Untitled

Download as pdf or txt
Download as pdf or txt
You are on page 1of 7

Korean Journal of Clinical Oncology 2019;15:79-85

https://doi.org/10.14216/kjco.19015
Original
pISSN 1738-8082 ∙ eISSN 2288-4084 Article

Patterns of antibiotics and pathogens for


anastomotic leakage after colorectal cancer surgery
Geunhyeok Yang, Chang Woo Kim, Suk-Hwan Lee
Department of Surgery, Kyung Hee University Hospital at Gangdong, Kyung Hee University School of Medicine, Seoul, Korea

Purpose: Anastomotic leakage (AL) is a type of intra-abdominal infection (IAI) which requires appropriate antibiotics with proper interven-
tion. This study aimed to improve the appropriateness of antibiotic treatment by assessing the patterns of antibiotic treatment and resistance
of pathogen profiles in patients who had AL after colorectal cancer surgery.
Methods: From June 2006 through December 2017, the medical records of the patients who had AL after elective abdominal surgery for col-
orectal cancer in Kyung Hee University Hospital at Gangdong, Seoul, Korea were reviewed retrospectively. Baseline characteristics and consis-
tence of antibiotics with culture study results were analyzed to evaluate the appropriateness of treatment.
Results: Among 982 patients who underwent primary surgery for colorectal cancer, 41 (4.2%) had AL. Mean time of diagnosis of AL from
surgery was 6.3 days. The most commonly used prophylactic antibiotics for the primary surgery was 2nd generation cephalosporin (66.6%).
Mean duration of prophylactic antibiotics usage was 2.8 days. The most commonly used empirical antibiotics after AL occurred was pipera-
cillin and tazobactam (32.6%). Mean duration of empirical antibiotics usage was 8.2 days. The most commonly identified pathogens were
Escherichia coli and Enterococci spp. (26.8% each), and 12.2% of the “ESKAPE” pathogens were identified. Resistance to empirical antibiotics
was 45.5% (10/22).
Conclusion: Penetration of culture study for AL after colorectal cancer surgery appeared relatively low, although the profile of pathogens iso-
lated from the AL patients can give important clues and evidence for appropriate antibiotics use. Surgeons should pay attention in perform-
ing culture studies for IAI including AL for proper patient treatment.

Keywords: Intraabdominal infection, Antibiotics, Resistance, Colonic neoplasms, Anastomotic leakage

INTRODUCTION logical conditions that can involve lesions of all the intra-abdomi-
nal organs. It should be treated with appropriate antibiotic therapy
Intra-abdominal infection (IAI) represents a wide variety of patho- with proper interventions for source control. Choice of appropri-
ate antibiotic must be based on the results of the culture study; the
Received: Oct 18, 2019  Revised: Nov 15, 2019  Accepted: Nov 19, 2019
strain that caused the infection, profile of bacteria, and resistance
Correspondence to: Suk-Hwan Lee to antibiotics. However, because the results usually require a few
Department of Surgery, Kyung Hee University Hospital at Gangdong, days, empirical antibiotics should be administered first, and then,
Kyung Hee University School of Medicine, 892 Dongnam-ro, Gangdong-
the extension of the administration or the replacement of antibiot-
gu, Seoul 05278, Korea
Tel: +82-2-440-6134, Fax: +82-2-440-6073 ics can be considered depending on the results of the test [1].
E-mail: [email protected] Antibiotic resistance disables several mechanisms of antibiotics
ORCID: Geunhyeok Yang (https://orcid.org/0000-0002-8260-1525), Chang Woo against bacteria, subsequently increases medical expense, as well as
Kim (https://orcid.org/0000-0002-6317-8354), Suk-Hwan Lee (https://orcid. affects effectiveness of antibiotics against infection [2-4]. The Cen-
org/0000-0001-6470-8620)
ters for Disease Control and Prevention has reported that the esti-
*This work was presented as an oral presentation at the 51st Annual mated minimum number of illnesses and deaths caused by antibi-
meeting of the Korean Society of Coloproctology, on March 30 to April 1, otics resistance were at least 2 million illness and 23,000 deaths
2018, in Gwangju, Korea.
each year in the United States [5]. In addition, guidelines already
Copyright © 2019 Korean Society of Surgical Oncology
This is an Open Access article distributed under the terms of the Creative Commons Attri-
recommend appropriate antimicrobial agents on the basis of
bution Non-Commercial License (http://creativecommons.org/licenses/by-nc/4.0) which high-quality evidence and advise understanding of the microbio-
permits unrestricted non-commercial use, distribution, and reproduction in any medium,
provided the original work is properly cited. logical profiles and resistance of the key pathogens causing IAI in

www.kjco.org   79
each local region [6-9]. Even some authors made the acronym To evaluate the appropriateness of treatment, consistence of an-
“ESKAPE” pathogens to emphasize the importance of appropri- tibiotics with culture study results and recurrent infection includ-
ate antimicrobial therapy despite increasing antibiotic resistance ing surgical site infection (SSI) occurring within 30 days after in-
[10]. tervention were analyzed.
Anastomotic leakage (AL) after colorectal cancer surgery re-
mains the most feared and disastrous complication for both sur- RESULTS
geon and patient, affecting long-term oncologic outcomes as well
as frequent need for redo interventions, longer hospitalization, and During the study period, a total of 982 patients underwent elective
high mortality rates [11]. AL is also a type of IAI in which the in- surgery for the treatment of primary colorectal cancer. Among
fection source leaks through the intestinal anastomosis for which them, 41 patients (4.2%) experienced AL (Table 1), and culture
proper antibiotics is mandatory with proper intervention. In most studies for intra-abdominal fluid or abscess from AL were per-
case of suspected AL, empirical antibiotics are administered target- formed in 22 patients (53.7%). The most frequent diagnosed site of
ing the gut flora. However, only a few studies assessed the relevance AL was rectum (n = 29, 70.7%), and 39 of 41 patients underwent
of antibiotics for AL. This study aimed to improve the appropriate- intervention for source control whereas two patients were treated
ness of antibiotic treatment by assessing the patterns of antibiotic with only antibiotics. Source control interventions were performed
treatment and resistance of pathogen profiles in patients who had within 1 day from AL in 19 patients (46.3%).
AL after colorectal cancer surgery. Surgical drainage and proximal diversion was performed most
for source control of AL (n = 23, 56.1%), followed by simple closure
METHODS (n = 4), resection and proximal diversion (n = 4), percutaneous
drainage (n = 3), surgical drainage (n = 3), and resection and
From June 2006 through December 2017, consecutive patients re-anastomosis (n = 2).
who underwent elective abdominal surgery for colorectal cancer
in our hospital were screened. The medical records of the patients Table 1. Patients characteristics
were reviewed retrospectively after approval by the Institutional Variable Value (n= 41)
Review Board (IRB) of Kyung Hee University Hospital at Gang- Age (yr) 62.2 ± 11.3
dong (IRB No. KHNMC 2018-08-017). Among the all screened Male sex 31 (75.6)
patients, cases of surgery for recurrence or reoperation were ex- Location of tumor  
cluded. Data of the patients who had AL after primary surgery Right colon 4 (9.8)
were reviewed retrospectively. Left colon 8 (19.5)
Rectum 29 (70.7)
Eligible patients’ sex, age, height, weight, location of tumor, type
Duration between surgery and AL (day) 6.3 (0–27)
of surgery, type and duration of prophylactic antibiotics before
Characteristics of index infection (AL)  
surgery, date of AL diagnosed from the day of surgery, white blood WBC at diagnosis (/mm3) 9,737 ± 4,078
cell count (WBC), C-reactive protein (CRP), type of procedure or CRP at diagnosis (mg/dL) 16.6 ± 10.2
operation for AL, and time from AL to procedure or surgery were Culture study performed 22 (53.7)
recorded. In addition, results of culture study from the abdominal Source control intervention  39 (95.1)
fluid or abscess after AL was diagnosed, antibiotic resistance, the Duration between AL and intervention  
≤ 1 day 19 (48.7)
type and duration of empirical or therapeutic antibiotics adminis-
> 1 day 20 (51.3) 
tered for the purpose of treatment for AL, hospital stay, and mor-
Intervention type  
tality were analyzed. Percutaneous drainage 3 (7.3)
Location of tumor varied as right colon, left colon, and rectum, Surgical drainage 3 (7.3)
and transverse colon cancer was regarded as right side near the Simple closure 4 (9.8)
proximal part or left side near the distal part. As for data on WBC Surgical drainage and proximal diversion 23 (56.1)
Resection and proximal diversion 4 (9.8)
and CRP, the most recent data from the diagnosis of AL were re-
Resection and re-anastomosis 2 (4.9)
corded. Types of source control procedure were classified as fol- Conservative management  2 (4.9)
lows; percutaneous drainage, surgical drainage, simple closure,
Values are presented as mean ± standard deviation, number (%), or median
surgical drainage and proximal diversion, resection and proximal (range). 
diversion, resection, and re-anastomosis. AL, anastomotic leakage; WBC, white blood cell; CRP, C-reactive protein.

80  
Korean Journal of Clinical Oncology
Geunhyeok Yang et al. • Antibiotics and pathogens for anastomotic leak

Table 2. Culture result and antibiotics resistance


Primary Prophylactic Empiric
Patient Pathogens 1 Pathogens 2 Pathogens 3 Sensitivity ESKAPE
surgery antibiotics antibiotics
1 uLAR Ceftriaxone, Ceftezole, Escherichia coli Streptococcus viridans Sensitive
metronidazole metronidazole   group
2 AR Ceftizoxime, Ceftizoxime, Enterococcus faecium Staphylococcus aureus Resistant MRSA
metronidazole metronidazole
3 LAR Cefotetan, Meropenem, Staphylococcus aureus Enterococcus faecalis Resistant MRSA
metronidazole metronidazole
4 LAR Cefminox, Ceftriaxone, Enterococcus faecium Acinetobacter baumannii Resistant IRAB
metronidazole metronidazole
5 LAR Cefminox, Cefminox, Enterococcus faecalis Pseudomonas aeruginosa Resistant
metronidazole metronidazole
6 LAR Cefminox, Cefminox, Escherichia coli Morganella morganii ssp. Sensitive
metronidazole metronidazole
7 LAR Cefotetan Meropenem Morganella morganii ssp. Sensitive
8 LAR Cefotetan Ceftriaxone, Klebsiella pneumoniae ssp. Escherichia coli Enterococcus Resistant
metronidazole  faecium
9 LAR Cefotetan Piperacillin/ Pseudomonas aeruginosa Enterococcus faecium Enterococcus Sensitive
tazobactam,  faecalis
levofloxacin
10 RHC Cefotetan Piperacillin/ Pseudomonas aeruginosa Klebsiella pneumoniae Sensitive
tazobactam
11 LAR Cefotetan Piperacillin/ No growth unknown
tazobactam,
metronidazole
12 LAR Cefotetan Cefotetan Pseudomonas aeruginosa Enterococcus avium Resistant
13 uLAR Cefotetan Cefotetan, Escherichia coli Streptococcus viridans Sensitive
metronidazole
14 RHC Cefotetan Cefotetan Escherichia coli Klebsiella oxytoca β-Hemolytic Sensitive
  streptococcus ,
  group G
15 LAR Cefotetan Cefminox, Enterococcus faecalis Pseudomonas aeruginosa Resistant
metronidazole
16 LAR Cefotetan Piperacillin/ Staphylococcus aureus Stenotrophomonas Resistant MRSA
tazobactam  maltophilia
17 LAR No No Escherichia coli Unknown ESBL+
Escherichia
coli
18 LAR Cefotetan Moxifloxacin Escherichia coli Sensitive
19 TC Cefotetan Piperacillin/ Escherichia coli Sensitive
tazobactam
20 uLAR Cefotetan Piperacillin/ Escherichia coli Enterococcus faecalis Sensitive
tazobactam
21 LAR Cefotetan Piperacillin/ Klebsiella pneumoniae Escherichia coli Sensitive
tazobactam
22 ERHC Cefotetan Piperacillin/ Enterococcus faecium Escherichia coli Resistant
tazobactam,
levofloxacin
LAR, low anterior resection; uLAR, ultra-low anterior resection; AR, anterior resection; RHC, right hemicolectomy; TC, total colectomy; ERHC, extended right
hemicolectomy; MRSA, methicillin-resistant S. aureus ; IRAB, imipenem-resistant A. baumannii ; ESBL+, extended-spectrum beta-lactamase positive.

www.kjco.org   81
Table 3. Pathogens identified from intra-abdominal samples
Pathogens No. (%)  Resistance (%)a)
Gram (+) Aerobic Staphylococcus aureus MSSA NA
MRSA 3 (7.3) 100
Streptococcus spp. 3 (7.3)
Enterococcus faecalis 5 (12.2)
Enterococcus avium 1 (2.4)
Enterococcus faecium 5 (12.2)
Anaerobic  NA
Gram (–) Aerobic Escherichia coli ESBL (–) 10 (24.4)
ESBL (+) 1 (2.4) 9.10
Klebsiella spp. ESBL (–) 4 (9.8)
ESBL (+) NA
Enterobacter aerogenes NA
Pseudomonas aeruginosa ISPA 5 (12.2)
IRPA NA
Acinetobacter baumannii ISAB NA
IRAB 1 (2.4) 100
Proteus mirabilis NA
Stenotrophomonas maltophilia 1 (2.4)
Morganella morganii 2 (4.9)
Anaerobic Bacteroides NA
MSSA, methicillin-sensitive S. aureus ; MRSA, methicillin-resistant S. aureus ; ESBL, extended-spectrum beta-lactamase; ISPA, imipenem-sensitive P. aeruginosa ;
IRPA, imipenem-resistant P. aeruginosa ; ISAB, imipenem-sensitive A. baumannii ; IRAB, imipenem-resistant A. baumannii; NA, not available.
a)
Resistance for each ESKAPE pathogen.

Table 4. Prophylactic antibiotics for colorectal cancer surgery Table 5. Empiric therapeutic antibiotics
Antibiotics agent No. (%)  Antibiotics agent No. (%) 
Cephalosporin 1st G Cephalosporin+MTD 1 (2.4) Penicillins/β-lactamase inhibitors Piperacillin/tazobactam 14 (32.6)
2nd G Cephalosporin only 28 (68.3) Carbapenems Meropenem 1 (2.3)
a)
2nd G Cephalosporin+MTD 4 (9.8) Fluoroquinolones Levofloxacin 2 (4.7)
3rd G Cephalosporin+MTD 6 (14.6) Moxifloxacin 3 (7.0)
No antibiotics 2 (4.9) Cephalosporin 1st G Cephalosporin+MTD 1 (2.3)
G, generation; MTD, metronidazole. 2nd G Cephalosporin only 8 (18.6)
2nd G Cephalosporin+MTD 5 (11.6)
3rd G Cephalosporin+MTD 5 (11.6)
Antibiotic use and the results of culture study for pathogens No antibiotics 4 (9.3)
from intra-abdominal samples are listed in Table 2. Except for one G, generation; MTD, metronidazole.
patient in which no bacteria grew, 11 kinds, 41 (duplicate) patho- a)
Levofloxacin used for underlying pneumonia treatment.
gens were identified in 21 patients, and approximately two kinds of
bacteria were found per patient. Escherichia coli and Enterococ- tant rates of MRSA (3/3), IRAB (1/1) were reported as 100%. Re-
cus spp. (26.8% each) were the most frequently identified, followed sistant rates of ESBL-producing E. coli isolates comprised 9.1%
by Pseudomonas aeruginosa (12.2%). Twelve point one percent of (1/11) of all E. coli isolates.
the “ESKAPE” pathogens were identified including methicillin-re- Prophylactic antibiotics administration was confined to the
sistant Staphylococcus aureus (MRSA) (7.3%), extended-spec- cephalosporins for 39 of 41 patients and combined with metroni-
trum beta-lactamase (ESBL)-producing E. coli (2.4%), imipen- dazole in 11 patients (26.2%) (Table 4). Two patients were not ad-
em-resistant Acinetobacter baumannii (IRAB) (2.4%) [12]. ministered prophylactic antibiotics because they were already be-
Pathogens identified were described in Table 3. Resistant rates of ing treated with therapeutic antibiotics that focused on underlying
each pathogen show a wide spectrum from 9.1% to 100%. Resis- infectious disease. The mean duration of administration was 2.8

82  
Korean Journal of Clinical Oncology
Geunhyeok Yang et al. • Antibiotics and pathogens for anastomotic leak

Table 6. Outcome measurement from AL after colorectal cancer surgery and found a relatively low
Variable Value proportion of culture study performance (22/41, 53.7%) and ap-
Primary outcome   propriate antibiotics according to antibiotic resistance (12/22,
Antibiotics use period (day) 8.2 ± 7.9 54.5%).
Mortality 1 (2.4) Although only 4.2% of AL was reported after overall colorectal
Hospital stay (day) 29.4 ± 15.5 cancer surgery, it scarcely occurred in right colon cancer surgery.
Secondary outcome  
When limited to left colon or rectal cancer surgery, 37 of 389 pa-
Recurrent infectiona) 14 (34.1)
tients (9.5%) had AL after primary surgery.
Values are presented as mean ± standard deviation or number (%).
a)
We reviewed empirical antibiotics prescription pattern and in-
Including surgical site infection.
fection severity with these patients. Only 22 patients (53.7%) had
culture study from the intraperitoneal source (abscess or fluid) and
days, but the duration of prophylactic antibiotic treatment for the the pathogens were identified from 21 patients. This low perfor-
last 5 years was 1.1 days. This is in accordance with the trend of re- mance of culture study might be due to lack of interest by surgeons,
cent guideline for prophylactic antibiotic in surgery, which recom- rather than lack of time. Moreover, although most of the pathogens
mended that the postoperative duration of antimicrobial prophy- are expected to be gut flora (possibly one of the reasons culture
laxis can be reduced [13,14]. studies were not performed), the authors found that proper antibi-
The prescribed therapeutic empiric antibiotics patterns are listed otics use rates were only 54.5% considering antibiotic resistance
in Table 5. Of the 43 antibiotics including overlapping, 14 (32.6%) (Table 2).
piperacillin/tazobactam were administered and eight 2nd genera- The pathogen distribution identified in this study was slightly
tion cephalosporin only (18.6%), and five 2nd and 3rd generation different from previous reports. Data from the Study for Monitor-
cephalosporin plus metronidazole, fluoroquinolone (11.6% each) ing Antimicrobial Resistance Trends (SMART) provide the best
were administered. Carbapenem was given only for one patient available evidence for the current status of complicated IAIs in Asia
(2.3%). Glycopeptides (Vancomycin) and Glycyclines (Tigecyclin) [17,18]. Over the course of the SMART, the five most commonly
were never used as empirical antibiotics. On the other hand, no isolated Gram-negative pathogens from IAIs were E. coli (47.8%),
antibiotics were prescribed to four patients (9.3%) because the Klebsiella pneumoniae (14.5%), P. aeruginosa (9.4%), Entero-
symptoms of AL were relatively mild for those patients. bacter cloacae (6.0%), and Proteus mirabilis (3.6%) [19]. The CI-
Mean duration of empirical antibiotics use were 8.2 days (Table AOW (Complicated intra-abdominal infections worldwide obser-
6), which is similar with the recommendations of recent guidelines vational study) collected the data from 1898 patients in 68 medical
[15]. In-hospital mortality rate was 2.4% and cause of death was institutions worldwide [19]. From the study, the top pathogens
sepsis. Mean hospital stay was 29.4 days (range, 10–68 days). Four- from IAIs were E. coli (35.7%), Enterococcus (12.9%), Klebsiella
teen patients (34.1%) had recurrent infection including SSI after (10.5%), P. aeruginosa (5.1%), Enterobacter spp. (4.1%). In our
source control. In 10 of 22 patients (45.5%) who had culture study, study, Gram-positive microbe was 41.5% of all pathogens identi-
identified pathogens were reported to be resistant to the given em- fied. Enterococci was found to be 26.8% the same as E. coli, and S.
pirical antibiotics (Table 2). aureus was as much as 7.3%. Regarding resistance, it is remarkable
that MRSA was identified in 100% of all S. aureus (4/4).
DISCUSSION Rice [10], in 2008, coined the acronym of “ESKAPE” pathogens
including Enterococcus faecium, S. aureus, K. pneumoniae, A.
Secondary peritonitis is a consequence of a mechanical breach of baumannii, P. aeruginosa, and Enterobacter species to empha-
the gastrointestinal tract. The microbial species isolated reflect the size that these bacteria currently cause the majority of hospital in-
patterns of colonization of the involved level of the gastrointestinal fections and effectively “escape” the effects of antibacterial drugs
tract: perforation of the stomach or duodenum results in an in- [20]. Published surveillance studies have consistently reported that
flammatory process that is primarily chemical, whereas perfora- Gram-negative bacilli, including ESKAPE pathogens, isolated
tions of the colon create polymicrobial infections including AL af- from patients in several countries within the Asia-Pacific region,
ter colorectal cancer surgery [16]. It explains the importance of generally demonstrate higher rates of antimicrobial resistance than
knowledge on organ origin of infection because it helps clinicians observed in North American and European studies, and that the
choose the appropriate treatment, including selection of antibiotics. majority of pathogens isolated from intensive care units in a num-
The authors assessed the pathogens from the infected source ber of Asia-Pacific countries are members of the ESKAPE group

www.kjco.org   83
[21,22]. 2. Ventola CL. The antibiotic resistance crisis: part 1: causes and
AL belongs to the category of hospital acquired (HA)-IAI and threats. P T 2015;40:277-83.
the pathogen spectrum is different from those of community ac- 3. Ventola CL. The antibiotic resistance crisis: part 2: management
quired-IAI. For this reason, treatment of AL patients should be ad- strategies and new agents. P T 2015;40:344-52.
ministration of broad antibiotics, as in the treatment of HA-IAI 4. Sturkenboom MC, Goettsch WG, Picelli G, in’t Veld B, Yin DD, de
patients, with an understanding of pathogen patterns in the region, Jong RB, et al. Inappropriate initial treatment of secondary in-
and the selection of antibiotics to cover the resistant strains accord- tra-abdominal infections leads to increased risk of clinical failure
ingly. Especially, it is recommended to consider prescribing agents and costs. Br J Clin Pharmacol 2005;60:438-43.
covering MRSA when clinicians treat the secondary peritonitis 5. Solomon SL, Oliver KB. Antibiotic resistance threats in the United
caused by colon and rectum in this region due to higher rates of States: stepping back from the brink. Am Fam Physician 2014;89:
MRSA identification than other guidelines. 938-41.
Regarding behavior of antibiotics prescription in accordance 6. Mazuski JE, Tessier JM, May AK, Sawyer RG, Nadler EP, Rosengart
with published guidelines, it could be considered that 54.5% of 41 MR, et al. The surgical infection society revised guidelines on the
patients were prescribed appropriately with narrow-spectrum an- management of intra-abdominal infection. Surg Infect (Larchmt)
tibiotics. Broad-spectrum antibiotics such as piperacillin/tazobact- 2017;18:1-76.
am or carbapenem should have been prescribed for HA-IAI such 7. Sartelli M, Weber DG, Ruppe E, Bassetti M, Wright BJ, Ansaloni L,
as AL patients, and narrow-spectrum antibiotics, which can resist et al. Antimicrobials: a global alliance for optimizing their rational
ESKAPE strains, should have been avoided [6,8,9]. use in intra-abdominal infections (AGORA). World J Emerg Surg
There are several limitations in this study. Selection bias from 2016;11:33.
the retrospective nature is inevitable. Moreover, culture study of 8. Sartelli M, Viale P, Catena F, Ansaloni L, Moore E, Malangoni M, et
pathogens, which is the most important procedure in this study, al. 2013 WSES guidelines for management of intra-abdominal in-
was performed only in about half of the patients with AL. Lastly, fections. World J Emerg Surg 2013;8:3.
consistency of prophylactic and empirical antibiotic use lack re- 9. Solomkin JS, Mazuski JE, Bradley JS, Rodvold KA, Goldstein EJ,
garding both kind and duration of antibiotics. Baron EJ, et al. Diagnosis and management of complicated in-
In conclusion, penetration of culture study for AL after colorec- tra-abdominal infection in adults and children: guidelines by the
tal cancer surgery appears relatively low, although the profile of Surgical Infection Society and the Infectious Diseases Society of
pathogens isolated from AL patients can give important clues and America. Clin Infect Dis 2010;50:133-64.
evidence for appropriate antibiotics use. Surgeons should pay at- 10. Rice LB. Federal funding for the study of antimicrobial resistance in
tention in performing culture studies for IAI including AL to treat nosocomial pathogens: no ESKAPE. J Infect Dis 2008;197:1079-
patients with the proper method without wasting time and cost. 81.
Further studies are required to update the current status and prob- 11. Hammond J, Lim S, Wan Y, Gao X, Patkar A. The burden of gastro-
lems of antibiotics use. intestinal anastomotic leaks: an evaluation of clinical and economic
outcomes. J Gastrointest Surg 2014;18:1176-85.
CONFLICT OF INTEREST 12. Sartelli M, Catena F, Ansaloni L, Coccolini F, Corbella D, Moore
EE, et al. Complicated intra-abdominal infections worldwide: the
No potential conflict of interest relevant to this article was reported. definitive data of the CIAOW Study. World J Emerg Surg 2014;9:
37.
ACKNOWLEDGMENTS 13. Bratzler DW, Dellinger EP, Olsen KM, Perl TM, Auwaerter PG, Bo-
lon MK, et al. Clinical practice guidelines for antimicrobial pro-
This work was supported by a National Research Foundation of phylaxis in surgery. Surg Infect (Larchmt) 2013;14:73-156.
Korea (NRF) grant funded by the Korean Government Ministry 14. Park YY, Kim CW, Park SJ, Lee KY, Lee JJ, Lee HO, et al. Influence of
of Education (No. 017R1D1A1B03030948). shorter duration of prophylactic antibiotic use on the incidence of
surgical site infection following colorectal cancer surgery. Ann
REFERENCES Coloproctol 2015;31:235-42.
15. Sawyer RG, Claridge JA, Nathens AB, Rotstein OD, Duane TM,
1. Menichetti F, Sganga G. Definition and classification of intra-ab- Evans HL, et al. Trial of short-course antimicrobial therapy for in-
dominal infections. J Chemother 2009;21 Suppl 1:3-4. traabdominal infection. N Engl J Med 2015;372:1996-2005.

84  
Korean Journal of Clinical Oncology
Geunhyeok Yang et al. • Antibiotics and pathogens for anastomotic leak

16. Marshall JC. Intra-abdominal infections. Microbes Infect 20. Boucher HW, Talbot GH, Bradley JS, Edwards JE, Gilbert D, Rice
2004;6:1015-25. LB, et al. Bad bugs, no drugs: no ESKAPE! An update from the In-
17. Hsueh PR. Study for monitoring antimicrobial resistance trends fectious Diseases Society of America. Clin Infect Dis 2009;48:1-12.
(SMART) in the Asia-Pacific region, 2002-2010. Int J Antimicrob 21. Paterson DL, Rossi F, Baquero F, Hsueh PR, Woods GL, Satishchan-
Agents 2012;40 Suppl:S1-3. dran V, et al. In vitro susceptibilities of aerobic and facultative
18. Chow JW, Satishchandran V, Snyder TA, Harvey CM, Friedland IR, Gram-negative bacilli isolated from patients with intra-abdominal
Dinubile MJ. In vitro susceptibilities of aerobic and facultative infections worldwide: the 2003 Study for Monitoring Antimicrobi-
gram-negative bacilli isolated from patients with intra-abdominal al Resistance Trends (SMART). J Antimicrob Chemother
infections worldwide: the 2002 Study for Monitoring Antimicrobi- 2005;55:965-73.
al Resistance Trends (SMART). Surg Infect (Larchmt) 2005;6:439- 22. Lu PL, Liu YC, Toh HS, Lee YL, Liu YM, Ho CM, et al. Epidemiolo-
48. gy and antimicrobial susceptibility profiles of Gram-negative bac-
19. Morrissey I, Hackel M, Badal R, Bouchillon S, Hawser S, Bieden- teria causing urinary tract infections in the Asia-Pacific region:
bach D. A review of ten years of the study for monitoring antimi- 2009-2010 results from the study for monitoring antimicrobial re-
crobial resistance trends (SMART) from 2002 to 2011. Pharma- sistance trends (SMART). Int J Antimicrob Agents 2012;40 Sup-
ceuticals (Basel) 2013;6:1335-46. pl:S37-43.

www.kjco.org   85

You might also like