Tamiflu PDF
Tamiflu PDF
Tamiflu PDF
Consider available information on influenza drug susceptibility patterns Prophylaxis studies – Nausea, vomiting, diarrhea, abdominal pain (6.1)
Pediatric patients 2 weeks to less than 1 year of age: 3mg/kg twice daily Do not administer TAMIFLU until 2 weeks following administration of
for 5 days. the live attenuated influenza vaccine, unless medically indicated.
Renally impaired adult patients (creatinine clearance 10-30 mL/min):
Reduce to 75 mg once daily for 5 days (2.4) ----------------------- USE IN SPECIFIC POPULATIONS -----------------------
Prophylaxis of influenza (2.3) Pregnancy: No data in pregnant women. Use only if clearly needed. (8.1)
Adults and adolescents (13 years and older): 75 mg once daily for at least Nursing mothers: Caution should be exercised when administered to a
10 days
nursing woman. (8.3).
- Community outbreak: 75 mg once daily for up to 6 weeks
Pediatric patients 1 to 12 years of age: Based on weight once daily for See 17 for PATIENT COUNSELING INFORMATION and FDA-
10 days approved patient labeling
- Community outbreak: Based on weight once daily for up to 6 weeks Revised: 12/2012
Table 1 Treatment (twice daily dosing for 5 days) and Prophylaxis (once daily dosing for
10 days) Dosing of Oral TAMIFLU for Influenza in Pediatric Patients
Weight Treatment Dosing Prophylaxis Dosing Volume of Number of Bottles Number of
(kg) for 5 days for 10 days Oral Suspension of Oral Capsules and
(6 mg/mL) for each Suspension to Strength to
Dose** Dispense Dispense§
Any weight 3 mg/kg twice daily Not applicable* 0.5 mL/kg† 1 bottle Not applicable
40.1 kg or more 75 mg twice daily 75 mg once daily 12.5 mL‡‡ 3 bottles 10 Capsules
75 mg
*TAMIFLU is not approved for prophylaxis of patients less than 1 year of age
**A 10 mL oral dosing dispenser is provided with the oral suspension. In the event that the dispenser provided is lost or damaged,
†For patients less than 1 year of age, remove the provided 10 mL oral dosing dispenser from the packaging, and provide an
appropriate dosing device that can accurately measure and administer small volumes.
‡‡Delivery of this TAMIFLU for Oral Suspension dose requires administering 10 mL followed by another 2.5 mL.
§Oral Suspension is the preferred formulation for patients who cannot swallow capsules.
30 mg 75 mL
45 mg 100 mL
60 mg 125 mL
75 mg 150 mL
* If the TAMIFLU dose is between the doses listed, the total volume of oral suspension to compound should default to the next greater
dose listed.
Second, determine the number of capsules and the amount of water and vehicle (Cherry Syrup, Ora-Sweet SF,
or simple syrup) that are needed to prepare the total volume (determined from Table 2: 37.5 mL, 75 mL,
100 mL, 125 mL, or 150 mL) of compounded oral suspension (6 mg/mL) (see Table 3).
Table 3 Number of TAMIFLU 75 mg Capsules and Amount of Vehicle (Cherry Syrup,
Ora-Sweet SF, or Simple Syrup) Needed to Prepare the Total Volume of a
Compounded Oral Suspension (6 mg/mL)
Total Volume of Compounded
Oral Suspension to be Prepared 37.5 mL 75 mL 100 mL 125 mL 150 mL
3 capsules 6 capsules 8 capsules 10 capsules 12 capsules
Number of TAMIFLU 75 mg
(225mg (450 mg (600 mg (750 mg (900 mg
Capsules*
oseltamivir) oseltamivir) oseltamivir) oseltamivir) oseltamivir)
Amount of Water 2.5 mL 5 mL 7 mL 8 mL 10 mL
Volume of Vehicle
Cherry Syrup (Humco) OR
34.5 mL 69 mL 91 mL 115 mL 137 mL
Ora-Sweet SF (Paddock
Laboratories) OR simple syrup
*Includes overage to ensure all doses can be delivered
Refrigeration: Stable for 5 weeks (35 days) when stored in a refrigerator at 2 to 8C (36° to 46°F).
Room Temperature: Stable for five days (5 days) when stored at room temperature, 25C (77°F).
Note: The storage conditions are based on stability studies of compounded oral suspensions, using the above
mentioned vehicles, which were placed in glass and polyethyleneterephthalate (PET) bottles. Stability studies
Place a pharmacy label on the bottle that includes the patient’s name, dosing instructions, and drug name and
any other required information to be in compliance with all State and Federal Pharmacy Regulations.
Refer to Dosage and Administration sections 2.2, 2.3, 2.4 and Table 1 for the proper dosing instructions for the
pharmacy label.
Serious skin and hypersensitivity reactions [see Warnings and Precautions (5.1)]
group.
b
The majority of subjects received placebo; 254 subjects from a randomized, open-label postexposure prophylaxis study in
b
Pooled data from trials of TAMIFLU treatment of naturally acquired influenza.
O COOC2H5
3
4
5
HN
NH2 . H3PO4
O
Plasma concentrations of oseltamivir carboxylate are proportional to doses up to 500 mg given twice daily.
Coadministration with food has no significant effect on the peak plasma concentration (551 ng/mL under fasted
conditions and 441 ng/mL under fed conditions) and the area under the plasma concentration time curve
(6218 ng·h/mL under fasted conditions and 6069 ng·h/mL under fed conditions) of oseltamivir carboxylate.
Distribution
The volume of distribution (Vss) of oseltamivir carboxylate, following intravenous administration in 24 subjects,
The binding of oseltamivir carboxylate to human plasma protein is low (3%). The binding of oseltamivir to
human plasma protein is 42%, which is insufficient to cause significant displacement-based drug interactions.
Metabolism
Oseltamivir is extensively converted to oseltamivir carboxylate by esterases located predominantly in the liver.
Neither oseltamivir nor oseltamivir carboxylate is a substrate for, or inhibitor of, cytochrome P450 isoforms.
Elimination
concentrations of oseltamivir declined with a half-life of 1 to 3 hours in most subjects after oral administration.
Oseltamivir carboxylate is not further metabolized and is eliminated in the urine. Plasma concentrations of
oseltamivir carboxylate declined with a half-life of 6 to 10 hours in most subjects after oral administration.
Oseltamivir carboxylate is eliminated entirely (>99%) by renal excretion. Renal clearance (18.8 L/h) exceeds
glomerular filtration rate (7.5 L/h), indicating that tubular secretion occurs in addition to glomerular filtration.
Special Populations
Renal Impairment
Administration of 100 mg of oseltamivir phosphate twice daily for 5 days to subjects with various degrees of
renal impairment showed that exposure to oseltamivir carboxylate is inversely proportional to declining renal
function. Oseltamivir carboxylate exposures in subjects with normal and impaired renal function administered
various dose regimens of oseltamivir are described in Table 7.
Reference ID: 3235738 14
Table 7 Oseltamivir Carboxylate Exposures in Subjects With Normal and
Reduced Serum Creatinine Clearance
Parameter Normal Renal Function Impaired Renal Function
75 mg 75 mg 150 mg
Creatinine Clearance Creatinine Clearance
once twice twice
<10 mL/min >10 and <30 mL/min
daily daily daily
CAPD Hemodialysis 75 mg
30 mg 30 mg alternate 75 mg alternate 30 mg
weekly HD cycle daily days daily
Cmax 259* 348* 705* 766 850 1638 1175 655
Cmin 39* 138* 288* 62 48 864 209 346
AUC48† 7476* 10876* 21864* 17381 12429 62636 21999 25054
*Observed values. All other values are predicted.
†AUC normalized to 48 hours.
Hepatic Impairment
In clinical studies oseltamivir carboxylate exposure was not altered in subjects with mild or moderate hepatic
impairment [see Dosage and Administration (2.5) and Use in Specific Populations (8.7)].
Pediatric Subjects (1 to 12 years of age)
The pharmacokinetics of oseltamivir and oseltamivir carboxylate have been evaluated in a single-dose
pharmacokinetic study in pediatric subjects aged 5 to 16 years (n=18) and in a small number of pediatric
subjects aged 3 to 12 years (n=5) enrolled in a clinical trial. Younger pediatric subjects cleared both the prodrug
and the active metabolite faster than adult subjects resulting in a lower exposure for a given mg/kg dose. For
oseltamivir carboxylate, apparent total clearance decreases linearly with increasing age (up to 12 years). The
pharmacokinetics of oseltamivir in pediatric subjects over 12 years of age are similar to those in adult subjects.
Pediatric Subjects (2 weeks to less than 1 year of age)
The pharmacokinetics of oseltamivir and oseltamivir carboxylate have been evaluated in two open-label studies
of pediatric subjects less than one year of age (n=122) infected with influenza. Apparent clearance of the active
metabolite decreases with decreasing age in subjects less than 1 year of age; however the oseltamivir and
oseltamivir carboxylate exposure following a 3 mg/kg dose in subjects under 1 year of age is expected to be
within the observed exposures in adults and adolescents receiving 75 mg twice daily and 150 mg twice daily.
Geriatric Patients
Exposure to oseltamivir carboxylate at steady-state was 25% to 35% higher in geriatric subjects (age range 65
to 78 years) compared to young adults given comparable doses of oseltamivir. Half-lives observed in the
geriatric subjects were similar to those seen in young adults. Based on drug exposure and tolerability, dose
adjustments are not required for geriatric patients for either treatment or prophylaxis [see Dosage and
Administration (2.6)].
12.4 Microbiology
Mechanism of Action
Oseltamivir phosphate is an ethyl ester prodrug requiring ester hydrolysis for conversion to the active form,
Selection of influenza A viruses resistant to oseltamivir can occur at higher frequencies in children. The
incidence of oseltamivir treatment-associated resistance in pediatric treatment studies has been detected at rates
of 27% to 37% and 3% to 18% (3/11 to 7/19 and 1/34 to 9/50 post-treatment isolates, respectively) for influenza
A/H1N1 and influenza A/H3N2, respectively. The frequency of resistance selection to oseltamivir and the
prevalence of such resistant virus vary seasonally and geographically.
Two placebo-controlled double-blind clinical trials were conducted: one in the U.S. and one outside the U.S.
Subjects were eligible for these trials if they had fever >100ºF, accompanied by at least one respiratory
symptom (cough, nasal symptoms, or sore throat) and at least one systemic symptom (myalgia, chills/sweats,
malaise, fatigue, or headache) and influenza virus was known to be circulating in the community. In addition,
all subjects enrolled in the trials were allowed to take fever-reducing medications.
Of 1355 subjects enrolled in these two trials, 849 (63%) subjects were influenza-infected (age range 18 to
65 years; median age 34 years; 52% male; 90% Caucasian; 31% smokers). Of the 849 influenza-infected
subjects, 95% were infected with influenza A, 3% with influenza B, and 2% with influenza of unknown type.
TAMIFLU was started within 40 hours of onset of symptoms. Subjects participating in the trials were required
to self-assess the influenza-associated symptoms as “none,” “mild,” “moderate,” or “severe.” Time to
improvement was calculated from the time of treatment initiation to the time when all symptoms (nasal
congestion, sore throat, cough, aches, fatigue, headaches, and chills/sweats) were assessed as “none” or “mild.”
In both studies, at the recommended dose of TAMIFLU 75 mg twice daily for 5 days, there was a 1.3 day
reduction in the median time to improvement in influenza-infected subjects receiving TAMIFLU compared to
subjects receiving placebo. Subgroup analyses of these studies by gender showed no differences in the treatment
effect of TAMIFLU in men and women.
In the treatment of influenza, no increased efficacy was demonstrated in subjects receiving treatment of 150 mg
TAMIFLU twice daily for 5 days.
Geriatric Subjects
Three double-blind placebo-controlled treatment trials were conducted in subjects 65 years of age in three
consecutive seasons. The enrollment criteria were similar to that of adult trials with the exception of fever being
defined as >97.5F. Of 741 subjects enrolled, 476 (65%) subjects were influenza-infected. Of the 476 influenza-
infected subjects, 95% were infected with influenza type A and 5% with influenza type B.
In the pooled analysis, at the recommended dose of TAMIFLU 75 mg twice daily for 5 days, there was a 1-day
reduction in the median time to improvement in influenza-infected subjects receiving TAMIFLU compared to
those receiving placebo (p=NS). However, the magnitude of treatment effect varied between studies.
Pediatric Subjects (1 to 12 years of age)
One double-blind placebo-controlled treatment trial was conducted in pediatric subjects aged 1 to 12 years
(median age 5 years), who had fever (>100ºF) plus one respiratory symptom (cough or coryza) when influenza
virus was known to be circulating in the community. Of 698 subjects enrolled in this trial, 452 (65%) were
influenza-infected (50% male; 68% Caucasian). Of the 452 influenza-infected subjects, 67% were infected with
influenza A and 33% with influenza B.
The primary endpoint in this study was the time to freedom from illness, a composite endpoint that required 4
individual conditions to be met. These were: alleviation of cough, alleviation of coryza, resolution of fever, and
parental opinion of a return to normal health and activity. TAMIFLU treatment of 2 mg/kg twice daily, started
within 48 hours of onset of symptoms, significantly reduced the total composite time to freedom from illness by
Reference ID: 3235738 18
1.5 days compared to placebo. Subgroup analyses of this study by gender showed no differences in the
treatment effect of TAMIFLU in male and female pediatric subjects.
Pediatric Subjects (2 weeks to less than 1 year of age)
Two open label trials evaluated the safety and pharmacokinetics of oseltamivir and oseltamivir carboxylate in
influenza infected pediatric subjects 2 weeks to less than 1 year of age (including premature infants at least 36
weeks post conceptional age). Subjects received TAMIFLU at doses ranging from 2 to 3.5 mg/kg twice daily
for 5 days depending on subject age. These clinical trials were not designed to evaluate clinical efficacy or
virologic response.
Of the 136 subjects under the age of 1 year enrolled and dosed in the trials, the majority of the subjects were
male (55%), white (79%), non-Hispanic (74%), full term (76%) and infected with influenza A (80%).
Pharmacokinetic data indicated that a dose of 3 mg/kg twice daily in pediatric subjects 2 weeks to less than 1
year of age provided TAMIFLU concentrations similar to or higher than those observed in older pediatric
subjects and adults receiving the approved dose and, by extrapolation, is expected to provide similar efficacy.
The trials provided adequate safety data to support this dose selection [see Adverse Reactions (6.1)].
14.2 Prophylaxis of Influenza
Adult and Adolescent Subjects (13 years of age and older)
The efficacy of TAMIFLU in preventing naturally occurring influenza illness has been demonstrated in three
seasonal prophylaxis studies and a postexposure prophylaxis study in households. The primary efficacy
parameter for all these studies was the incidence of laboratory-confirmed clinical influenza. Laboratory-
confirmed clinical influenza was defined as oral temperature 99.0ºF/37.2ºC plus at least one respiratory
symptom (cough, sore throat, nasal congestion) and at least one constitutional symptom (aches and pain,
fatigue, headache, chills/sweats), all recorded within 24 hours, plus either a positive virus isolation or a four
fold increase in virus antibody titers from baseline.
In a pooled analysis of two seasonal prophylaxis studies in healthy unvaccinated adults (aged 13 to 65 years),
TAMIFLU 75 mg once daily taken for 42 days during a community outbreak reduced the incidence of
laboratory-confirmed clinical influenza from 5% (25/519) for the placebo group to 1% (6/520) for the
TAMIFLU group.
In a seasonal prophylaxis study in elderly residents of skilled nursing homes, TAMIFLU 75 mg once daily
taken for 42 days reduced the incidence of laboratory-confirmed clinical influenza from 4% (12/272) for the
placebo group to <1% (1/276) for the TAMIFLU group. About 80% of this elderly population were vaccinated,
14% of subjects had chronic airway obstructive disorders, and 43% had cardiac disorders.
In a study of postexposure prophylaxis in household contacts (aged 13 years) of an index case, TAMIFLU
75 mg once daily administered within 2 days of onset of symptoms in the index case and continued for 7 days
reduced the incidence of laboratory-confirmed clinical influenza from 12% (24/200) in the placebo group to 1%
(2/205) for the TAMIFLU group. Index cases did not receive TAMIFLU in the study.
Pediatric Subjects (1 to 12 years of age)
The efficacy of TAMIFLU in preventing naturally occurring influenza illness has been demonstrated in a
randomized, open-label, postexposure prophylaxis study in households that included pediatric subjects aged 1 to
12 years, both as index cases and as family contacts. All index cases in this study received treatment. The
primary efficacy parameter for this study was the incidence of laboratory-confirmed clinical influenza in the
household. Laboratory-confirmed clinical influenza was defined as oral temperature 100F/37.8C plus cough
and/or coryza recorded within 48 hours, plus either a positive virus isolation or a four-fold or greater increase in
virus antibody titers from baseline or at illness visits. Among household contacts 1 to 12 years of age not
already shedding virus at baseline, TAMIFLU for oral suspension 30 mg to 60 mg taken once daily for 10 days
30-mg capsules (30 mg free base equivalent of the phosphate salt): light yellow hard gelatin capsules.
“ROCHE” is printed in blue ink on the light yellow body and “30 mg” is printed in blue ink on the light yellow
45-mg capsules (45 mg free base equivalent of the phosphate salt): grey hard gelatin capsules. “ROCHE” is
printed in blue ink on the grey body and “45 mg” is printed in blue ink on the grey cap. Available in blister
packages of 10 (NDC 0004-0801-85).
75-mg capsules (75 mg free base equivalent of the phosphate salt): grey/light yellow hard gelatin capsules.
“ROCHE” is printed in blue ink on the grey body and “75 mg” is printed in blue ink on the light yellow cap.
Available in blister packages of 10 (NDC 0004-0800-85).
Storage
Store the capsules at 25ºC (77ºF); excursions permitted to 15º to 30ºC (59º to 86ºF) [See USP Controlled Room
Temperature].
TAMIFLU for Oral Suspension
Supplied as a white powder blend in a glass bottle. After constitution, the powder blend produces a white tutti
frutti–flavored oral suspension. After constitution with 55 mL of water, each bottle delivers a usable volume of
60 mL of oral suspension equivalent to 360 mg oseltamivir base (6 mg/mL). Each bottle is supplied with a
bottle adapter and a 10 mL oral dispenser (NDC 0004-0820-09).
Storage
Store dry powder at 25ºC (77ºF); excursions permitted to 15º to 30ºC (59º to 86ºF) [See USP Controlled Room
Temperature].
Store constituted suspension under refrigeration for up to 17 days at 2º to 8ºC (36º to 46ºF). Do not freeze.
Alternatively, store constituted suspension for up to 10 days at 25ºC (77ºF); excursions permitted to 15º to 30ºC
(59º to 86ºF) [See USP Controlled Room Temperature].
Tell your healthcare provider about all the medicines you take,
including prescription or over-the-counter medicines, vitamins, and herbal
supplements.
Know the medicines you take. Keep a list of them to show your
healthcare provider and pharmacist when you get a new medicine.
The most common side effects of TAMIFLU when used for treatment of the flu
include nausea and vomiting.
The most common side effect of TAMIFLU when used for prevention of the flu
include nausea, vomiting, diarrhea, and stomach (abdomen) pain.
Tell your healthcare provider if you have any side effect that bothers you or
that does not go away.
These are not all of the possible side effects of TAMIFLU.
Call your doctor for medical advice about side effects. You may report side
effects to FDA at 1-800-FDA-1088.
How should I store TAMIFLU?
Store TAMIFLU capsules at room temperature between 68°F to 77°F
(20°C to 25°C).
Store TAMIFLU for oral suspension in the refrigerator for up to 17 days
between 36ºF to 46ºF (2ºC to 8ºC)
Store TAMIFLU for oral suspension for up to 10 days at room
temperature between 68°F to 77°F (20°C to 25°C).
Safely throw away any unused TAMIFLU that is out of date or no
longer needed.
Keep TAMIFLU and all medicines out of the reach of children.
If you would like more information, talk with your healthcare provider. You
can ask your healthcare provider or pharmacist for information about
TAMIFLU that is written for health professionals.
Step 1. Shake the TAMIFLU for oral suspension bottle well before each use.
Step 2. Open the bottle by pushing downward on the child resistant bottle
cap and twisting it in the direction of the arrow.
Step 3. Fully push down the plunger of the oral dispenser toward the tip
before inserting into the bottle. Insert the tip of the oral dispenser
into the opening of the bottle adapter.
Step 4. Turn the entire unit (bottle and oral dispenser) upside down.
Step 5. Gently pull back on the plunger of the oral dispenser until the
bottom of the plunger is even with the line for the dose prescribed
by your healthcare provider. (See Figure C).
This Patient Information and Instructions for Use have been approved by the
U.S. Food and Drug Administration.
Tamiflu® (oseltamivir phosphate)
Distributed by: Licensor:
Genentech, Inc.
Gilead Sciences, Inc.
A Member of the Roche Group Foster City, California 94404
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