glycemic manage-
ment relies on the accuracy of blood glu-
cose measurements using point-of-care
blood glucose meters, which have several
important limitations. Although the FDA
allows a 20% error for glucose meters,
questions about the appropriateness of
this criterion have been raised (388). Glu-
cose measures differ signicantly between
plasma and whole blood, terms which are
often used interchangeably and can lead
to misinterpretation. Most commercially
available capillary glucose meters intro-
duce a correction factor of 1.12 to re-
port a plasma-adjusted value (389).
Signicant discrepancies between
capillary, venous, and arterial plasma
samples have been observed in patients
with low or high hemoglobin concentra-
tions, hypoperfusion, and the presence of
interfering substances (389,390). Analyt-
ical variability has been described with
several point-of-care meters (391). Any
glucose result that does not correlate with
the patients status should be conrmed
through conventional laboratory sam-
pling of PG.
While laboratory measurement of PG
has less variability and interference, mul-
tiple daily phlebotomies are not practical.
The use of indwelling lines as the sam-
pling source also poses risks for infection.
Studies performed using continuous in-
terstitial glucose monitoring systems in
the critical care setting (392) currently are
limited by the lack of reliability in the hy-
poglycemic range as well as by cost.
8. Discharge planning
It is important to anticipate the postdis-
charge antihyperglycemic regimen in all
patients with diabetes or newly discov-
ered hyperglycemia. The optimal pro-
gram will need to consider the type and
severity of diabetes, the effects of the
patients illness on blood glucose levels,
and the capacities and desires of the pa-
tient. Smooth transition to outpatient
care should be ensured, especially in
those new to insulin therapy or in
whom the diabetes regimen has been
substantially altered during the hospi-
talization. All patients in whom the di-
agnosis of diabetes is new should have,
at minimum, survival skills training
prior to discharge.
It is recommended that the following
areas be reviewed and addressed prior to
hospital discharge:
level of understanding related to the di-

agnosis of diabetes
SMBG and explanation of home blood

glucose goals
denition, recognition, treatment, and

prevention of hyperglycemia and
hypoglycemia
identication of health care provider

who will provide diabetes care after
discharge
information on consistent eating

patterns
when and how to take blood glucose

lowering medications including insulin
administration (if going home on
insulin)
sick-day management
proper use and disposal of needles and

syringes
More expanded diabetes education can
be arranged in the community. An out-
patient follow-up visit with the primary
care provider, endocrinologist, or diabe-
tes educator within 1 month of discharge
is advised for all patients having hypergly-
cemia in the hospital. Clear communica-
tion with outpatient providers either
directly or via hospital discharge summa-
ries facilitates safe transitions to outpa-
ti ent care. Provi di ng i nf ormati on
regarding the cause or the plan for deter-
mining the cause of hyperglycemia, re-
lated complications and comorbidities,
and recommended treatments can assist
outpatient providers as they assume on-
going care.
IX. STRATEGIES FOR
IMPROVING DIABETES
CARE The implementation of the
standards of care for diabetes has been
suboptimal in most clinical settings. A re-
cent report (393) indicated that only
57.1% of adults with diagnosed diabetes
achieved an A1C of 7%, only 45.5%
had a blood pressure 130/80 mmHg,
and just 46.5% had a total cholesterol
200 mg/dl. Most distressing was that
only 12.2% of people with diabetes
achieved all three treatment goals.
While numerous interventions to im-
prove adherence to the recommended
standards have been implemented, the
challenge of providing uniformly effective
diabetes care has thus far deed a simple
solution. A major contributor to subopti-
mal care is a delivery systemthat too often
is fragmented, lacks clinical information
capabilities, often duplicates services, and
is poorly designed for the delivery of
chronic care. The chronic care model
(CCM) includes ve core elements for the
provision of optimal care of patients with
chronic disease: delivery system design,
self-management support, decision sup-
port, clinical information systems, and
community resources and policies. Redef-
inition of the roles of the clinic staff and
promoting self-management on the part
of the patient are fundamental to the suc-
cessful implementation of the CCM
(394). Collaborative, multidisciplinary
teams are best suited to provide such care
for people with chronic conditions like
diabetes and to empower patients perfor-
mance of appropriate self-management.
Alterations in reimbursement that reward
the provision of quality care, as dened by
the attainment of quality measures devel-
oped by such programs as the ADA/
Nat i onal Commi t t ee f or Qual i t y
Assurance Diabetes Provider Recognition
Program, will also be required to achieve
desired outcome goals.
In recent years, numerous health care
organizations, ranging from large health
care systems such as the U.S. Veterans
Administration to small private practices,
have implemented strategies to improve
diabetes care. Successful programs have
published results showing improvement
in process measures such as measurement
of A1C, lipids, and blood pressure. Effects
on in important intermediate outcomes,
such as mean A1C for populations, have
been more difcult to demonstrate (395
397), although examples do exist (398
402), often taking more than 1 year to
manifest (394). Features of successful
Position Statement
programs reported in the literature
include
Delivery of DSME: increases adherence

to standard of care and educating pa-
tients on glycemic targets and improves
the percentage of patients who reach
goal A1C (142,403)
Adoption of practice guidelines, with

participation of health care profession-
als in the process of development:
Guidelines should be readily accessible
at the point of service, preferably as
computerized reminders at the point of
care. Guidelines should begin with a
summary of their major recommenda-
tions instructing health care profes-
sionals what to do and how to do it.
Use of checklists that mirror guidelines:

successful at improving adherence to
standards of care
Systems changes: such as provision of

automated reminders to health care
professionals and patients and audit
and feedback of process and outcome
data to providers
Quality improvement programs com-

bining continuous quality improve-
ment or other cycles of analysis and
intervention with provider perfor-
mance data
Practice changes: such as availability of

point of care testing of A1C, scheduling
planned diabetes visits, clustering of
dedicated diabetes visits into specic
times within a primary care practice
schedule, or group visits and/or visits
with multiple health care professionals
on a single day
Tracking systems with either an elec-

tronic medical record or patient regis-
try: helpful at increasing adherence to
standards of care by prospectively iden-
tifying those requiring assessments
and/or treatment modications. They
likely could have greater efcacy if they
suggested specic therapeutic interven-
tions to be considered for a particular
patient at a particular point in time
(404).
Availability of case or (preferably) care

management services (405): Nurses,
pharmacists, and other nonphysician
health care professionals using detailed
algorithms working under the supervi-
sion of physicians have demonstrated
the greatest reduction in A1C and
blood pressure (406,407).
Evidence suggests that these individual
initiatives work best when provided as
components of a multifactorial interven-
tion. When practices are compared, those
that address more of the CCM elements
demonstrate lower A1C levels and lower
cardiovascular risk scores (408). The
most successful practices have an institu-
tional priority for quality of care, involve
all of the staff in their initiatives, redesign
their delivery system, activate and edu-
cate their patients, and use electronic
health record tools (409,410).
NDEP maintains an online resource
(www.betterdiabetescare.nih.gov) to help
health care professionals design and im-
plement more effective health care deliv-
ery systems for those with diabetes.
It is clear that optimal diabetes man-
agement requires an organized, system-
atic approach and involvement of a
coordinated teamof dedicated health care
professionals working in an environment
where quality care is a priority.
References
1. American Diabetes Asociation. Medical
Management of Type 1 Diabetes. Alexan-
dria, VA, American Diabetes Associa-
tion, 2008
2. American Diabetes Asociation. Medical
Management of Type 2 Diabetes. Alexan-
dria, VA, American Diabetes Associa-
tion, 2008
3. American Diabetes Association. Intensive
Diabetes Management. Alexandria, VA,
American Diabetes Association, 2009
4. Expert Committee on the Diagnosis and
Classication of Diabetes Mellitus. Re-
port of the Expert Committee on the Di-
agnosis and Classication of Diabetes
Mellitus. Diabetes Care 1997;20:1183
1197
5. International Expert Committee. Inter-
national Expert Committee report on the
role of the A1C assay in the diagnosis of
diabetes. Diabetes Care 2009;32:1327
1334
6. American Diabetes Association. Diagno-
sis and classication of diabetes mellitus.
Diabetes Care 2010;33(Suppl. 1):S62
S69
7. Genuth S, Alberti KG, Bennett P, Buse J,
Defronzo R, Kahn R, Kitzmiller J,
Knowler WC, Lebovitz H, Lernmark A,
Nathan D, Palmer J, Rizza R, Saudek C,
ShawJ, Steffes M, Stern M, Tuomilehto J,
Zimmet P, Expert Committee on the Di-
agnosis and Classication of Diabetes
Mellitus. Follow-up report on the diag-
nosis of diabetes mellitus. Diabetes Care
2003;26:31603167
9. Engelgau MM, Narayan KM, Herman
WH. Screening for type 2 diabetes. Dia-
betes Care 2000;23:15631580
10. Gabir MM, Hanson RL, Dabelea D, Im-
peratore G, Roumain J, Bennett PH,
Knowler WC. The 1997 American Dia-
betes Association and 1999 World
Health Organization criteria for hyper-
glycemia in the diagnosis and prediction
of diabetes. Diabetes Care 2000;23:
11081112
11. Knowler WC, Barrett-Connor E, Fowler
SE, Hamman RF, Lachin JM, Walker EA,
Nathan DM, Diabetes Prevention Pro-
gram Research Group. Reduction in the
incidence of type 2 diabetes with lifestyle
intervention or metformin. NEngl J Med
2002;346:393403
12. Tuomilehto J, Lindstro m J, Eriksson JG,
Valle TT, Ha ma la inen H, Ilanne-Parikka
P, Keina nen-Kiukaanniemi S, Laakso M,
Louheranta A, Rastas M, Salminen V,
Uusitupa M, Finnish Diabetes Preven-
tion Study Group. Prevention of type 2
diabetes mellitus by changes in lifestyle
among subjects with impaired glucose
tolerance. N Engl J Med 2001;344:
13431350
13. Pan XR, Li GW, Hu YH, Wang JX, Yang
WY, An ZX, Hu ZX, Lin J, Xiao JZ, Cao
HB, Liu PA, Jiang XG, Jiang YY, Wang JP,
Zheng H, Zhang H, Bennett PH, Howard
BV. Effects of diet and exercise in pre-
venting NIDDMin people with impaired
glucose tolerance. The Da Qing IGT and
Diabetes Study. Diabetes Care 1997;20:
537544
14. Buchanan TA, Xiang AH, Peters RK, Kjos
SL, Marroquin A, Goico J, Ochoa C, Tan
S, Berkowitz K, Hodis HN, Azen SP.
Preservation of pancreatic beta-cell
function and prevention of type 2 diabe-
tes by pharmacological treatment of in-
sulin resistance in high-risk hispanic
women. Diabetes 2002;51:27962803
15. Chiasson JL, Josse RG, Gomis R,
Hanefeld M, Karasik A, Laakso M,
STOP-NIDDM Trail Research Group.
Acarbose for prevention of type 2 diabe-
tes mellitus: the STOP-NIDDMrandom-
ised trial. Lancet 2002;359:20722077
16. DREAM (Diabetes REduction Assess-
ment with ramipril and rosiglitazone
Medication) Trial Investigators, Gerstein
HC, Yusuf S, Bosch J, Pogue J, Sheridan
P, Dinccag N, Hanefeld M, Hoogwerf B,
Laakso M, Mohan V, Shaw J, Zinman B,
Holman RR. Effect of rosiglitazone on
the frequency of diabetes in patients
with impaired glucose tolerance or im-
paired fasting glucose: a randomised
controlled trial. Lancet 2006;368:1096
1105
17. Ramachandran A, Snehalatha C, Mary S,
Mukesh B, Bhaskar AD, Vijay V, Indian
Diabetes Prevention Programme (IDPP).
The Indian Diabetes Prevention Pro-
gramme shows that lifestyle modica-
tion and metformin prevent type 2
diabetes in Asian Indian subjects with
impaired glucose tolerance (IDPP-1).
Diabetologia 2006;49:289297
18. Johnson SL, Tabaei BP, Herman WH.
The efcacy and cost of alternative strat-
egies for systematic screening for type 2
diabetes in the U.S. population 4574
years of age. Diabetes Care 2005;28:
307311
19. Harris R, Donahue K, Rathore SS, Frame
P, Woolf SH, Lohr KN. Screening adults
for type 2 diabetes: a review of the evi-
dence for the U.S. Preventive Services
Task Force. Ann Intern Med 2003;138:
215229
20. U.S. Preventive Services Task Force. S.
Preventive Services Task Force. S. Pre-
ventive Services Task Force: Screening
for type 2 diabetes mellitus in adults:
recommendations and rationale. Ann
Intern Med 2003;138:212214
21. Writing Group for the SEARCH for Dia-
betes in Youth Study Group, Dabelea D,
Bell RA, DAgostino RB Jr, Imperatore G,
Johansen JM, Linder B, Liu LL, Loots B,
Marcovina S, Mayer-Davis EJ, Pettitt DJ,
Waitzfelder B. Incidence of diabetes in
youth in the United States. JAMA 2007;
297:27162724
22. SEARCH for Diabetes in Youth Study
Group, Liese AD, DAgostino RB Jr,
Hamman RF, Kilgo PD, Lawrence JM,
Liu LL, Loots B, Linder B, Marcovina S,
Rodriguez B, Standiford D, Williams DE.
The burden of diabetes mellitus among
US youth: prevalence estimates from the
SEARCH for Diabetes in Youth Study.
Pediatrics 2006;118:15101518
23. American Diabetes Association: Type 2
diabetes in children and adolescents
(Consensus Statement). Diabetes Care
2000;23:381389
24. Lawrence JM, Contreras R, Chen W,
Sacks DA. Trends in the prevalence of
preexisting diabetes and gestational dia-
betes mellitus among a racially/ethni-
cally diverse population of pregnant
women, 19992005. Diabetes Care
2008;31:899904
25. American Diabetes Association: Gesta-
tional diabetes mellitus (Position State-
ment). Diabetes Care 2004;27(Suppl.
1):S88S90
26. HAPO Study Cooperative Research
Group, Metzger BE, Lowe LP, Dyer AR,
Trimble ER, Chaovarindr U, Coustan
DR, Hadden DR, McCance DR, Hod M,
McIntyre HD, Oats JJ, Persson B, Rogers
MS, Sacks DA. Hyperglycemia and ad-
verse pregnancy outcomes. NEngl J Med
2008;358:19912002
27. Landon MB, Spong CY, Thom E, Car-
penter MW, Ramin SM, Casey B, Wap-
ner RJ, Varner MW, Rouse DJ, Thorp JM
Jr, Sciscione A, Catalano P, Harper M,
Saade G, Lain KY, Sorokin Y, Peaceman
AM, Tolosa JE, Anderson GB, Eunice
Kennedy Shriver National Institute of
Child Health and Human Development
Maternal-Fetal Medicine Units Network.
A multicenter, randomized trial of treat-
ment for mild gestational diabetes.
N Engl J Med 2009;361:13391348
28. Kim C, Newton KM, Knopp RH. Gesta-
tional diabetes and the incidence of type
2 diabetes: a systematic review. Diabetes
Care 2002;25:18621868
29. Lindstro m J, Ilanne-Parikka P, Peltonen
M, Aunola S, Eriksson JG, Hemio K, Ha -
ma la inen H, Ha rko nen P, Keina nen-
Kiukaanniemi S, Laakso M, Louheranta
A, Mannelin M, Paturi M, Sundvall J,
Valle TT, Uusitupa M, Tuomilehto J,
Finnish Diabetes Prevention Study
Group. Sustained reduction in the inci-
dence of type 2 diabetes by lifestyle in-
tervention: follow-up of the Finnish
Diabetes Prevention Study. Lancet 2006;
368:16731679
30. Li G, Zhang P, Wang J, Gregg EW, Yang
W, Gong Q, Li H, Li H, Jiang Y, An Y,
Shuai Y, Zhang B, Zhang J, Thompson
TJ, Gerzoff RB, Roglic G, Hu Y, Bennett
PH. The long-term effect of lifestyle in-
terventions to prevent diabetes in the
China Da Qing Diabetes Prevention
Study: a 20-year follow-up study. Lancet
2008;371:17831789
31. Kosaka K, Noda M, Kuzuya T. Preven-
tion of type 2 diabetes by lifestyle inter-
vention: a Japanese trial in IGT males.
Diabetes Res Clin Pract 2005;67:152
162
32. Torgerson JS, Hauptman J, Boldrin MN,
Sjo stro mL. XENical in the prevention of
diabetes in obese subjects (XENDOS)
study: a randomized study of orlistat as
an adjunct to lifestyle changes for the
prevention of type 2 diabetes in obese
patients. Diabetes Care 2004;27:155
161
33. Kawamori R, Tajima N, Iwamoto Y,
Kashiwagi A, Shimamoto K, Kaku K,
Voglibose Ph-3 Study Group. Voglib-
ose for prevention of type 2 diabetes
mellitus: a randomised, double-blind
trial in Japanese individuals with im-
paired glucose tolerance. Lancet 2009;
373:16071614
34. DeFronzo RA, for ACT NOW Study
Group. ACTos NOW Study for the Pre-
vention of Diabetes (ACT NOW) Study.
Late-breaking abstract presented at 68th
Annual Scientic Sessions of the Ameri-
can Diabetes Association, 6 June 2008,
San Francisco, CA
35. Gerstein HC. Point: If it is important to
prevent type 2 diabetes, it is important to
consider all proven therapies within a
comprehensive approach. Diabetes Care
2007;30:432434
36. Nathan DM, Davidson MB, DeFronzo
RA, Heine RJ, Henry RR, Pratley R, Zin-
man B, American Diabetes Association.
Impaired fasting glucose and impaired
glucose tolerance: implications for care.
Diabetes Care 2007;30:753759
37. American Diabetes Association: Consen-
sus statement on self-monitoring of
blood glucose. Diabetes Care 1987;10:
9599
38. American Diabetes Association: Self-
monitoring of blood glucose. Diabetes
Care 1994;17:8186
39. Welschen LM, Bloemendal E, Nijpels G,
Dekker JM, Heine RJ, Stalman WA,
Bouter LM. Self-monitoring of blood
glucose in patients with type 2 diabetes
who are not using insulin: a systematic
review. Diabetes Care 2005;28:1510
1517
40. Farmer A, Wade A, Goyder E, Yudkin
P, French D, Craven A, Holman R,
Kinmonth AL, Neil A. Impact of self
monitoring of blood glucose in the man-
agement of patients with non-insulin
treated diabetes: open parallel group
randomised trial. BMJ 2007;335:132
41. OKane MJ, Bunting B, Copeland M,
Coates VE, ESMON study group. Ef-
cacy of self monitoring of blood glucose
in patients with newly diagnosed type 2
diabetes (ESMON study): randomised
controlled trial. BMJ 2008;336:1174
1177
42. Simon J, Gray A, Clarke P, Wade A, Neil
A, Farmer A, Diabetes Glycaemic Educa-
tion and Monitoring Trial Group. Cost
effectiveness of self monitoring of blood
glucose in patients with non-insulin
treated type 2 diabetes: economic evalu-
ation of data from the DiGEM trial. BMJ
2008;336:11771180
43. Sacks DB, Bruns DE, Goldstein DE, Ma-
claren NK, McDonald JM, Parrott M.
Guidelines and recommendations for
laboratory analysis in the diagnosis and
management of diabetes mellitus. Clin
Chem 2002;48:436472
44. Juvenile Diabetes Research Foundation
Continuous Glucose Monitoring Study
Group, Tamborlane WV, Beck RW,
Bode BW, Buckingham B, Chase HP,
Clemons R, Fiallo-Scharer R, Fox LA,
Gilliam LK, Hirsch IB, Huang ES, Koll-
man C, Kowalski AJ, Laffel L, Lawrence
JM, Lee J, Mauras N, OGrady M, Ruedy
KJ, Tansey M, Tsalikian E, Weinzimer S,
Wilson DM, Wolpert H, Wysocki T,
Xing D: Continuous glucose monitoring
and intensive treatment of type 1 diabe-
tes. NEngl J Med 2008; 359:14641476
45. Juvenile Diabetes Research Foundation
Continuous Glucose Monitoring Study
Group: The effect of continuous glucose
monitoring in well-controlled type 1 di-
abetes. Diabetes Care 2009;32:1378
1383
46. Stratton IM, Adler AI, Neil HA, Mat-
thews DR, Manley SE, Cull CA, Hadden
D, Turner RC, Holman RR. Association
of glycaemia with macrovascular and
microvascular complications of type 2
diabetes (UKPDS 35): prospective ob-
servational study. BMJ 2000;321:405
412
47. Cagliero E, Levina EV, Nathan DM. Im-
mediate feedback of HbA1c levels im-
proves glycemic control in type 1 and
Position Statement
insulin-treated type 2 diabetic patients.
48. Miller CD, Barnes CS, Phillips LS, Zi-
emer DC, Gallina DL, Cook CB, Mary-
man SD, El-Kebbi IM. Rapid A1c
availability improves clinical decision-
making in an urban primary care clinic.
49. Nathan DM, Kuenen J, Borg R, Zheng H,
Schoenfeld D, Heine RJ, A1c-Derived
Average Glucose Study Group. Translat-
ing the A1C assay into estimated average
glucose values. Diabetes Care 2008;31:
14731478
50. Rohlng CL, Wiedmeyer HM, Little RR,
England JD, Tennill A, Goldstein DE.
Dening the relationship between
plasma glucose and HbA(1c): analysis of
glucose proles and HbA(1c) in the Di-
abetes Control and Complications Trial.
51. Diabetes Research in Children Network
(DirecNet) Study Group, Wilson DM,
Kollman. Relationship of A1Cto glucose
concentrations in children with type 1
diabetes: assessments by high-frequency
glucose determinations by sensors. Dia-
betes Care 2008;31:381385
52. Skyler JS, Bergenstal R, BonowRO, Buse
J, Deedwania P, Gale EA, Howard BV,
Kirkman MS, Kosiborod M, Reaven P,
Sherwin RS, American Diabetes Associ-
ation, American College of Cardiology
Foundation, American Heart Associa-
tion. Intensive glycemic control and the
prevention of cardiovascular events: im-
plications of the ACCORD, ADVANCE,
and VA diabetes trials: a position state-
ment of the American Diabetes Associa-
tion and a scientic statement of the
American College of Cardiology Foun-
dation and the American Heart Associa-
tion. Diabetes Care 2009;32:187192
53. The effect of intensive treatment of dia-
betes on the development and progres-
sion of long-term complications in
insulin-dependent diabetes mellitus.
The Diabetes Control and Complica-
tions Trial Research Group. N Engl
J Med 1993;329:977986
54. Retinopathy and nephropathy in pa-
tients with type 1 diabetes four years af-
ter a trial of intensive therapy. The
Diabetes Control and Complications
Trial/Epidemiology of Diabetes Interven-
tions and Complications Research Group.
N Engl J Med 2000;342:381389
55. Martin CL, Albers J, Herman WH,
Cleary P, Waberski B, Greene DA,
Stevens MJ, Feldman EL, DCCT/EDIC
Research Group. Neuropathy among the
diabetes control and complications trial
cohort 8 years after trial completion. Di-
abetes Care 2006;29:340344
56. Ohkubo Y, Kishikawa H, Araki E, Miyata
T, Isami S, Motoyoshi S, Kojima Y, Fu-
ruyoshi N, Shichiri M. Intensive insulin
therapy prevents the progression of dia-
betic microvascular complications in
Japanese patients with non-insulin-de-
pendent diabetes mellitus: a randomized
prospective 6-year study. Diabetes Res
Clin Pract 1995;28:103117
57. Effect of intensive blood-glucose control
with metformin on complications in
overweight patients with type 2 diabetes
(UKPDS 34): UK Prospective Diabetes
Study (UKPDS) Group. Lancet 1998;
352:854865
58. Intensive blood-glucose control with
sulphonylureas or insulin compared
with conventional treatment and risk of
complications in patients with type 2 di-
abetes (UKPDS 33): UK Prospective Di-
abetes Study (UKPDS) Group. Lancet
1998;352:837853
59. Holman RR, Paul SK, Bethel MA, Mat-
thews DR, Neil HA: 10-Year follow-up of
intensive glucose control in type 2 dia-
betes. N Engl J Med 2008;359:1577
1589
60. Duckworth W, Abraira C, Moritz T,
Reda D, Emanuele N, Reaven PD, Zieve
FJ, Marks J, Davis SN, Hayward R, War-
ren SR, Goldman S, McCarren M, Vitek
ME, Henderson WG, Huang GD, VADT
Investigators. Glucose control and vas-
cular complications in veterans with
type 2 diabetes. NEngl J Med 2009;360:
129139
61. Moritz T, Duckworth W, Abraira C. Vet-
erans Affairs diabetes trialcorrections.
N Engl J Med 2009;361:10241025
62. Lawson ML, Gerstein HC, Tsui E, Zin-
man B. Effect of intensive therapy on
early macrovascular disease in young in-
dividuals with type 1 diabetes: Asystem-
atic review and meta-analysis. Diabetes
Care 1999;22(Suppl. 2):B35B39
63. ADVANCE Collaborative Group, Patel
A, MacMahon S, Chalmers J, Neal B, Bil-
lot L, Woodward M, Marre M, Cooper
M, Glasziou P, Grobbee D, Hamet P,
Harrap S, Heller S, Liu L, Mancia G, Mo-
gensen CE, Pan C, Poulter N, Rodgers A,
Williams B, Bompoint S, de Galan BE,
Joshi R, Travert F. Intensive blood glu-
cose control and vascular outcomes in
patients with type 2 diabetes. N Engl
J Med 2008;358:25602572
64. Selvin E, Marinopoulos S, Berkenblit G,
Rami T, Brancati FL, Powe NR, Golden
SH. Meta-analysis: glycosylated hemo-
globin and cardiovascular disease in di-
abetes mellitus. Ann Intern Med 2004;
141:421431
65. Stettler C, Allemann S, Ju ni P, Cull CA,
Holman RR, Egger M, Kra henbu hl S,
Diem P. Glycemic control and macro-
vascular disease in types 1 and 2 diabetes
mellitus: Meta-analysis of randomized
trials. Am Heart J 2006;152:2738
66. Nathan DM, Cleary PA, Backlund JY,
Genuth SM, Lachin JM, Orchard TJ,
Raskin P, Zinman B, Diabetes Control
and Complications Trial/Epidemiology
of Diabetes Interventions and Complica-
tions (DCCT/EDIC) Study Research
Group. Intensive diabetes treatment and
cardiovascular disease in patients with
type 1 diabetes. NEngl J Med 2005;353:
26432653
67. Diabetes Control and Complications
Trial/Epidemiology of Diabetes Inter-
ventions and Complications (DCCT/
EDIC) Research Group, Nathan DM,
Zinman B, Cleary PA, Backlund JY, Ge-
nuth S, Miller R, Orchard TJ. Modern-
day clinical course of type 1 diabetes
mellitus after 30 years duration: the di-
abetes control and complications trial/
epidemiology of diabetes interventions
and complications and Pittsburgh epide-
miology of diabetes complications expe-
rience (19832005). Arch Intern Med
2009;169:13071316
68. Action to Control Cardiovascular Risk in
Diabetes Study Group, Gerstein HC,
Miller ME, Byington RP, Goff DC Jr, Big-
ger JT, Buse JB, Cushman WC, Genuth
S, Ismail-Beigi F, Grimm RH Jr, Probst-
eld JL, Simons-Morton DG, Friedewald
WT. Effects of intensive glucose lower-
ing in type 2 diabetes. N Engl J Med
2008;358:25452559
69. Duckworth W. VADT Results. Late-
breaking abstract presented at 68th An-
nual Scientic Sessions of the American
Diabetes Association, 6 June 2008, San
Francisco, CA
70. Reaven PD, Moritz TE, Schwenke DC,
Anderson RJ, Criqui M, Detrano R,
Emanuele N, Kayshap M, Marks J, Mu-
daliar S, Rao RH, Shah JH, Goldman S,
Reda DJ, McCarren M, Abraira C, Duck-
worth W: Intensive glucose lowering
therapy reduces cardiovascular disease
events in VADT participants with lower
calcied coronary atherosclerosis. Dia-
betes 2009;59:26422648
71. Turnbull FM, Abraira C, Anderson RJ,
Byington RP, Chalmers JP, Duckworth
WC, Evans GW, Gerstein HC, Holman
RR, Moritz TE, Neal BC, Ninomiya T,
Patel AA, Paul SK, Travert F, Woodward
M: Intensive glucose control and macro-
vascular outcomes in type 2 diabetes.
Diabetologia 2009;52:22882298
72. American Diabetes Association: Post-
prandial blood glucose (Consensus
Statement). Diabetes Care 2001;24:775
778
73. Ceriello A, Taboga C, Tonutti L, Quagli-
aro L, Piconi L, Bais B, Da Ros R, Motz E.
Evidence for an independent and cu-
mulative effect of postprandial hyper-
triglyceridemia and hyperglycemia on
endothelial dysfunction and oxidative
stress generation: effects of short- and
long-term simvastatin treatment. Circu-
lation 2002;106:12111218
74. Raz I, Wilson PW, Strojek K, Kowalska I,
Bozikov V, Gitt AK, Jermendy G, Cam-
paigne BN, Kerr L, Milicevic Z, Jacober
SJ. Effects of prandial versus fasting gly-
cemia on cardiovascular outcomes in
type 2 diabetes: the HEART2D trial. Di-
abetes Care 2009;32:381386
75. Metzger BE, Buchanan TA, Coustan DR,
de Leiva A, Dunger DB, Hadden DR,
Hod M, Kitzmiller JL, Kjos SL, Oats JN,
Pettitt DJ, Sacks DA, Zoupas C. Sum-
mary and recommendations of the Fifth
International Workshop-Conference on
Gestational Diabetes Mellitus. Diabetes
Care 2007;30(Suppl. 2):S251S260
76. Kitzmiller JL, Block JM, Brown FM,
Catalano PM, Conway DL, Coustan DR,
Gunderson EP, Herman WH, Hoffman
LD, Inturrisi M, Jovanovic LB, Kjos SI,
Knopp RH, Montoro MN, Ogata ES,
Paramsothy P, Reader DM, Rosenn BM,
Thomas AM, Kirkman MS. Managing
preexisting diabetes for pregnancy: sum-
mary of evidence and consensus recom-
mendations for care. Diabetes Care
2008;31:10601079
77. DeWitt DE, Hirsch IB. Outpatient insu-
lin therapy in type 1 and type 2 diabetes
mellitus: scientic review. JAMA 2003;
289:22542264
78. Rosenstock J, Dailey G, Massi-Benedetti
M, Fritsche A, Lin Z, Salzman A. Re-
duced hypoglycemia risk with insulin
glargine: a meta-analysis comparing in-
sulin glargine with human NPH insulin
in type 2 diabetes. Diabetes Care 2005;
28:950955
79. Mooradian AD, BernbaumM, Albert SG.
Narrative review: a rational approach to
starting insulin therapy. Ann Intern Med
2006;145:125134
80. Nathan DM, Buse JB, Davidson MB,
Heine RJ, Holman RR, Sherwin R, Zin-
man B. Management of hyperglycemia in
type 2 diabetes: a consensus algorithm
for the initiation and adjustment of ther-
apy: a consensus statement from the
American Diabetes Association and the
European Association for the Study of
Diabetes. Diabetes Care 2006;29:1963
1972
81. Nathan DM, Buse JB, Davidson MB, Fer-
rannini E, Holman RR, Sherwin R, Zin-
man B, American Diabetes Association,
European Association for Study of Dia-
betes. Medical management of hypergly-
cemia in type 2 diabetes: a consensus
algorithm for the initiation and adjust-
ment of therapy: a consensus statement
of the American Diabetes Association
and the European Association for the
Study of Diabetes. Diabetes Care 2009;
32:193203
82. Bantle JP, Wylie-Rosett J, Albright AL,
Apovian CM, Clark NG, Franz MJ,
Hoogwerf BJ, Lichtenstein AH, Mayer-
Davis E, Mooradian AD, Wheeler ML.
Nutrition recommendations and inter-
ventions for diabetes2006. Diabetes
Care 2006;29:21402157
83. DAFNE Study Group. Training in exi-
ble, intensive insulin management to en-
able dietary freedomin people with type
1 diabetes: dose adjustment for normal
eating (DAFNE) randomised controlled
trial. BMJ 2002;325:746
84. Franz MJ, Monk A, Barry B, McClain K,
Weaver T, Cooper N, Upham P, Bergen-
stal R, Mazze RS. Effectiveness of medi-
cal nutrition therapy provided by
dietitians in the management of non-in-
sulin-dependent diabetes mellitus: a
randomized, controlled clinical trial.
J Am Diet Assoc 1995;95:10091017
85. Goldhaber-Fiebert JD, Goldhaber-Fiebert
SN, Tristan ML, Nathan DM. Randomized
controlled community-based nutrition
and exercise intervention improves glyce-
mia and cardiovascular risk factors in type
2 diabetic patients in rural Costa Rica. Di-
abetes Care 2003;26:2429
86. Lemon CC, Lacey K, Lohse B, Hubacher
DO, Klawitter B, Palta M. Outcomes
monitoring of health, behavior, and
quality of life after nutrition intervention
in adults with type 2 diabetes. J Am Diet
Assoc 2004;104:18051815
87. Miller CK, Edwards L, Kissling G, San-
ville L. Nutrition education improves
metabolic outcomes among older adults
with diabetes mellitus: results from a
randomized controlled trial. Prev Med
2002;34:252259
88. Wilson C, Brown T, Acton K, Gilliland S.
Effects of clinical nutrition education
and educator discipline on glycemic
control outcomes in the Indian health
service. Diabetes Care 2003;26:2500
2504
89. Graber AL, Elasy TA, Quinn D, Wolff K,
Brown A. Improving glycemic control in
adults with diabetes mellitus: shared re-
sponsibility in primary care practices.
South Med J 2002;95:684690
90. Gaetke LM, Stuart MA, Truszczynska H.
A single nutrition counseling session
with a registered dietitian improves
short-term clinical outcomes for rural
Kentucky patients with chronic diseases.
J Am Diet Assoc 2006;106:109112
91. Yu-Poth S, Zhao G, Etherton T, Naglak
M, Jonnalagadda S, Kris-Etherton PM.
Effects of the National Cholesterol Ed-
ucation Programs Step I and Step II
dietary intervention programs on car-
diovascular disease risk factors: a meta-
analysis. Am J Clin Nutr 1999;69:632
646
92. Van Horn L, McCoin M, Kris-Etherton
PM, Burke F, Carson JA, Champagne
CM, Karmally W, Sikand G. The evi-
dence for dietary prevention and treat-
ment of cardiovascular disease. J Am
Diet Assoc 2008;108:287331
93. Appel LJ, Moore TJ, Obarzanek E,
Vollmer WM, Svetkey LP, Sacks FM,
Bray GA, Vogt TM, Cutler JA,
Windhauser MM, Lin PH, Karanja N. A
clinical trial of the effects of dietary pat-
terns on blood pressure. DASH Collab-
orative Research Group. N Engl J Med
1997;336:11171124
94. Norris SL, Zhang X, Avenell A, Gregg E,
Bowman B, Schmid CH, Lau J. Long-
term effectiveness of weight-loss inter-
ventions in adults with pre-diabetes: a
review. Am J Prev Med 2005;28:126
139
95. Klein S, Sheard NF, Pi-Sunyer X, Daly A,
Wylie-Rosett J, Kulkarni K, Clark NG,
American Diabetes Association, North
American Association for the Study of
Obesity, American Society for Clinical
Nutrition. Weight management through
lifestyle modication for the prevention
and management of type 2 diabetes: ra-
tionale and strategies: a statement of
the American Diabetes Association, the
North American Association for the
Study of Obesity, and the American So-
ciety for Clinical Nutrition. Diabetes
Care 2004;27:20672073
96. Norris SL, Zhang X, Avenell A, Gregg E,
Schmid CH, Kim C, Lau J. Efcacy of
pharmacotherapy for weight loss in
adults with type 2 diabetes mellitus: a
meta-analysis. Arch Intern Med 2004;
164:13951404
97. Wolf AM, Conaway MR, Crowther JQ,
Hazen KY, L Nadler J, Oneida B, Bovb-
jerg VE, Improving Control with Activity
and Nutrition (ICAN) Study. Translat-
ing lifestyle intervention to practice in
obese patients with type 2 diabetes: Im-
proving Control with Activity and Nutri-
tion (ICAN) study. Diabetes Care 2004;
27:15701576
98. Manning RM, Jung RT, Leese GP, New-
ton RW. The comparison of four weight
reduction strategies aimed at overweight
patients with diabetes mellitus: four-
yearfollow-up.DiabetMed1998;15:497
502
99. Shai I, Schwarzfuchs D, Henkin Y, Sha-
har DR, Witkow S, Greenberg I, Golan
R, Fraser D, Bolotin A, Vardi H, Tangi-
Rozental O, Zuk-Ramot R, Sarusi B,
Brickner D, Schwartz Z, Sheiner E,
Marko R, Katorza E, Thiery J, Fiedler
GM, Blu her M, Stumvoll M, Stampfer
MJ, Dietary Intervention Randomized
Controlled Trial (DIRECT) Group.
Weight loss with a low-carbohydrate,
Mediterranean, or low-fat diet. N Engl
J Med 2008;359:229241
100. Franz MJ, VanWormer JJ, Crain AL,
Boucher JL, Histon T, Caplan W, Bow-
man JD, Pronk NP. Weight-loss out-
comes: a systematic review and meta-
analysis of weight-loss clinical trials with
a minimum 1-year follow-up. J Am Diet
Assoc 2007;107:17551767
101. Look AHEAD Research Group, Pi-Su-
nyer X, Blackburn G, Brancati FL, Bray
GA, Bright R, Clark JM, Curtis JM, Es-
peland MA, Foreyt JP, Graves K, Haffner
SM, Harrison B, Hill JO, Horton ES, Ja-
Position Statement
kicic J, Jeffery RW, Johnson KC, Kahn S,
Kelley DE, Kitabchi AE, Knowler WC,
Lewis CE, Maschak-Carey BJ, Montgom-
ery B, Nathan DM, Patricio J, Peters A,
Redmon JB, Reeves RS, Ryan DH, Safford
M, Van Dorsten B, Wadden TA, Wagen-
knecht L, Wesche-Thobaben J, Wing RR,
Yanovski SZ. Reductioninweight andcar-
diovascular disease risk factors in individ-
uals with type 2 diabetes: one-year results
of the look AHEAD trial. Diabetes Care
2007;30:13741383
102. Foster GD, Wyatt HR, Hill JO,
McGuckin BG, Brill C, Mohammed BS,
Szapary PO, Rader DJ, Edman JS, Klein
S. A randomized trial of a low-carbohy-
drate diet for obesity. N Engl J Med
2003;348:20822090
103. Stern L, Iqbal N, Seshadri P, Chicano
KL, Daily DA, McGrory J, Williams M,
Gracely EJ, Samaha FF. The effects of
low-carbohydrate versus conventional
weight loss diets in severely obese
adults: one-year follow-up of a random-
ized trial. Ann Intern Med 2004;140:
778785
104. Gardner CD, Kiazand A, Alhassan S,
Kim S, Stafford RS, Balise RR, Kraemer
HC, King AC. Comparison of the At-
kins, Zone, Ornish, and LEARN diets
for change in weight and related risk
factors among overweight premeno-
pausal women. JAMA 2007;297:969
977
105. Nordmann AJ, Nordmann A, Briel M,
Keller U, Yancy WS, Jr, Brehm BJ,
Bucher HC. Effects of low-carbohydrate
vs low-fat diets on weight loss and car-
diovascular risk factors: a meta-analysis
of randomized controlled trials. Arch In-
tern Med 2006;166:285293
106. Institute of Medicine: DIetary Reference
Intakes: Energy, Carbohydrate, Fiber, Fat,
Fatty Acids, Cholesterol, Protein, and
Amino Acids. Washington, DC, National
Academies Press, 2002
107. Barnard ND, Cohen J, Jenkins DJ, Turner-
McGrievy G, Gloede L, Jaster B, Seidl K,
Green AA, Talpers S. A low-fat vegan
diet improves glycemic control and car-
diovascular risk factors in a randomized
clinical trial in individuals with type 2
diabetes. Diabetes Care 2006;29:1777
1783
108. Turner-McGrievy GM, Barnard ND, Co-
hen J, Jenkins DJ, Gloede L, Green AA.
Changes in nutrient intake and dietary
quality among participants with type 2
diabetes following a low-fat vegan diet or
a conventional diabetes diet for 22
weeks. J Am Diet Assoc 2008;108:
16361645
109. Franz MJ, Bantle JP, Beebe CA, Brunzell
JD, Chiasson JL, Garg A, Holzmeister
LA, Hoogwerf B, Mayer-Davis E, Moora-
dian AD, Purnell JQ, Wheeler M. Evi-
dence-based nutrition principles and
recommendations for the treatment and
prevention of diabetes and related com-
plications. Diabetes Care 2002;25:148
198
110. Buchwald H, Estok R, Fahrbach K, Banel
D, Jensen MD, Pories WJ, Bantle JP,
Sledge I. Weight and type 2 diabetes af-
ter bariatric surgery: systematic review
and meta-analysis. Am J Med 2009;122:
248256
111. Dixon JB, OBrien PE, Playfair J, Chap-
man L, Schachter LM, Skinner S, Proi-
etto J, Bailey M, Anderson M. Adjustable
gastric banding and conventional ther-
apy for type 2 diabetes: a randomized
controlled trial. JAMA 2008;299:316
323
112. Buchwald H, Estok R, Fahrbach K, Banel
D, Sledge I. Trends in mortality in bari-
atric surgery: a systematic review and
meta-analysis. Surgery 2007;142:621
632
113. Sjo stro m L, Narbro K, Sjo stro m CD,
Karason K, Larsson B, Wedel H, Lystig
T, Sullivan M, Bouchard C, Carlsson B,
Bengtsson C, Dahlgren S, Gummesson
A, Jacobson P, Karlsson J, Lindroos AK,
Lo nroth H, Na slund I, Olbers T, Stenlo f
K, Torgerson J, Agren G, Carlsson LM,
Swedish Obese Subjects Study. Effects of
bariatric surgery on mortality in Swedish
obese subjects. N Engl J Med 2007;357:
741752
114. Piette JD, Glasgow RE: Sttategies for im-
proving behavioral and health outcomes
among people with diabetes: self man-
agement education. In Evidence-Based
Diabetes Care. Gerstein HC, Hayes RB,
Eds. Ontario, Canada, BC Decker, 2000
115. Norris SL, Engelgau MM, Narayan KM.
Effectiveness of self-management train-
ing in type 2 diabetes: a systematic re-
view of randomized controlled trials.
116. Norris SL, Lau J, Smith SJ, Schmid CH,
Engelgau MM. Self-management educa-
tion for adults with type 2 diabetes: a
meta-analysis of the effect on glycemic
control. Diabetes Care 2002;25:1159
1171
117. Gary TL, Genkinger JM, Guallar E, Pey-
rot M, Brancati FL. Meta-analysis of ran-
domized educational and behavioral
interventions in type 2 diabetes. Diabe-
tes Educ 2003;29:488501
118. Steed L, Cooke D, Newman S. A system-
atic review of psychosocial outcomes
following education, self-management
and psychological interventions in dia-
betes mellitus. Patient Educ Couns
2003;51:515
119. Ellis SE, Speroff T, Dittus RS, Brown A,
Pichert JW, Elasy TA. Diabetes patient
education: a meta-analysis and meta-re-
gression. Patient Educ Couns 2004;52:
97105
120. Warsi A, Wang PS, LaValley MP, Avorn
J, Solomon DH. Self-management edu-
cation programs in chronic disease: a
systematic review and methodological
critique of the literature. Arch Intern
Med 2004;164:16411649
121. Funnell MM, Brown TL, Childs BP, Haas
LB, Hosey GM, Jensen B, Maryniuk M,
Peyrot M, Piette JD, Reader D, Siminerio
LM, Weinger K, Weiss MA. National
standards for diabetes self-management
education. Diabetes Care 2007;30:
16301637
122. Mulcahy K, Maryniuk M, Peeples M, Pey-
rot M, Tomky D, Weaver T, YarboroughP.
Diabetes self-management education core
outcomes measures. Diabetes Educ
29:768- 2003;84:787
123. Glasgow RE, Peeples M, Skovlund SE.
Where is the patient in diabetes perfor-
mance measures? The case for including
patient-centered and self-management
measures. Diabetes Care 2008;31:1046
1050
124. Barker JM, Goehrig SH, Barriga K, Hoff-
man M, Slover R, Eisenbarth GS, Norris
JM, Klingensmith GJ, Rewers M, DAISY
study. Clinical characteristics of chil-
dren diagnosed with type 1 diabetes
through intensive screening and follow-
up. Diabetes Care 2004;27:13991404
125. Cochran J, Conn VS. Meta-analysis of
quality of life outcomes following diabe-
tes self-management training. Diabetes
Educ 2008;34:815823
126. Fisher EB, Thorpe CT, Devellis BM, De-
vellis RF. Healthy coping, negative emo-
tions, and diabetes management: a
systematic review and appraisal. Diabe-
tes Educ 2007;33:10801103
127. Robbins JM, Thatcher GE, Webb DA,
Valdmanis VG. Nutritionist visits, diabe-
tes classes, and hospitalization rates and
charges: the Urban Diabetes Study. Dia-
betes Care 2008;31:655660
128. Renders CM, Valk GD, Grifn SJ, Wag-
ner EH, Eijk Van JT, Assendelft WJ. In-
terventions to improve the management
of diabetes in primary care, outpatient,
and community settings: a systematic re-
view. Diabetes Care 2001;24:1821
1833
129. Polonsky WH, Earles J, Smith S, Pease
DJ, Macmillan M, Christensen R, Taylor
T, Dickert J, Jackson RA. Integrating
medical management with diabetes self-
management training: a randomized
control trial of the Diabetes Outpatient
Intensive Treatment program. Diabetes
Care 2003;26:30483053
130. Anderson RM, Funnell MM, Nwankwo
R, Gillard ML, Oh M, Fitzgerald JT.
Evaluating a problem-based empower-
ment program for African Americans
with diabetes: results of a randomized
controlled trial. Ethn Dis 2005;15:
671678
131. Brown SA, Blozis SA, Kouzekanani K,
Garcia AA, Winchell M, Hanis CL. Dos-
age effects of diabetes self-management
education for Mexican Americans: the
Starr County Border Health Initiative.
132. Glazier RH, Bajcar J, Kennie NR, Willson
K. A systematic review of interventions
to improve diabetes care in socially dis-
advantaged populations. Diabetes Care
2006;29:16751688
133. Sarkisian CA, Brown AF, Norris KC,
Wintz RL, Mangione CM. A systematic
reviewof diabetes self-care interventions
for older, African American, or Latino
adults. Diabetes Educ 2003;29:467479
134. Chodosh J, Morton SC, Mojica W, Ma-
glione M, Suttorp MJ, Hilton L, Rhodes
S, Shekelle P. Meta-analysis: chronic dis-
ease self-management programs for
older adults. Ann Intern Med 2005;143:
427438
135. Peyrot M, Rubin RR. Behavioral and psy-
chosocial interventions in diabetes: a
conceptual review. Diabetes Care 2007;
30:24332440
136. Rickheim PL, Weaver TW, Flader JL,
Kendall DM. Assessment of group versus
individual diabetes education: a ran-
domized study. Diabetes Care 2002;25:
269274
137. Trento M, Passera P, Borgo E, Tomalino
M, Bajardi M, Cavallo F, Porta M. A
5-year randomized controlled study of
learning, problem solving ability, and
quality of life modications in people
with type 2 diabetes managed by group
care. Diabetes Care 2004;27:670675
138. Deakin T, McShane CE, Cade JE, Wil-
liams RD: Group based training for self-
management strategies in people with
type 2 diabetes mellitus. Cochrane Da-
tabase Syst Rev CD003417, 2005
139. Heisler, M. Building Peer Support Pro-
grams to Manage Chronic Disease: Seven
Models for Success. Oakland, CA, Califor-
nia Health Care Foundation, 2006
140. Foster G, Taylor SJ, Eldridge SE, Ramsay
J, Grifths CJ: Self-management educa-
tion programmes by lay leaders for peo-
ple with chronic conditions. Cochrane
Database Syst Rev CD005108, 2007
141. Norris SL, Chowdhury FM, Van Le K,
Horsley T, Brownstein JN, Zhang X, Jack
L Jr, Sattereld DW. Effectiveness of
community health workers in the care of
persons with diabetes. Diabet Med
2006;23:544556
142. Duncan I, Birkmeyer C, Coughlin S, Li
QE, Sherr D, Boren S. Assessing the
value of diabetes education. Diabetes
Educ 2009;35:752760
143. Sigal RJ, Kenny GP, Wasserman DH,
Castaneda-Sceppa C. Physical activity/
exercise and type 2 diabetes. Diabetes
Care 2004;27:25182539
144. Wasserman DH, Zinman B. Exercise in
individuals with IDDM. Diabetes Care
1994;17:924937
145. Boule NG, Haddad E, Kenny GP, Wells
GA, Sigal RJ. Effects of exercise on gly-
cemic control and body mass in type 2
diabetes mellitus: a meta-analysis of
controlledclinicaltrials.JAMA2001;286:
12181227
146. Boule NG, Kenny GP, Haddad E, Wells
GA, Sigal RJ. Meta-analysis of the effect
of structured exercise training on cardio-
respiratory tness in Type 2 diabetes
mellitus. Diabetologia 2003;46:1071
1081
147. U.S. Department of Health and Human
Services. 2008 Physical Activity Guide-
lines for Americans. Atlanta, GA,
Centers for Disease Control and Pre-
vention, 2008
148. Cauza E, Hanusch-Enserer U, Strasser B,
Ludvik B, Metz-Schimmerl S, Pacini G,
Wagner O, Georg P, Prager R, Kostner K,
Dunky A, Haber P. The relative benets
of endurance and strength training on
the metabolic factors and muscle func-
tion of people with type 2 diabetes mel-
litus. Arch Phys Med Rehabil 2005;86:
15271533
149. Dunstan DW, Daly RM, Owen N, Jolley
D, De Courten M, Shaw J, Zimmet P.
High-intensity resistance training im-
proves glycemic control in older patients
with type 2 diabetes. Diabetes Care
2002;25:17291736
150. Castaneda C, Layne JE, Munoz-Orians
L, Gordon PL, Walsmith J, Foldvari M,
Roubenoff R, Tucker KL, Nelson ME. A
randomized controlled trial of resistance
exercise training to improve glycemic
control in older adults with type 2 dia-
betes. Diabetes Care 2002;25:2335
2341
151. Sigal RJ, Kenny GP, Boule NG, Wells
GA, Prudhomme D, Fortier M, Reid RD,
Tulloch H, Coyle D, Phillips P, Jennings
A, Jaffey J. Effects of aerobic training, re-
sistance training, or both on glycemic
control in type 2 diabetes: a randomized
trial. Ann Intern Med 2007;147:
357369
152. Bax JJ, Young LH, Frye RL, Bonow RO,
Steinberg HO, Barrett EJ, ADA. Screen-
ing for coronary artery disease in pa-
tients with diabetes. Diabetes Care 2007;
30:27292736
153. Berger M, Berchtold P, Cu ppers HJ,
Drost H, Kley HK, Mu ller WA,
Wiegelmann W, Zimmerman-Telschow
H, Gries FA, Kru skemper HL, Zimmer-
mann H. Metabolic and hormonal ef-
fects of muscular exercise in juvenile
type diabetics. Diabetologia 1977;13:
355365
154. American Diabetes Association: Physical
activity/exercise and diabetes (Position
Statement). Diabetes Care 2004;
27(Suppl. 1):S58S62
155. Berger M: Adjustment of insulin and oral
agent therapy. In Handbook of Exercise in
Diabetes. 2nd ed. Ruderman N, Devlin
JTSSH, Krisska A, Eds. Alexandria, VA,
American Diabetes Association, 2002, p.
365376
156. Aiello LP, Wong J, Cavallerano J, Bursell
SE, Aiello LM: Retinopathy. In Handbook
of Exercise in Diabetes. 2nd ed. Ru-
derman N, Devlin JT, Kriska A, Eds.
Alexandria, VA, American Diabetes As-
sociation, 2002, p. 401413
157. Lemaster JW, Reiber GE, Smith DG,
Heagerty PJ, Wallace C. Daily weight-
bearing activity does not increase the
risk of diabetic foot ulcers. Med Sci
Sports Exerc 2003;35:10931099
158. Vinik A, Erbas T: Neuropathy. In Hand-
book of Exercise in Diabetes. 2nd ed. Ru-
sociation, 2002, p. 463496
159. Wackers FJ, Young LH, Inzucchi SE,
Chyun DA, Davey JA, Barrett EJ,
Taillefer R, Wittlin SD, Heller GV, Filip-
chuk N, Engel S, Ratner RE, Iskandrian
AE, Detection of Ischemia in Asymp-
tomatic Diabetics Investigators. Detec-
tion of silent myocardial ischemia in
asymptomatic diabetic subjects: the
DIAD study. Diabetes Care 2004;27:
19541961
160. Valensi P, Sachs RN, Harfouche B,
Lormeau B, Paries J, Cosson E, Paycha F,
Leutenegger M, Attali JR. Predictive
value of cardiac autonomic neuropathy
in diabetic patients with or without si-
lent myocardial ischemia. Diabetes Care
2001;24:339343
161. Mogensen CE: Nephropathy. In Hand-
book of Exercise in Diabetes. 2nd ed. Ru-
sociation, 2002, p. 433449
162. Anderson RJ, Grigsby AB, Freedland KE,
de Groot M, McGill JB, Clouse RE, Lust-
man PJ. Anxiety and poor glycemic con-
trol: a meta-analytic review of the
literature. Int J Psychiatry Med 2002;32:
235247
163. Delahanty LM, Grant RW, Wittenberg E,
Bosch JL, Wexler DJ, Cagliero E, Meigs
JB. Association of diabetes-related emo-
tional distress with diabetes treatment in
primary care patients with Type 2 diabe-
tes. Diabet Med 2007;24:4854
164. American Diabetes Association: Psycho-
social factors affecting adherence, qual-
ity of life, and well-being: Helping
Patients cope. In Medical Management of
Type 1 Diabetes. 5 ed. Francine R. Kauf-
man, Ed. Alexandria, VA, American Di-
abetes Association, 2008, p. 173193
165. Fisher L, Skaff MM, Mullan JT, Arean P,
Mohr D, Masharani U, Glasgow R, Lau-
rencin G. Clinical depression versus dis-
tress among patients with type 2
diabetes: not just a question of seman-
tics. Diabetes Care 2007;30:542548
166. Surwit RS, Schneider MS, Feinglos MN.
Stress and diabetes mellitus. Diabetes
Care 1992;15:14131422
167. McCulloch DK, Glasgow RE, Hampson
SE, Wagner E. A systematic approach to
Position Statement
diabetes management in the post-DCCT
era. Diabetes Care 1994;17:765769
168. Rubin RR, Peyrot M. Psychological is-
sues and treatments for people with di-
abetes. J Clin Psychol 2001;57:457478
169. Jacobson AM. Depression and diabetes.
170. Lustman PJ, Grifth LS, Clouse RE,
Cryer PE. Psychiatric illness in diabetes
mellitus. Relationship to symptoms and
glucose control. J Nerv Ment Dis 1986;
174:736742
171. Blonde L, Merilainen M, Karwe V,
Raskin P, TITRATE Study Group. Pa-
tient-directed titration for achieving gly-
caemic goals using a once-daily basal
insulin analogue: an assessment of two
different fasting plasma glucose targets
-the TITRATE study. Diabetes Obes
Metab 2009;11:623631
172. American Diabetes Association: Hyper-
glycemic crises in diabetes. Diabetes
Care 2004;27 (Suppl. 1):S94S102
173. Kitabchi AE, Umpierrez GE, Miles JM,
Fisher JN. Hyperglycemic crises in adult
patients with diabetes. Diabetes Care
2009;32:13351343
174. Cryer PE. Hypoglycaemia: the limiting
factor in the glycaemic management of
Type I and Type II diabetes. Diabetolo-
gia 2002;45:937948
175. Gannon MC, Nuttall FQ: Protein and
Diabetes. In American Diabetes Associa-
tion Guide to Medical Nutrition Therapy
for Diabetes. Franz MJ, Bantle JP, Eds.
sociation, 1999, p. 107125
176. Cryer PE. Diverse causes of hypoglyce-
mia-associated autonomic failure in dia-
betes. N Engl J Med 2004;350:2272
2279
177. Cryer PE, Davis SN, Shamoon H. Hypo-
glycemia in diabetes. Diabetes Care
2003;26:19021912
178. Smith SA, Poland GA. Use of inuenza
and pneumococcal vaccines in people
with diabetes. Diabetes Care 2000;23:
95108
179. Colquhoun AJ, Nicholson KG, Botha JL,
Raymond NT. Effectiveness of inuenza
vaccine in reducing hospital admissions
in people with diabetes. Epidemiol In-
fect 1997;119:335341
180. Bridges CB, Fukuda K, Uyeki TM, Cox
NJ, Singleton JA. Prevention and control
of inuenza. Recommendations of the
Advisory Committee on Immunization
Practices (ACIP). MMWR Recomm Rep
2002;51:131
181. American Diabetes Association: Inu-
enza and pneumococcal immunization
in diabetes (Position Statement). Diabe-
tes Care 2004;27(Suppl. 1):S111S113
182. Gaede P, Lund-Andersen H, Parving
HH, Pedersen O. Effect of a multifacto-
rial intervention on mortality in type 2
diabetes. N Engl J Med 2008;358:580
591
183. Buse JB, Ginsberg HN, Bakris GL, Clark
NG, Costa F, Eckel R, Fonseca V, Ger-
stein HC, Grundy S, Nesto RW, Pignone
MP, Plutzky J, Porte D, Redberg R, Stit-
zel KF, Stone NJ, American Heart Asso-
ciation, American Diabetes Association.
Primary prevention of cardiovascular
diseases in people with diabetes melli-
tus: a scientic statement from the
American Heart Association and the
American Diabetes Association. Diabe-
tes Care 2007;30:162172
184. Chobanian AV, Bakris GL, Black HR,
Cushman WC, Green LA, Izzo JL Jr,
Jones DW, Materson BJ, Oparil S,
Wright JT Jr, Roccella EJ, National
Heart, Lung, and Blood Institute Joint
National Committee on Prevention, De-
tection, Evaluation, and Treatment of
High Blood Pressure, National High Blood
Pressure Education Program Coordinat-
ing Committee. The Seventh Report of the
Joint National Committee on Prevention,
Detection, Evaluation, and Treatment of
High Blood Pressure: the JNC 7 report.
JAMA 2003;289:25602572
185. Bobrie G, Chatellier G, Genes N, Clerson
P, Vaur L, Vaisse B, Menard J, Mallion
JM. Cardiovascular prognosis of
masked hypertension detected by
blood pressure self-measurement in el-
derly treated hypertensive patients.
JAMA 2004;291:13421349
186. Sega R, Facchetti R, Bombelli M, Cesana
G, Corrao G, Grassi G, Mancia G. Prog-
nostic value of ambulatory and home
blood pressures compared with ofce
blood pressure in the general popula-
tion: follow-up results from the Pres-
sioni Arteriose Monitorate e Loro
Associazioni (PAMELA) study. Circula-
tion 2005;111:17771783
187. UKPDS: Tight blood pressure control
and risk of macrovascular and microvas-
cular complications in type 2 diabetes:
UKPDS 38. UK Prospective Diabetes
Study Group. BMJ 1998;317:703713
188. Hansson L, Zanchetti A, Carruthers SG,
Dahlo f B, Elmfeldt D, Julius S, Me nard J,
Rahn KH, Wedel H, Westerling S. Ef-
fects of intensive blood-pressure lower-
ing and low-dose aspirin in patients
with hypertension: principal results of
the Hypertension Optimal Treatment
(HOT) randomised trial. HOT Study
Group. Lancet 1998;351:17551762
189. Adler AI, Stratton IM, Neil HA, Yudkin
JS, Matthews DR, Cull CA, Wright AD,
Turner RC, Holman RR. Association of
systolic blood pressure with macrovas-
cular and microvascular complications
of type 2 diabetes (UKPDS 36): prospec-
tive observational study. BMJ 2000;321:
412419
190. Lewington S, Clarke R, Qizilbash N,
Peto R, Collins R, Prospective Studies
Collaboration. Age-specic relevance of
usual blood pressure to vascular mortal-
ity: a meta-analysis of individual data for
one million adults in 61 prospective
studies. Lancet 2002;360:19031913
191. Stamler J, Vaccaro O, Neaton JD, Went-
worth D. Diabetes, other risk factors,
and 12-yr cardiovascular mortality for
men screened in the Multiple Risk Fac-
tor Intervention Trial. Diabetes Care
1993;16:434444
192. Cushman WC, Grimm RH Jr, Cutler JA,
Evans GW, Capes S, Corson MA, Sadler
LS, Alderman MH, Peterson K, Bertoni
A, Basile JN, ACCORDStudy Group: Ra-
tionale and design for the blood pressure
intervention of the Action to Control
Cardiovascular Risk in Diabetes (AC-
CORD) trial. AmJ Cardiol 2007;99:44i
55i
193. Sacks FM, Svetkey LP, Vollmer WM, Ap-
pel LJ, Bray GA, Harsha D, Obarzanek E,
Conlin PR, Miller ER 3rd, Simons-Mor-
ton DG, Karanja N, Lin PH, DASH-So-
dium Collaborative Research Group.
Effects on blood pressure of reduced di-
etary sodium and the Dietary Ap-
proaches to Stop Hypertension (DASH)
diet. DASH-Sodium Collaborative Re-
search Group. N Engl J Med 2001;344:
310
194. Tatti P, Pahor M, Byington RP, Di Mauro
P, Guarisco R, Strollo G, Strollo F. Out-
come results of the Fosinopril Versus
Amlodipine Cardiovascular Events Ran-
domized Trial (FACET) in patients with
hypertension and NIDDM. Diabetes
Care 1998;21:597603
195. Estacio RO, Jeffers BW, Hiatt WR, Big-
gerstaff SL, Gifford N, Schrier RW. The
effect of nisoldipine as compared with
enalapril on cardiovascular outcomes in
patients with non-insulin-dependent di-
abetes and hypertension. N Engl J Med
1998;338:645652
196. Schrier RW, Estacio RO, Mehler PS, Hi-
att WR. Appropriate blood pressure
control in hypertensive and normoten-
sive type 2 diabetes mellitus: a summary
of the ABCD trial. Nat Clin Pract Neph-
rol 2007;3:428438
197. ALLHAT Ofcers and Coordinators for
the ALLHAT Collaborative Research
Group. The Antihypertensive and Lipid-
Lowering Treatment to Prevent Heart
Attack Trial: the Antihypertensive and
Lipid-Lowering Treatment to Prevent
Heart Attack Trial (ALLHAT). JAMA
2002;288:29812997
198. Psaty BM, Lumley T, Furberg CD, Schel-
lenbaum G, Pahor M, Alderman MH,
Weiss NS. Health outcomes associated
with various antihypertensive therapies
used as rst-line agents: a network meta-
analysis. JAMA 2003;289:25342544
199. Effects of ramipril on cardiovascular and
microvascular outcomes in people with
diabetes mellitus: results of the HOPE
study and MICRO-HOPE substudy:
Heart Outcomes Prevention Evaluation
Study Investigators. Lancet 2000;355:
253259
200. Pfeffer MA, Swedberg K, Granger CB,
Held P, McMurray JJ, Michelson EL,
Olofsson B, Ostergren J, Yusuf S, Pocock
S, CHARM Investigators and Commit-
tees. Effects of candesartan on mortality
and morbidity in patients with chronic
heart failure: the CHARM-Overall pro-
gramme. Lancet 2003;362:759766
201. Granger CB, McMurray JJ, Yusuf S, Held
P, Michelson EL, Olofsson B, Ostergren
J, Pfeffer MA, Swedberg K, CHARM In-
vestigators and Committees. Effects of
candesartan in patients with chronic
heart failure and reduced left-ventricular
systolic function intolerant to angioten-
sin-converting-enzyme inhibitors: the
CHARM-Alternative trial. Lancet 2003;
362:772776
202. McMurray JJ, Ostergren J, Swedberg K,
Granger CB, Held P, Michelson EL,
Olofsson B, Yusuf S, Pfeffer MA,
CHARM Investigators and Committees.
Effects of candesartan in patients with
chronic heart failure and reduced left-
ventricular systolic function taking an-
giotensin-converting-enzyme
inhibitors: the CHARM-Added trial.
Lancet 2003;362:767771
203. Lindholm LH, Ibsen H, Dahlo f B, De-
vereux RB, Beevers G, de Faire U, Fyhr-
quist F, Julius S, Kjeldsen SE,
Kristiansson K, Lederballe-Pedersen O,
Nieminen MS, Omvik P, Oparil S,
Wedel H, Aurup P, Edelman J, Snapinn
S, LIFE Study Group. Cardiovascular
morbidity and mortality in patients with
diabetes in the Losartan Intervention For
Endpoint reduction in hypertension
study (LIFE): a randomised trial against
atenolol. Lancet 2002;359:10041010
204. Berl T, Hunsicker LG, Lewis JB, Pfeffer
MA, Porush JG, Rouleau JL, Drury PL,
Esmatjes E, Hricik D, Parikh CR, Raz I,
Vanhille P, Wiegmann TB, Wolfe BM,
Locatelli F, Goldhaber SZ, Lewis EJ,
Irbesartan Diabetic Nephropathy Trial.
Collaborative Study Group. Collabora-
tive Study Group. Cardiovascular out-
comes in the Irbesartan Diabetic
Nephropathy Trial of patients with type
2 diabetes and overt nephropathy. Ann
Intern Med 2003;138:542549
205. Laffel LM, McGill JB, Gans DJ. The ben-
ecial effect of angiotensin-converting
enzyme inhibition with captopril on di-
abetic nephropathy in normotensive
IDDM patients with microalbuminuria.
North American Microalbuminuria
Study Group. Am J Med 1995;99:497
504
206. Bakris GL, Williams M, Dworkin L, El-
liott WJ, Epstein M, Toto R, Tuttle K,
Douglas J, Hsueh W, Sowers J. Preserv-
ing renal function in adults with hyper-
tension and diabetes: a consensus
approach: National Kidney Foundation
Hypertension and Diabetes Executive
Committees Working Group. Am J Kid-
ney Dis 2000;36:646661
207. Psaty BM, Smith NL, Siscovick DS, Ko-
epsell TD, Weiss NS, Heckbert SR, Le-
maitre RN, Wagner EH, Furberg CD.
Health outcomes associated with antihy-
pertensive therapies used as rst-line
agents: a systematic review and meta-
analysis. JAMA 1997;277:739745
208. Patel A, ADVANCE Collaborative
Group, MacMahon S, Chalmers J, Neal
B, Woodward M, Billot L, Harrap S,
Poulter N, Marre M, Cooper M, Glasziou
P, Grobbee DE, Hamet P, Heller S, Liu
LS, Mancia G, Mogensen CE, Pan CY,
Rodgers A, Williams B. Effects of a xed
combination of perindopril and indap-
amide on macrovascular and microvas-
cular outcomes in patients with type 2
diabetes mellitus (the ADVANCE trial):
a randomised controlled trial. Lancet
2007;370:829840
209. Sibai BM. Treatment of hypertension in
pregnant women. N Engl J Med 1996;
335:257265
210. Baigent C, Keech A, Kearney PM, Black-
well L, Buck G, Pollicino C, Kirby A,
Sourjina T, Peto R, Collins R, Simes R,
Cholesterol Treatment Trialists (CTT)
Collaborators. Efcacy and safety of
cholesterol-lowering treatment: pro-
spective meta-analysis of data from
90,056 participants in 14 randomised
trials of statins. Lancet 2005;366:1267
1278
211. Pyo ra la K, Pedersen TR, Kjekshus J,
Faergeman O, Olsson AG, Thorgeirsson
G. Cholesterol lowering with simvasta-
tin improves prognosis of diabetic pa-
tients with coronary heart disease: a
subgroup analysis of the Scandinavian
Simvastatin Survival Study (4S). Diabe-
tes Care 1997;20:614620
212. Collins R, Armitage J, Parish S, Sleigh P,
Peto R, Heart Protection Study Collabo-
rative Group: MRC/BHF Heart Protec-
tion Study of cholesterol-lowering with
simvastatin in 5963 people with diabe-
tes: a randomised placebo-controlled
trial. Lancet 2003;361:20052016
213. Goldberg RB, Mellies MJ, Sacks FM,
Moye LA, Howard BV, Howard WJ,
Davis BR, Cole TG, Pfeffer MA, Braun-
wald E. Cardiovascular events and their
reduction with pravastatin in diabetic
and glucose-intolerant myocardial in-
farction survivors with average choles-
terol levels: subgroup analyses in the
cholesterol and recurrent events (CARE)
trial. The Care Investigators. Circulation
1998;98:25132519
214. Shepherd J, Barter P, Carmena R, Deed-
wania P, Fruchart JC, Haffner S, Hsia J,
Breazna A, LaRosa J, Grundy S, Waters
D. Effect of lowering LDL cholesterol
substantially below currently recom-
mended levels in patients with coronary
heart disease and diabetes: the Treating
to New Targets (TNT) study. Diabetes
Care 2006;29:12201226
215. Sever PS, Poulter NR, Dahlo f B, Wedel
H, Collins R, Beevers G, Cauleld M,
Kjeldsen SE, Kristinsson A, McInnes GT,
Mehlsen J, Nieminen M, OBrien E, Os-
tergren J. Reduction in cardiovascular
events with atorvastatin in 2,532 pa-
tients with type 2 diabetes: Anglo-Scan-
dinavian Cardiac Outcomes Triallipid-
lowering arm (ASCOT-LLA). Diabetes
Care 2005;28:11511157
216. Knopp RH, dEmden M, Smilde JG, Po-
cock SJ. Efcacy and safety of atorvasta-
tin in the prevention of cardiovascular
end points in subjects with type 2 di-
abetes: the Atorvastatin Study for Pre-
vention of Coronary Heart Disease
Endpoints in non-insulin-dependent di-
abetes mellitus (ASPEN). Diabetes Care
2006;29:14781485
217. Singh IM, Shishehbor MH, Ansell BJ.
High-density lipoprotein as a therapeu-
tic target: a systematic review. JAMA
2007;298:786798
218. Canner PL, Berge KG, Wenger NK,
Stamler J, Friedman L, Prineas RJ,
Friedewald W. Fifteen year mortality in
Coronary Drug Project patients: long-
term benet with niacin. J Am Coll Car-
diol 1986;8:12451255
219. Rubins HB, Robins SJ, Collins D, Fye CL,
Anderson JW, Elam MB, Faas FH, Lin-
ares E, Schaefer EJ, Schectman G, Wilt
TJ, Wittes J. Gembrozil for the second-
ary prevention of coronary heart disease
in men with low levels of high-density
lipoprotein cholesterol. Veterans Affairs
High-Density Lipoprotein Cholesterol
Intervention Trial Study Group. N Engl
J Med 1999;341:410418
220. Frick MH, Elo O, Haapa K, Heinonen
OP, Heinsalmi P, Helo P, Huttunen JK,
Kaitaniemi P, Koskinen P, Manninen V:
Helsinki Heart Study: primary-preven-
tion trial with gembrozil in middle-
aged men with dyslipidemia: safety of
treatment, changes in risk factors, and
incidence of coronary heart disease.
N Engl J Med 1987;317:12371245
221. Keech A, Simes RJ, Barter P, Best J, Scott
R, Taskinen MR, Forder P, Pillai A, Davis
T, Glasziou P, Drury P, Kesa niemi YA,
Sullivan D, Hunt D, Colman P, dEmden
M, Whiting M, Ehnholm C, Laakso M,
FIELD study investigators. Effects of
long-termfenobrate therapy on cardio-
vascular events in 9795 people with type
2 diabetes mellitus (the FIELD study):
randomised controlled trial. Lancet
2005;366:18491861
222. Expert Panel on Detection, Evaluation,
and Treatment of High Blood Choles-
terol in Adults: Executive Summary of
The Third Report of The National Cho-
lesterol Education Program (NCEP) Ex-
pert Panel on Detection, Evaluation,
Position Statement
And Treatment of High Blood Choles-
terol In Adults (Adult Treatment Panel
III). JAMA 2001;285:24862497
223. Hayward RA, Hofer TP, Vijan S. Nar-
rative review: lack of evidence for rec-
ommended low-density lipoprotein
treatment targets: a solvable problem.
Ann Intern Med 2006;145:520530
224. Cannon CP, Braunwald E, McCabe CH,
Rader DJ, Rouleau JL, Belder R, Joyal SV,
Hill KA, Pfeffer MA, Skene AM, Prava-
statin or Atorvastatin Evaluation and
Infection Therapy-Thrombolysis in
Myocardial Infarction 22 Investigators.
Intensive versus moderate lipid lowering
with statins after acute coronary syn-
dromes. N Engl J Med 2004;350:1495
1504
225. de Lemos JA, Blazing MA, Wiviott SD,
Lewis EF, Fox KA, White HD, Rouleau
JL, Pedersen TR, Gardner LH, Mukher-
jee R, Ramsey KE, Palmisano J, Bilhei-
mer DW, Pfeffer MA, Califf RM,
Braunwald E, A to Z Investigators. Early
intensive vs a delayed conservative sim-
vastatin strategy in patients with acute
coronary syndromes: phase Z of the A to
Z trial. JAMA 2004;292:13071316
226. Nissen SE, Tuzcu EM, Schoenhagen P,
Brown BG, Ganz P, Vogel RA, Crowe T,
Howard G, Cooper CJ, Brodie B, Grines
CL, DeMaria AN, REVERSAL Investiga-
tors. Effect of intensive compared with
moderate lipid-lowering therapy on pro-
gression of coronary atherosclerosis: a
randomized controlled trial. JAMA
2004;291:10711080
227. Grundy SM, Cleeman JI, Merz CN,
Brewer HB Jr, Clark LT, Hunninghake
DB, Pasternak RC, Smith SCJr, Stone NJ,
National Heart, Lung, and Blood Institute,
American College of Cardiology Founda-
tion, American Heart Association. Impli-
cations of recent clinical trials for the
National Cholesterol Education Program
Adult Treatment Panel III guidelines. Cir-
culation 2004;110:227239
228. Chasman DI, Posada D, Subrahmanyan
L, Cook NR, Stanton VP, Jr, Ridker PM.
Pharmacogenetic study of statin therapy
and cholesterol reduction. JAMA 2004;
291:28212827
229. Baigent C, Keech A, Kearney PM, Black-
well L, Buck G, Pollicino C, Kirby A,
Sourjina T, Peto R, Collins R, Simes R,
Cholesterol Treatment Trialists (CTT)
Collaborators. Efcacy and safety of
cholesterol-lowering treatment: pro-
spective meta-analysis of data from
90,056 participants in 14 randomised
trials of statins. Lancet 2005;366:1267
1278
230. Elam MB, Hunninghake DB, Davis KB,
Garg R, Johnson C, Egan D, Kostis JB,
Sheps DS, Brinton EA. Effect of niacin on
lipid and lipoprotein levels and glycemic
control in patients with diabetes and pe-
ripheral arterial disease: the ADMIT
study: A randomized trial. Arterial Dis-
ease Multiple Intervention Trial. JAMA
2000;284:12631270
231. Grundy SM, Vega GL, McGovern ME,
Tulloch BR, Kendall DM, Fitz-Patrick D,
Ganda OP, Rosenson RS, Buse JB, Rob-
ertson DD, Sheehan JP, Diabetes Multi-
center Research Group. Efcacy, safety,
and tolerability of once-daily niacin for
the treatment of dyslipidemia associated
with type 2 diabetes: results of the as-
sessment of diabetes control and evalu-
ation of the efcacy of niaspan trial. Arch
Intern Med 2002;162:15681576
232. Jones PH, Davidson MH. Reporting rate
of rhabdomyolysis with fenobrate
statin versus gembrozil any statin.
Am J Cardiol 2005;95:120122
233. Brunzell JD, Davidson M, Furberg CD,
Goldberg RB, Howard BV, Stein JH, Wit-
ztumJL, American Diabetes Association,
American College of Cardiology Foun-
dation. Lipoprotein management in
patients with cardiometabolic risk: con-
sensus statement from the American Di-
abetes Association and the American
College of Cardiology Foundation. Dia-
betes Care 2008;31:811822
234. Colhoun HM, Betteridge DJ, Durrington
PN, Hitman GA, Neil HA, Livingstone SJ,
Thomason MJ, Mackness MI, Charlton-
Menys V, Fuller JH, CARDS investigators.
Primary prevention of cardiovascular dis-
ease with atorvastatin in type 2 diabetes in
the Collaborative Atorvastatin Diabetes
Study (CARDS): multicentre randomised
placebo-controlledtrial. Lancet 2004;364:
685696
235. Buse JB, Ginsberg HN, Bakris GL, Clark
NG, Costa F, Eckel R, Fonseca V, Ger-
stein HC, Grundy S, Nesto RW, Pignone
MP, Plutzky J, Porte D, Redberg R, Stit-
zel KF, Stone NJ, American Heart Asso-
ciation, American Diabetes Association.
Primary prevention of cardiovascular
diseases in people with diabetes melli-
tus: a scientic statement from the
American Heart Association and the
tes Care 2007;30:162172
236. Antithrombotic Trialists (ATT) Collab-
oration, Baigent C, Blackwell L, Collins
R, Emberson J, Godwin J, Peto R, Buring
J, Hennekens C, Kearney P, Meade T,
Patrono C, Roncaglioni MC, Zanchetti
A. Aspirin in the primary and secondary
prevention of vascular disease: collabo-
rative meta-analysis of individual partic-
ipant data from randomised trials.
Lancet 2009;373:18491860
237. Wolff T, Miller T, Ko S. Aspirin for the
primary prevention of cardiovascular
events: an update of the evidence for the
U.S. Preventive Services Task Force.
238. US Preventive Services Task Force: As-
pirin for the prevention of cardiovascu-
lar disease: U.S. Preventive Services Task
Force recommendation statement. Ann
Intern Med 2009;150:396404
239. Ogawa H, Nakayama M, Morimoto T,
Uemura S, Kanauchi M, Doi N, Jinnou-
chi H, Sugiyama S, Saito Y, Japanese Pri-
mary Prevention of Atherosclerosis With
Aspirin for Diabetes (JPAD) Trial Inves-
tigators. Low-dose aspirin for primary
prevention of atherosclerotic events in
patients with type 2 diabetes: a random-
ized controlled trial. JAMA 2008;300:
21342141
240. Belch J, MacCuish A, Campbell I, Cobbe
S, Taylor R, Prescott R, Lee R, Bancroft J,
MacEwan S, Shepherd J, Macfarlane P,
Morris A, Jung R, Kelly C, Connacher A,
Peden N, Jamieson A, Matthews D, Leese
G, McKnight J, OBrien I, Semple C, Pet-
rie J, Gordon D, Pringle S, MacWalter R.
The prevention of progression of arterial
disease and diabetes (POPADAD) trial:
factorial randomised placebo controlled
trial of aspirin and antioxidants in pa-
tients with diabetes and asymptomatic
peripheral arterial disease. BMJ 2008;
337:a1840
241. Pignone M, Earnshaw S, Tice JA,
Pletcher MJ. Aspirin, statins, or both
drugs for the primary prevention of cor-
onary heart disease events in men: a
cost-utility analysis. Ann Intern Med
2006;144:326336
242. Campbell CL, Smyth S, Montalescot G,
Steinhubl SR. Aspirin dose for the pre-
vention of cardiovascular disease: a sys-
tematic review. JAMA 2007;297:2018
2024
243. Dav G, Patrono C. Platelet activation
and atherothrombosis. N Engl J Med
2007;357:24822494
244. Watala C, Golanski J, Pluta J, Boncler M,
Rozalski M, Luzak B, Kropiwnicka A,
Drzewoski J. Reduced sensitivity of
platelets from type 2 diabetic patients to
acetylsalicylic acid (aspirin)-its relation
to metabolic control. Thromb Res 2004;
113:101113
245. Lev EI. Aspirin resistance transient lab-
oratory nding or important clinical en-
tity? J Am Coll Cardiol 2009;53:678
680
246. Santilli F, Rocca B, De Cristofaro R, Lat-
tanzio S, Pietrangelo L, Habib A, Petti-
nella C, Recchiuti A, Ferrante E,
Ciabattoni G, Dav G, Patrono C. Platelet
cyclooxygenase inhibition by low-dose
aspirin is not reected consistently by
platelet function assays: implications for
aspirin resistance. J Am Coll Cardiol
2009;53:667677
247. Bhatt DL, Marso SP, Hirsch AT, Ringleb
PA, Hacke W, Topol EJ. Amplied ben-
et of clopidogrel versus aspirin in pa-
tients with diabetes mellitus. Am J
Cardiol 2002;90:625628
248. Haire-Joshu D, Glasgow RE, Tibbs TL.
Smoking and diabetes. Diabetes Care
1999;22:18871898
249. American Diabetes Asociation: Smoking
and diabetes (Position Statement). Dia-
betes Care 2004;27(Suppl. 1):S74S75
250. US Preventive Services Task Force.
Counseling to Prevent Tobacco Use and To-
bacco-Related Diseases: Recommendation
Statement. Rockville, MD, Agency for
Healthcare Research and Quality, 2003
251. Ranney L, Melvin C, Lux L, McClain E,
Lohr KN. Systematic review: smoking
cessation intervention strategies for
adults and adults in special populations.
252. Scognamiglio R, Negut C, Ramondo A,
Tiengo A, Avogaro A. Detection of coro-
nary artery disease in asymptomatic pa-
tients with type 2 diabetes mellitus. J Am
Coll Cardiol 2006;47:6571
253. Boden WE, ORourke RA, Teo KK, Har-
tigan PM, Maron DJ, Kostuk WJ, Knudt-
son M, Dada M, Casperson P, Harris CL,
Chaitman BR, Shaw L, Gosselin G,
Nawaz S, Title LM, Gau G, Blaustein AS,
Booth DC, Bates ER, Spertus JA, Berman
DS, Mancini GB, Weintraub WS,
COURAGE Trial Research Group. Opti-
mal medical therapy with or without PCI
for stable coronary disease. NEngl J Med
2007;356:15031516
254. BARI 2D Study Group, Frye RL, August
P, Brooks MM, Hardison RM, Kelsey SF,
MacGregor JM, Orchard TJ, Chaitman
BR, Genuth SM, Goldberg SH, Hlatky
MA, Jones TL, Molitch ME, Nesto RW,
Sako EY, Sobel BE. A randomized trial of
therapies for type 2 diabetes and coro-
nary artery disease. N Engl J Med 2009;
360:25032515
255. Wackers FJ, Chyun DA, Young LH,
Heller GV, Iskandrian AE, Davey JA,
Barrett EJ, Taillefer R, Wittlin SD, Filip-
chuk N, Ratner RE, Inzucchi SE: Reso-
lution of asymptomatic myocardial
ischemia in patients with type 2 diabetes
mellitus in the DIAD Study. Diabetes
Care 2007;30:28922898
256. Young LH, Wackers FJ, Chyun DA,
Davey JA, Barrett EJ, Taillefer R, Heller
GV, Iskandrian AE, Wittlin SD, Filip-
chuk N, Ratner RE, Inzucchi SE, DIAD
Investigators. Cardiac outcomes after
screening for asymptomatic coronary ar-
tery disease in patients with type 2 dia-
betes: the DIAD study: a randomized
controlled trial. JAMA 2009;301:1547
1555
257. Braunwald E, Domanski MJ, Fowler SE,
Geller NL, Gersh BJ, Hsia J, Pfeffer MA,
Rice MM, Rosenberg YD, Rouleau JL,
PEACE Trial Investigators. Angiotensin-
converting-enzyme inhibition in stable
coronary artery disease. N Engl J Med
2004;351:20582068
258. Effects of the angiotensin-receptor
blocker telmisartan on cardiovascular
events in high-risk patients intolerant to
angiotensin-converting enzyme inhibi-
tors: a randomised controlled trial. Lan-
cet 2008;372:11741183
259. Garg JP, Bakris GL. Microalbuminuria:
marker of vascular dysfunction, risk fac-
tor for cardiovascular disease. Vasc Med
2002;7:3543
260. Klausen K, Borch-Johnsen K, Feldt-Ras-
mussen B, Jensen G, Clausen P,
Scharling H, Appleyard M, Jensen JS.
Very low levels of microalbuminuria are
associated with increased risk of coro-
nary heart disease and death indepen-
dently of renal function, hypertension,
and diabetes. Circulation 2004;110:
3235
261. Gall MA, Hougaard P, Borch-Johnsen K,
Parving HH. Risk factors for develop-
ment of incipient and overt diabetic ne-
phropathy in patients with non-insulin
dependent diabetes mellitus: prospec-
tive, observational study. BMJ 1997;314:
783788
262. Ravid M, Lang R, Rachmani R, Lishner
M. Long-term renoprotective effect of
angiotensin-converting enzyme inhibi-
tion in non-insulin-dependent diabetes
mellitus. A 7-year follow-up study. Arch
Intern Med 1996;156:286289
263. Reichard P, Nilsson BY, Rosenqvist U. The
effect of long-term intensied insulin
treatment on the development of micro-
vascular complications of diabetes melli-
tus. N Engl J Med 1993;329:304309
264. Effect of intensive therapy on the devel-
opment and progression of diabetic ne-
phropathy in the Diabetes Control and
Complications Trial. The Diabetes Con-
trol and Complications (DCCT) Re-
search Group. Kidney Int 1995;47:
17031720
265. Lewis EJ, Hunsicker LG, Bain RP, Rohde
RD. The effect of angiotensin-convert-
ing-enzyme inhibition on diabetic ne-
phropathy. The Collaborative Study
Group. N Engl J Med 1993;329:1456
1462
266. Remuzzi G, Macia M, Ruggenenti P. Pre-
vention and treatment of diabetic renal
disease in type 2 diabetes: the BENE-
DICT study. JAmSocNephrol 2006;17:
S90S97
267. Bilous R, Chaturvedi N, Sjlie AK, Fuller
J, Klein R, Orchard T, Porta M, Parving
HH. Effect of candesartan on microalbu-
minuria and albumin excretion rate in
diabetes: three randomized trials. Ann
Intern Med 2009;151:1114
268. Mauer M, Zinman B, Gardiner R, Suissa
S, Sinaiko A, Strand T, Drummond K,
Donnelly S, Goodyer P, Gubler MC,
Klein R. Renal and retinal effects of ena-
lapril and losartan in type 1 diabetes.
N Engl J Med 2009;361:4051
269. Lewis EJ, Hunsicker LG, Clarke WR,
Berl T, Pohl MA, Lewis JB, Ritz E, Atkins
RC, Rohde R, Raz I, Collaborative Study
Group. Renoprotective effect of the an-
giotensin-receptor antagonist irbesartan
in patients with nephropathy due to type
2 diabetes. NEngl J Med 2001;345:851
860
270. Brenner BM, Cooper ME, de Zeeuw D,
Keane WF, Mitch WE, Parving HH, Re-
muzzi G, Snapinn SM, Zhang Z, Shahin-
far S, RENAAL Study Investigators.
Effects of losartan on renal and cardio-
vascular outcomes in patients with type
2 diabetes and nephropathy. N Engl
J Med 2001;345:861869
271. Parving HH, Lehnert H, Bro chner-
Mortensen J, Gomis R, Andersen S,
Arner P, Irbesartan in Patients with Type
2 Diabetes and Microalbuminuria Study
Group. The effect of irbesartan on the
development of diabetic nephropathy in
patients with type 2 diabetes. N Engl
J Med 2001;345:870878
272. Pepine CJ, Handberg EM, Cooper-De-
Hoff RM, Marks RG, Kowey P, Messerli
FH, Mancia G, Cangiano JL, Garcia-Bar-
reto D, Keltai M, Erdine S, Bristol HA,
Kolb HR, Bakris GL, Cohen JD, Parmley
WW, INVEST Investigators. A calcium
antagonist vs a non-calcium antagonist
hypertension treatment strategy for pa-
tients with coronary artery disease: the
International Verapamil-Trandolapril
study (INVEST): a randomized con-
trolled trial. JAMA 2003;290:2805
2816
273. Bakris GL, Siomos M, Richardson D,
Janssen I, Bolton WK, Hebert L, Agarwal
R, Catanzaro D. ACE inhibition or an-
giotensin receptor blockade: impact on
potassium in renal failure. VAL-K Study
Group. Kidney Int 2000;58:20842092
274. Mogensen CE, Neldam S, Tikkanen I,
Oren S, Viskoper R, Watts RW, Cooper
ME. Randomised controlled trial of dual
blockade of renin-angiotensin system in
patients with hypertension, microalbu-
minuria, and non-insulin dependent di-
abetes: the candesartan and lisinopril
microalbuminuria (CALM) study. BMJ
2000;321:14401444
275. Schjoedt KJ, Jacobsen P, Rossing K,
Boomsma F, Parving HH. Dual blockade
of the renin-angiotensin-aldosterone
system in diabetic nephropathy: the role
of aldosterone. Horm Metab Res 2005;
37(Suppl. 1):48
276. Schjoedt KJ, Rossing K, Juhl TR,
Boomsma F, Rossing P, Tarnow L, Parv-
ing HH. Benecial impact of spironolac-
tone in diabetic nephropathy. Kidney
Int 2005;68:28292836
277. Parving HH, Persson F, Lewis JB, Lewis
EJ, Hollenberg NK, AVOIDStudy Inves-
tigators. Aliskiren combined with losar-
tan in type 2 diabetes and nephropathy.
N Engl J Med 2008;358:24332446
278. Pijls LT, de Vries H, Donker AJ, van Eijk
JT. The effect of protein restriction on
albuminuria in patients with type 2 dia-
betes mellitus: a randomized trial.
Nephrol Dial Transplant 1999;14:1445
1453
Position Statement
279. Pedrini MT, Levey AS, Lau J, Chalmers
TC, Wang PH. The effect of dietary pro-
tein restriction on the progression of di-
abetic and nondiabetic renal diseases: a
meta-analysis. Ann Intern Med 1996;
124:627632
280. Hansen HP, Tauber-Lassen E, Jensen
BR, Parving HH. Effect of dietary protein
restriction on prognosis in patients with
diabetic nephropathy. Kidney Int 2002;
62:220228
281. Kasiske BL, Lakatua JD, Ma JZ, Louis TA.
A meta-analysis of the effects of dietary
protein restriction on the rate of decline
in renal function. AmJ Kidney Dis 1998;
31:954961
282. Eknoyan G, Hostetter T, Bakris GL, He-
bert L, Levey AS, Parving HH, Steffes
MW, Toto R. Proteinuria and other
markers of chronic kidney disease: a po-
sition statement of the national kidney
foundation (NKF) and the national insti-
tute of diabetes and digestive and kidney
diseases (NIDDK). Am J Kidney Dis
2003;42:617622
283. Levey AS, Coresh J, Balk E, Kausz AT,
Levin A, Steffes MW, Hogg RJ, Perrone
RD, Lau J, Eknoyan G, National Kidney
Foundation. National Kidney Founda-
tion practice guidelines for chronic kid-
ney disease: evaluation, classication,
and stratication. Ann Intern Med 2003;
139:137147
284. Kramer H, Molitch ME. Screening for
kidney disease in adults with diabetes.
285. Kramer HJ, Nguyen QD, Curhan G, Hsu
CY. Renal insufciency in the absence of
albuminuria and retinopathy among
adults with type 2 diabetes mellitus.
JAMA 2003;289:32733277
286. Tsalamandris C, Allen TJ, Gilbert RE,
Sinha A, Panagiotopoulos S, Cooper ME,
Jerums G. Progressive decline in renal
function in diabetic patients with and
without albuminuria. Diabetes 1994;43:
649655
287. Levey AS, Bosch JP, Lewis JB, Greene T,
Rogers N, Roth D. A more accurate
method to estimate glomerular ltration
rate from serum creatinine: a new pre-
diction equation. Modication of Diet in
Renal Disease Study Group. Ann Intern
Med 1999;130:461470
288. Rigalleau V, Lasseur C, Perlemoine C,
Barthe N, Raffaitin C, Liu C, Chauveau
P, Baillet-Blanco L, Beauvieux MC,
Combe C, Gin H. Estimation of glomer-
ular ltration rate in diabetic subjects:
Cockcroft formula or modication of
Diet in Renal Disease study equation?
289. Levinsky NG. Specialist evaluation in
chronic kidney disease: too little, too
late. Ann Intern Med 2002;137:542
543
290. American Diabetes Association: Ne-
phropathy in diabetes (Position State-
1):S79S83
291. Klein R. Hyperglycemia and microvas-
cular and macrovascular disease in dia-
betes. Diabetes Care 1995;18:258268
292. Estacio RO, McFarling E, Biggerstaff S,
Jeffers BW, Johnson D, Schrier RW.
Overt albuminuria predicts diabetic ret-
inopathy in Hispanics with NIDDM.
Am J Kidney Dis 1998;31:947953
293. Leske MC, Wu SY, Hennis A, Hyman L,
Nemesure B, Yang L, Schachat AP, Bar-
bados Eye Study Group. Hyperglycemia,
blood pressure, and the 9-year incidence
of diabetic retinopathy: the Barbados
Eye Studies. Ophthalmology 2005;112:
799805
294. Fong DS, Aiello LP, Ferris FL 3rd, Klein
R. Diabetic retinopathy. Diabetes Care
2004;27:25402553
295. Diabetes Control and Complications
Trial Research Group: Effect of preg-
nancy on microvascular complications
in the diabetes control and complica-
tions trial. The Diabetes Control and
Complications Trial Research Group.
296. The Diabetic Retinopathy Study (DRS)
Research Group. Preliminary report on
the effects of photocoagulation therapy:
DRS Report #1. AmJ Ophthalmol 1976;
81:383396.
297. Photocoagulation for diabetic macular
edema. Early Treatment Diabetic Reti-
nopathy Study report number 1. Early
Treatment Diabetic Retinopathy Study
research group. Arch Ophthalmol 1985;
103:17961806
298. Klein R, Klein BE, Moss SE, Davis MD,
DeMets DL. The Wisconsinepidemiologic
study of diabetic retinopathy. II. Preva-
lence and risk of diabetic retinopathy
when age at diagnosis is less than 30 years.
Arch Ophthalmol 1984;102:520526
299. Harris MI, Klein R, Welborn TA,
Knuiman MW. Onset of NIDDM occurs
at least 47 yr before clinical diagnosis.
300. Vijan S, Hofer TP, Hayward RA. Cost-
utility analysis of screening intervals for
diabetic retinopathy in patients with
type 2 diabetes mellitus. JAMA 2000;
283:889896
301. Klein R. Screening interval for retinopa-
thy in type 2 diabetes. Lancet 2003;361:
190191
302. Younis N, Broadbent DM, Vora JP, Har-
ding SP, Liverpool Diabetic Eye Study.
Incidence of sight-threatening retinopa-
thy in patients with type 2 diabetes in the
Liverpool Diabetic Eye Study: a cohort
study. Lancet 2003;361:195200
303. Ahmed J, Ward TP, Bursell SE, Aiello
LM, Cavallerano JD, Vigersky RA. The
sensitivity and specicity of nonmydri-
atic digital stereoscopic retinal imaging
in detecting diabetic retinopathy. Diabe-
tes Care 2006;29:22052209
304. American Diabetes Association: Reti-
nopathy in diabetes. Diabetes Care
2004;27 Suppl. 1:S84S87
305. Ciulla TA, Amador AG, Zinman B. Dia-
betic retinopathy and diabetic macular
edema: pathophysiology, screening, and
novel therapies. Diabetes Care 2003;26:
26532664
306. Boulton AJ, Vinik AI, Arezzo JC, Bril V,
Feldman EL, Freeman R, Malik RA, Ma-
ser RE, Sosenko JM, Ziegler D, American
Diabetes Association. Diabetic neuropa-
thies: a statement by the American Dia-
betes Association. Diabetes Care 2005;
28:956962
307. Vinik AI, Maser RE, Mitchell BD, Free-
man R. Diabetic autonomic neuropathy.
308. Boulton AJ, Armstrong DG, Albert SF,
Frykberg RG, Hellman R, Kirkman MS,
Lavery LA, Lemaster JW, Mills JL Sr,
Mueller MJ, Sheehan P, Wukich DK,
American Diabetes Association, Ameri-
can Association of Clinical Endocrinolo-
gists. Comprehensive foot examination
and risk assessment: a report of the task
force of the foot care interest group of
the American Diabetes Association, with
endorsement by the American Associa-
tion of Clinical Endocrinologists. Diabe-
tes Care 2008;31:16791685
309. American Diabetes Association: Periph-
eral arterial disease in people with dia-
betes (Consensus Statement). Diabetes
Care 2003;26:33333341
310. American Diabetes Association: Consen-
sus Development Conference on Dia-
betic Foot Wound Care, 78 April
1999, Boston, Massachusetts. Diabetes
Care 1999;22:13541360
311. Silverstein J, Klingensmith G, Copeland
KC, Plotnick L, Kaufman F, Laffel L,
Deeb LC, Grey M, Anderson BJ, Hol-
zmeister LA, and Clark NG Care of chil-
dren and adolescents with type 1
diabetes mellitus: A statement of the
tes Care 2005; 28:186212.
312. NorthamEA, Anderson PJ, Werther GA,
Warne GL, Adler RG, Andrewes D. Neu-
ropsychological complications of IDDM
in children 2 years after disease onset.
313. Rovet J, Alvarez M. Attentional function-
ing in children and adolescents with
IDDM. Diabetes Care 1997;20:803810
314. Bjrgaas M, Gimse R, Vik T, Sand T.
Cognitive function in type 1 diabetic
children with and without episodes of
severe hypoglycaemia. Acta Paediatr
1997;86:148153
315. Doyle EA, Weinzimer SA, Steffen AT,
Ahern JA, Vincent M, Tamborlane WV.
Arandomized, prospective trial compar-
ing the efcacy of continuous subcuta-
neous insulin infusion with multiple
daily injections using insulin glargine.
316. Nimri R, Weintrob N, Benzaquen H,
Ofan R, Fayman G, Phillip M. Insulin
pump therapy in youth with type 1 dia-
betes: a retrospective paired study. Pedi-
atrics 2006;117:21262131
317. Krantz JS, Mack WJ, Hodis HN, Liu CR,
Liu CH, Kaufman FR. Early onset of sub-
clinical atherosclerosis in young persons
with type 1 diabetes. J Pediatr 2004;145:
452457
318. Ja rvisalo MJ, Putto-Laurila A, Jartti L,
Lehtima ki T, Solakivi T, Ro nnemaa T,
Raitakari OT. Carotid artery intima-me-
dia thickness in children with type 1 di-
abetes. Diabetes 2002;51:493498
319. Haller MJ, Samyn M, Nichols WW,
Brusko T, Wasserfall C, Schwartz RF, At-
kinson M, Shuster JJ, Pierce GL, Silver-
stein JH. Radial artery tonometry
demonstrates arterial stiffness in chil-
dren with type 1 diabetes. Diabetes Care
2004;27:29112917
320. Orchard TJ, Forrest KY, Kuller LH,
Becker DJ, Pittsburgh Epidemiology of
Diabetes Complications Study. Lipid
and blood pressure treatment goals for
type 1 diabetes: 10-year incidence data
fromthe Pittsburgh Epidemiology of Di-
abetes Complications Study. Diabetes
Care 2001;24:10531059
321. Kavey RE, Allada V, Daniels SR, Hayman
LL, McCrindle BW, Newburger JW,
Parekh RS, Steinberger J, American
Heart Association Expert Panel on Pop-
ulation and Prevention Science, Ameri-
can Heart Association Council on
Cardiovascular Disease in the Young,
American Heart Association Council on
Epidemiology and Prevention, Ameri-
can Heart Association Council on Nutri-
tion, Physical Activity and Metabolism,
American Heart Association Council on
High Blood Pressure Research, Ameri-
can Heart Association Council on Car-
diovascular Nursing, American Heart
Association Council on the Kidney in
Heart Disease, Interdisciplinary Work-
ing Group on Quality of Care and Out-
comes Research. Cardiovascular risk
reduction in high-risk pediatric patients:
a scientic statement from the American
Heart Association Expert Panel on Pop-
ulation and Prevention Science; the
Councils on Cardiovascular Disease in
the Young, Epidemiology and Preven-
tion, Nutrition, Physical Activity and
Metabolism, High Blood Pressure Re-
search, Cardiovascular Nursing, and the
Kidney in Heart Disease; and the Inter-
disciplinary Working Group on Quality
of Care and Outcomes Research: en-
dorsed by the American Academy of Pe-
diatrics. Circulation 2006;114:2710
2738
322. McCrindle BW, Urbina EM, Dennison
BA, Jacobson MS, Steinberger J, Roc-
chini AP, Hayman LL, Daniels SR, Amer-
ican Heart Association Atherosclerosis,
Hypertension, and Obesity in Youth
Committee, American Heart Association
Council of Cardiovascular Disease in the
Young, American Heart Association
Council on Cardiovascular Nursing.
Drug therapy of high-risk lipid abnor-
malities in children and adolescents: a
scientic statement from the American
Heart Association Atherosclerosis, Hy-
pertension, and Obesity in Youth Com-
mittee, Council of Cardiovascular
Disease in the Young, with the Council
on Cardiovascular Nursing. Circulation
2007;115:19481967
323. Salo P, Viikari J, Ha ma la inen M, Lapin-
leimu H, Routi T, Ro nnemaa T, Sep-
pa nen R, Jokinen E, Va lima ki I, Simell
O. Serum cholesterol ester fatty acids in
7- and 13-month-old children in a pro-
spective randomized trial of a low-satu-
rated fat, low-cholesterol diet: the STRIP
baby project. Special Turku coronary
Risk factor Intervention Project for chil-
dren. Acta Paediatr 1999;88:505512
324. Efcacy and safety of lowering dietary
intake of fat and cholesterol in children
with elevated low-density lipoprotein
cholesterol. The Dietary Intervention
Study in Children (DISC). The Writing
Group for the DISC Collaborative Re-
search Group. JAMA 1995;273:1429
1435
325. McCrindle BW, Ose L, Marais AD. Ef-
cacy and safety of atorvastatin in chil-
dren and adolescents with familial
hypercholesterolemia or severe hyper-
lipidemia: a multicenter, randomized,
placebo-controlled trial. J Pediatr 2003;
143:7480
326. de Jongh S, Lilien MR, opt RJ, Stroes ES,
Bakker HD, Kastelein JJ. Early statin
therapy restores endothelial function in
children with familial hypercholesterol-
emia. J Am Coll Cardiol 2002;40:2117
2121
327. Wiegman A, Hutten BA, de Groot E, Ro-
denburg J, Bakker HD, Bu ller HR, Si-
jbrands EJ, Kastelein JJ. Efcacy and
safety of statin therapy in children with
familial hypercholesterolemia: a ran-
domized controlled trial. JAMA 2004;
292:331337
328. Holmes GK. Screening for coeliac dis-
ease in type 1 diabetes. Arch Dis Child
2002;87:495498
329. Rewers M, Liu E, Simmons J, Redondo
MJ, Hoffenberg EJ: Celiac disease asso-
ciated with type 1 diabetes mellitus. En-
docrinol Metab Clin North Am2004;33:
197214, xi
330. Roldan MB, Alonso M, Barrio R. Thyroid
autoimmunity in children and adoles-
cents with Type 1 diabetes mellitus. Di-
abetes Nutr Metab 1999;12:2731
331. Kordonouri O, Deiss D, Danne T,
Dorow A, Bassir C, Gru ters-Kieslich A.
Predictivity of thyroid autoantibodies
for the development of thyroid disorders
in children and adolescents with Type 1
diabetes. Diabet Med 2002;19:518521
332. Mohn A, Di Michele S, Di Luzio R,
Tumini S, Chiarelli F. The effect of sub-
clinical hypothyroidism on metabolic
control in children and adolescents with
Type 1 diabetes mellitus. Diabet Med
2002;19:7073
333. Chase HP, Garg SK, Cockerham RS,
Wilcox WD, Walravens PA. Thyroid
hormone replacement and growth of
children with subclinical hypothyroid-
ism and diabetes. Diabet Med 1990;7:
299303
334. Eppens MC, Craig ME, Cusumano J,
Hing S, Chan AK, Howard NJ, Silink M,
Donaghue KC. Prevalence of diabetes
complications in adolescents with type 2
compared with type 1 diabetes. Diabetes
Care 2006;29:13001306
335. Kitzmiller JL, Gavin LA, Gin GD, Jo-
vanovic-Peterson L, Main EK, Zigrang
WD. Preconception care of diabetes.
Glycemic control prevents congenital
anomalies. JAMA 1991;265:731736
336. Goldman JA, Dicker D, Feldberg D, Ye-
shaya A, Samuel N, Karp M. Pregnancy
outcome in patients with insulin-depen-
dent diabetes mellitus with preconcep-
tional diabetic control: a comparative
study. AmJ Obstet Gynecol 1986;155:
293297
337. Rosenn B, Miodovnik M, Combs CA,
Khoury J, Siddiqi TA. Pre-conception
management of insulin-dependent dia-
betes: improvement of pregnancy out-
come. Obstet Gynecol 1991;77:846
849
338. Tchobroutsky C, Vray MM, Altman JJ.
Risk/benet ratio of changing late ob-
stetrical strategies in the management of
insulin-dependent diabetic pregnancies.
A comparison between 19711977 and
19781985 periods in 389 pregnancies.
Diabete Metab 1991;17:287294
339. Willhoite MB, Bennert HW, Jr, Palomaki
GE, Zaremba MM, Herman WH, Wil-
liams JR, Spear NH. The impact of pre-
conception counseling on pregnancy
outcomes. The experience of the Maine
Diabetes in Pregnancy Program. Diabe-
tes Care 1993;16:450455
340. Cooper WO, Hernandez-Diaz S, Arbo-
gast PG, Dudley JA, Dyer S, Gideon PS,
Hall K, Ray WA. Major congenital mal-
formations after rst-trimester exposure
to ACE inhibitors. N Engl J Med 2006;
354:24432451
341. American Diabetes Association: Precon-
ception care of women with diabetes
(Position Statement). Diabetes Care
2004;27(Suppl. 1):S76S78
342. Brown AF, Mangione CM, Saliba D,
Sarkisian CA, California Healthcare
Foundation/American Geriatrics Society
Panel on Improving Care for Elders with
Diabetes. Guidelines for improving the
care of the older person with diabetes
Position Statement
mellitus. J Am Geriatr Soc 2003;51:
S265S280
343. Curb JD, Pressel SL, Cutler JA, Savage
PJ, Applegate WB, Black H, Camel G,
Davis BR, Frost PH, Gonzalez N, Guthrie
G, Oberman A, Rutan GH, Stamler J. Ef-
fect of diuretic-based antihypertensive
treatment on cardiovascular disease risk
in older diabetic patients with isolated
systolic hypertension. Systolic Hyper-
tension in the Elderly Program Cooper-
ative Research Group. JAMA 1996;276:
18861892
344. Beckett NS, Peters R, Fletcher AE, Staes-
sen JA, Liu L, Dumitrascu D, Stoyanovsky
V, Antikainen RL, Nikitin Y, Anderson C,
Belhani A, Forette F, Rajkumar C, Thijs L,
Banya W, Bulpitt CJ, HYVET Study
Group. Treatment of hypertension in pa-
tients 80 years of age or older. N Engl
J Med 2008;358:18871898
345. Clement S, Braithwaite SS, Magee MF,
Ahmann A, Smith EP, Schafer RG, Hir-
sch IB, Hirsh IB, American Diabetes As-
sociation Diabetes in Hospitals Writing
Committee. Management of diabetes
and hyperglycemia in hospitals. Diabe-
tes Care 2004;27:553591
346. Moghissi ES, Korytkowski MT, DiNardo
M, Einhorn D, Hellman R, Hirsch IB, In-
zucchi SE, Ismail-Beigi F, Kirkman MS,
Umpierrez GE, American Association of
Clinical Endocrinologists, American
Diabetes Association. American Asso-
ciation of Clinical Endocrinologists
and American Diabetes Association
consensus statement on inpatient gly-
cemic control. Diabetes Care 2009;32:
11191131
347. American Diabetes Association: Eco-
nomic costs of diabetes in the U.S. In
2007. Diabetes Care 2008;31:596615
348. Centers for Disease Control and Preven-
tion. National Diabetes Fact Sheet: Gen-
eral Information and National Estimates on
Diabetes in the United States, 2007. At-
lanta, GA, US Department of Health and
Human Services, 2008
349. Levetan CS, Passaro M, Jablonski K, Kass
M, Ratner RE. Unrecognized diabetes
among hospitalized patients. Diabetes
Care 1998;21:246249
350. Umpierrez GE, Isaacs SD, Bazargan N,
You X, Thaler LM, Kitabchi AE. Hyper-
glycemia: an independent marker of in-
hospital mortality in patients with
undiagnosed diabetes. J Clin Endocrinol
Metab 2002;87:978982
351. van den Berghe G, Wouters P, Weekers
F, Verwaest C, Bruyninckx F, Schetz M,
Vlasselaers D, Ferdinande P, Lauwers P,
Bouillon R. Intensive insulin therapy in
the critically ill patients. N Engl J Med
2001;345:13591367
352. Malmberg K, Norhammar A, Wedel H,
Ryden L. Glycometabolic state at admis-
sion: important risk marker of mortality in
conventionally treated patients with dia-
betes mellitus and acute myocardial in-
farction: long-term results from the
Diabetes and Insulin-Glucose Infusion in
Acute Myocardial Infarction (DIGAMI)
study. Circulation 1999;99:26262632
353. Wiener RS, Wiener DC, Larson RJ. Ben-
ets and risks of tight glucose control in
critically ill adults: a meta-analysis.
JAMA 2008;300:933944
354. Brunkhorst FM, Engel C, Bloos F, Meier-
Hellmann A, Ragaller M, Weiler N, Mo-
erer O, Gruendling M, Oppert M, Grond
S, Olthoff D, Jaschinski U, John S, Ros-
saint R, Welte T, Schaefer M, Kern P,
Kuhnt E, Kiehntopf M, Hartog C, Natan-
son C, Loefer M, Reinhart K, German
Competence Network Sepsis (SepNet).
Intensive insulin therapy and pen-
tastarch resuscitation in severe sepsis.
N Engl J Med 2008;358:125139
355. NICE-SUGAR Study Investigators, Fin-
fer S, Chittock DR, Su SY, Blair D, Foster
D, Dhingra V, Bellomo R, Cook D,
Dodek P, Henderson WR, He bert PC,
Heritier S, Heyland DK, McArthur C,
McDonald E, Mitchell I, Myburgh JA,
Norton R, Potter J, Robinson BG, Ronco
JJ. Intensive versus conventional glucose
control in critically ill patients. N Engl
J Med 2009;360:12831297
356. Krinsley JS, Grover A. Severe hypoglyce-
mia in critically ill patients: risk factors
and outcomes. Crit Care Med 2007;35:
22622267
357. Van den Berghe G, Wilmer A, Hermans
G, Meersseman W, Wouters PJ, Milants
I, Van Wijngaerden E, Bobbaers H,
Bouillon R. Intensive insulin therapy in
the medical ICU. N Engl J Med 2006;
354:449461
358. Griesdale DE, de Souza RJ, van DamRM,
Heyland DK, Cook DJ, Malhotra A,
Dhaliwal R, Henderson WR, Chittock
DR, Finfer S, Talmor D. Intensive insulin
therapy and mortality among critically
ill patients: a meta-analysis including
NICE-SUGAR study data. CMAJ 2009;
180:821827
359. Saudek CD, Herman WH, Sacks DB,
Bergenstal RM, Edelman D, Davidson
MB. A new look at screening and diag-
nosing diabetes mellitus. J Clin Endocri-
nol Metab 2008;93:24472453
360. Mitrakou A, Ryan C, Veneman T, Mokan
M, Jenssen T, Kiss I, Durrant J, Cryer P,
Gerich J. Hierarchy of glycemic thresholds
for counterregulatory hormone secretion,
symptoms, andcerebral dysfunction. AmJ
Physiol 1991;260:E67E74
361. Korytkowski M, DiNardo M, Donihi AC,
Bigi L, Devita M. Evolution of a diabetes
inpatient safety committee. Endocr Pract
2006;12(Suppl. 3):9199
362. DiNardo M, Noschese M, Korytkowski
M, Freeman S. The medical emergency
team and rapid response system: nd-
ing, treating, and preventing hypoglyce-
mia. Jt Comm J Qual Patient Saf 2006;
32:591595
363. Donihi AC, Raval D, Saul M, Koryt-
kowski MT, DeVita MA. Prevalence and
predictors of corticosteroid-related hy-
perglycemia in hospitalized patients.
Endocr Pract 2006;12:358362
364. Goldberg PA, Siegel MD, Sherwin RS,
Halickman JI, Lee M, Bailey VA, Lee SL,
Dziura JD, Inzucchi SE. Implementation
of a safe and effective insulin infusion
protocol in a medical intensive care unit.
365. Rea RS, Donihi AC, Bobeck M, Herout P,
McKaveney TP, Kane-Gill SL, Koryt-
kowski MT. Implementing an intrave-
nous insulin infusion protocol in the
intensive care unit. Am J Health Syst
Pharm 2007;64:385395
366. Nazer LH, Chow SL, Moghissi ES. Insu-
lin infusion protocols for critically ill pa-
tients: a highlight of differences and
similarities. Endocr Pract 2007;13:137
146
367. DeSantis AJ, Schmeltz LR, Schmidt K,
OShea-Mahler E, Rhee C, Wells A,
Brandt S, Peterson S, Molitch ME. Inpa-
tient management of hyperglycemia: the
Northwestern experience. Endocr Pract
2006;12:491505
368. Noschese M, Donihi AC, Koerbel G,
Karslioglu E, DiNardo M, Curll M, Ko-
rytkowski MT. Effect of a diabetes order
set on glycaemic management and con-
trol in the hospital. Qual Saf Health Care
2008;17:464468
369. Umpierrez GE, Hor T, Smiley D, Tem-
poni A, Umpierrez D, Ceron M, Munoz
C, Newton C, Peng L, Baldwin D. Com-
parison of inpatient insulin regimens
with detemir plus aspart versus neutral
protamine hagedorn plus regular in
medical patients with type 2 diabetes.
J Clin Endocrinol Metab 2009;94:564
569
370. Moghissi ES, Hirsch IB. Hospital man-
agement of diabetes. Endocrinol Metab
Clin North Am 2005;34:99116
371. Umpierrez GE, Smiley D, Zisman A, Pri-
eto LM, Palacio A, Ceron M, Puig A, Me-
jia R. Randomized study of basal-bolus
insulin therapy in the inpatient manage-
ment of patients with type 2 diabetes
(RABBIT2 trial). Diabetes Care 2007;30:
21812186
372. Umpierrez GE, Palacio A, Smiley D.
Sliding scale insulin use: myth or insan-
ity? Am J Med 2007;120:563567
373. Queale WS, Seidler AJ, Brancati FL. Gly-
cemic control and sliding scale insulin
use in medical inpatients with diabetes
mellitus. Arch Intern Med 1997;157:
545552
374. Korytkowski MT, Salata RJ, Koerbel GL,
Selzer F, Karslioglu E, Idriss AM, Lee
KK, Moser AJ, Toledo FG. Insulin ther-
apy and glycemic control in hospitalized
patients with diabetes during enteral nu-
trition therapy: a randomized controlled
clinical trial. Diabetes Care 2009;32:
594596
375. Hirsch IB. Sliding scale insulintime to
stop sliding. JAMA 2009;301:213214
376. Umpierrez GE. Basal versus sliding-scale
regular insulin in hospitalized patients
with hyperglycemia during enteral nu-
trition therapy. Diabetes Care 2009;32:
751753
377. Pancorbo-Hidalgo PL, Garca-Fernan-
dez FP, Ramrez-Pe rez C. Complications
associated with enteral nutrition by na-
sogastric tube in an internal medicine
unit. J Clin Nurs 2001;10:482490
378. Nylen ES, Muller B. Endocrine changes
in critical illness. J Intensive Care Med
2004;19:6782
379. Shilo S, Berezovsky S, Friedlander Y,
Sonnenblick M. Hypoglycemia in hospi-
talized nondiabetic older patients. J Am
Geriatr Soc 1998;46:978982
380. Fischer KF, Lees JA, Newman JH. Hypo-
glycemia in hospitalized patients.
Causes and outcomes. N Engl J Med
1986;315:12451250
381. Markovitz LJ, Wiechmann RJ, Harris N,
Hayden V, Cooper J, Johnson G, Harel-
stad R, Calkins L, Braithwaite SS. De-
scription and evaluation of a glycemic
management protocol for patients with
diabetes undergoing heart surgery. En-
docr Pract 2002;8:1018
382. Levetan CS, Salas JR, Wilets IF, Zumoff
B. Impact of endocrine and diabetes
team consultation on hospital length of
stay for patients with diabetes. AmJ Med
1995;99:2228
383. Levetan CS, Passaro MD, Jablonski KA,
Ratner RE. Effect of physician specialty
on outcomes in diabetic ketoacidosis.
384. Koproski J, Pretto Z, Poretsky L. Effects
of an intervention by a diabetes team in
hospitalized patients with diabetes. Dia-
betes Care 1997;20:15531555
385. Furnary AP, Braithwaite SS. Effects of
outcome on in-hospital transition from
intravenous insulin infusion to subcuta-
neous therapy. Am J Cardiol 2006;98:
557564
386. American Diabetes Association: Diabe-
tes nutrition recommendations for
health care institutions (Position State-
1):S55S57
387. Boucher JL, Swift CS, Franz MJ,
Kulkarni K, Schafer RG, Pritchett E,
Clark NG. Inpatient management of di-
abetes and hyperglycemia: implications
for nutrition practice and the food and
nutrition professional. J Am Diet Assoc
2007;107:105111
388. Scott MG, Bruns DE, Boyd JC, Sacks DB.
Tight glucose control in the intensive
care unit: are glucose meters up to the
task? Clin Chem 2009;55:1820
389. DOrazio P, Burnett RW, Fogh-
Andersen N, Jacobs E, Kuwa K, Ku lp-
mann WR, Larsson L, Lewenstam A,
Maas AH, Mager G, Naskalski JW,
Okorodudu AO, International Federa-
tion of Clinical Chemistry Scientic Di-
vision Working Group on Selective
Electrodes and Point of Care Testing.
Approved IFCC recommendation on re-
porting results for blood glucose (abbre-
viated). Clin Chem2005;51:15731576
390. Dungan K, Chapman J, Braithwaite SS,
Buse J. Glucose measurement: con-
founding issues in setting targets for in-
patient management. Diabetes Care
2007;30:403409
391. Boyd JC, Bruns DE. Quality specica-
tions for glucose meters: assessment by
simulation modeling of errors in insulin
dose. Clin Chem 2001;47:209214
392. Goldberg PA, Siegel MD, Russell RR, Sh-
erwin RS, Halickman JI, Cooper DA,
Dziura JD, Inzucchi SE. Experience with
the continuous glucose monitoring sys-
tem in a medical intensive care unit. Di-
abetes Technol Ther 2004;6:339347
393. Cheung BM, Ong KL, Cherny SS, Sham
PC, Tso AW, Lam KS. Diabetes preva-
lence and therapeutic target achieve-
ment in the United States, 1999 to 2006.
Am J Med 2009;122:443453
394. Coleman K, Austin BT, Brach C, Wagner
EH. Evidence on the Chronic Care
Model in the new millennium. Health
Aff (Millwood) 2009;28:7585
395. Clark CM, Jr, Snyder JW, Meek RL, Stutz
LM, Parkin CG. A systematic approach
to risk stratication and intervention
within a managed care environment im-
proves diabetes outcomes and patient
satisfaction. DiabetesCare2001;24:1079
1086
396. Meigs JB, Cagliero E, Dubey A, Murphy-
Sheehy P, Gildesgame C, Chueh H,
Barry MJ, Singer DE, Nathan DM. Acon-
trolled trial of web-based diabetes dis-
ease management: the MGH diabetes
primary care improvement project. Dia-
betes Care 2003;26:750757
397. OConnor PJ, Desai J, Solberg LI, Reger
LA, Crain AL, Asche SE, Pearson TL,
Clark CK, Rush WA, Cherney LM,
Sperl-Hillen JM, Bishop DB. Random-
ized trial of quality improvement inter-
vention to improve diabetes care in
primary care settings. Diabetes Care
2005;28:18901897
398. Sperl-Hillen JM, OConnor PJ. Factors
driving diabetes care improvement in a
large medical group: ten years of
progress. Am J Manag Care 2005;11:
S177S185
399. Siminerio LM. Implementing diabetes
self-management training programs:
breaking through the barriers in pri-
mary care. EndocrPract 2006;12(Suppl.
1):124130
400. Mahoney JJ. Reducing patient drug ac-
quisition costs can lower diabetes health
claims. Am J Manag Care 2005;11:
S170S176
401. Maney M, Tseng CL, Safford MM, Miller
DR, Pogach LM. Impact of self-reported
patient characteristics upon assessment
of glycemic control in the Veterans
Health Administration. Diabetes Care
2007;30:245251
402. Bergenstal RM. Treatment models from
the International Diabetes Center: ad-
vancing from oral agents to insulin ther-
apy in type 2 diabetes. Endocr Pract
2006;12(Suppl. 1):98104
403. Berikai P, Meyer PM, Kazlauskaite R,
Savoy B, Kozik K, Fogelfeld L. Gain in
patients knowledge of diabetes manage-
ment targets is associated with better
glycemic control. Diabetes Care 2007;
30:15871589
404. OConnor PJ. Electronic medical records
and diabetes care improvement: are we
waiting for Godot? Diabetes Care 2003;
26:942943
405. Shojania KG, Ranji SR, McDonald KM,
Grimshaw JM, Sundaram V, Rushakoff
RJ, Owens DK. Effects of quality im-
provement strategies for type 2 diabetes
on glycemic control: a meta-regression
analysis. JAMA 2006;296:427440
406. Davidson MB. How our current medical
care system fails people with diabetes:
lack of timely, appropriate clinical deci-
sions. Diabetes Care 2009;32:370372
407. McLean DL, McAlister FA, Johnson JA,
King KM, Makowsky MJ, Jones CA,
Tsuyuki RT, SCRIP-HTN Investigators. A
randomized trial of the effect of commu-
nity pharmacist andnurse care onimprov-
ing blood pressure management in
patients with diabetes mellitus: study of
cardiovascular risk intervention by phar-
macists-hypertension(SCRIP-HTN). Arch
Intern Med 2008;168:23552361
408. Parchman ML, Zeber JE, Romero RR,
Pugh JA. Risk of coronary artery disease
in type 2 diabetes and the delivery of
care consistent with the chronic care
model in primary care settings: a STAR-
Net study. Med Care 2007;45:1129
1134
409. Feifer C, Nemeth L, Nietert PJ, Wessell
AM, Jenkins RG, Roylance L, Ornstein
SM. Different paths to high-quality care:
three archetypes of top-performing
practice sites. Ann Fam Med 2007;5:
233241
410. Ornstein S, Nietert PJ, Jenkins RG, Wes-
sell AM, Nemeth LS, Feifer C, Corley
ST. Improving diabetes care through a
multicomponent quality improvement
model in a practice-based research net-
work. Am J Med Qual 2007;22:3441
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Standards of Medical Care in Diabetes2010

AMERICAN DIABETES ASSOCIATION

type 1 diabetes (results from -cell de-

type 2 diabetes (results from a progres-

other specic types of diabetes due to

gestational diabetes mellitus (GDM)

Testing to detect type 2 diabetes and

If tests are normal, repeat testing should

To test for diabetes or to assess risk of

In those identied with increased risk

Screen for GDM using risk factor anal-

Women with GDM should be screened

Patients with IGT (A), IFG (E), or an

Follow-up counseling appears to be im-

Based on potential cost savings of dia-

In addition to lifestyle counseling, met-

Monitoring for the development of di-

SMBG should be carried out three or

For patients using less frequent insulin

To achieve postprandial glucose tar-

When prescribing SMBG, ensure that

Continuous glucose monitoring (CGM)

Although the evidence for A1C lower-

CGM may be a supplemental tool to

Perform the A1C test at least two times

Perform the A1C test quarterly in pa-

Use of point-of-care testing for A1C al-

Lowering A1C to below or around 7%

In type 1 and type 2 diabetes, random-

Subgroup analyses of clinical trials such

Conversely, less-stringent A1C goals

Preprandial 95 mg/dl (5.3 mmol/l)

1-h postmeal 140 mg/dl (7.8

2-h postmeal 120 mg/dl (6.7

premeal, bedtime, and overnight glu-

peak postprandial glucose 100129

Individuals who have pre-diabetes or

Because it can result in cost savings and

In overweight and obese insulin-

For weight loss, either low-carbohy-

For patients on low-carbohydrate diets,

Physical activity and behavior modi-

Among individuals at high risk for de-

Individuals at high risk for type 2 dia-

Saturated fat intake should be 7% of

Reducing intake of trans fat lowers LDL

Monitoring carbohydrate intake,

For individuals with diabetes, use of the

Sugar alcohols and nonnutritive sweet-

If adults with diabetes choose to use

Routine supplementation with antioxi-

Benet from chromium supplementa-

Individualized meal planning should

Bariatric surgery should be considered

Patients with type 2 diabetes who have

Although small trials have shown glyce-

The long-term benets, cost-effectiveness,

People with diabetes should receive

Effective self-management and quality

DSME should address psychosocial is-