Tamiflu
SIDE EFFECTS
Treatment Studies in Adult Patients
A total of 1171 patients who participated in adult phase III controlled clinical trials for the treatment of influenza were treated with TAMIFLU. The most frequently reported adverse events in these studies were nausea and vomiting. These events were generally of mild to moderate degree and usually occurred on the first 2 days of administration. Less than 1% of subjects discontinued prematurely from clinical trials due to nausea and vomiting.
Adverse events that occurred with an incidence of ≥ 1% in 1440 patients taking placebo or TAMIFLU 75 mg twice daily in adult phase III treatment studies are shown in Table 3. This summary includes 945 healthy young adults and 495 “at risk” patients (elderly patients and patients with chronic cardiac or respiratory disease). Those events reported numerically more frequently in patients taking TAMIFLU compared with placebo were nausea, vomiting, bronchitis, insomnia, and vertigo.
Prophylaxis Studies in Adult Patients
A total of 4187 subjects (adolescents, healthy adults and elderly) participated in phase III prophylaxis studies, of whom 1790 received the recommended dose of 75 mg once daily for up to 6 weeks. Adverse events were qualitatively very similar to those seen in the treatment studies, despite a longer duration of dosing (see Table 3). Events reported more frequently in subjects receiving TAMIFLU compared to subjects receiving placebo in prophylaxis studies, and more commonly than in treatment studies, were aches and pains, rhinorrhea, dyspepsia and upper respiratory tract infections. However, the difference in incidence between TAMIFLU and placebo for these events was less than 1%. There were no clinically relevant differences in the safety profile of the 942 elderly subjects who received TAMIFLU or placebo, compared with the younger population.
Table 3 : Most Frequent Adverse Events in Studies in Naturally
Acquired Influenza in Patients 13 Years of Age and Older
| Treatment Prophylaxis | ||||
| Adverse Event | Placebo N=716 |
Oseltamivir 75 mg bid N=724 |
Placebo/ No Prophylaxisa N=1688 |
Oseltamivir 75 mg qd N=1790 |
| Nausea (without vomiting) | 40 (6%) | 72 (10%) | 56 (3%) | 129 (7%) |
| Vomiting | 21 (3%) | 68 (9%) | 16 (1%) | 39 (2%) |
| Diarrhea | 70 (10%) | 48 (7%) | 40 (2%) | 50 (3%) |
| Bronchitis | 15 (2%) | 17 (2%) | 22 (1%) | 15 (1%) |
| Abdominal pain | 16 (2%) | 16 (2%) | 25 (1%) | 37 (2%) |
| Dizziness | 25 (3%) | 15 (2%) | 21 (1%) | 24 (1%) |
| Headache | 14 (2%) | 13 (2%) | 306 (18%) | 326 (18%) |
| Cough | 12 (2%) | 9 (1%) | 119 (7%) | 94 (5%) |
| Insomnia | 6 (1%) | 8 (1%) | 15 (1%) | 22 (1%) |
| Vertigo | 4 (1%) | 7 (1%) | 4 ( < 1%) | 4 ( < 1%) |
| Fatigue | 7 (1%) | 7 (1%) | 163 (10%) | 139 (8%) |
| a The majority of subjects received placebo; 254 subjects from a randomized, open-label post exposure prophylaxis study in households did not receive placebo or prophylaxis therapy. | ||||
Adverse events included are: all events reported in the treatment studies with frequency ≥ 1% in the oseltamivir 75 mg bid group.
Additional adverse events occurring in < 1% of patients receiving TAMIFLU for treatment included unstable angina, anemia, pseudomembranous colitis, humerus fracture, pneumonia, pyrexia, and peritonsillar abscess.
Treatment Studies in Pediatric Patients
A total of 1032 pediatric patients aged 1 to 12 years (including 698 otherwise healthy pediatric patients aged 1 to 12 years and 334 asthmatic pediatric patients aged 6 to 12 years) participated in phase III studies of TAMIFLU given for the treatment of influenza. A total of 515 pediatric patients received treatment with TAMIFLU for Oral Suspension.
Adverse events occurring in ≥ 1% of pediatric patients receiving TAMIFLU treatment are listed in Table 4. The most frequently reported adverse event was vomiting. Other events reported more frequently by pediatric patients treated with TAMIFLU included abdominal pain, epistaxis, ear disorder, and conjunctivitis. These events generally occurred once and resolved despite continued dosing. They did not cause discontinuation of drug in the vast majority of cases.
The adverse event profile in adolescents is similar to that described for adult patients and pediatric patients aged 1 to 12 years.
Prophylaxis in Pediatric Patients
Pediatric patients aged 1 to 12 years participated in a postexposure prophylaxis study in households, both as index cases (134) and as contacts (222). Gastrointestinal events were the most frequent, particularly vomiting. The adverse events noted were consistent with those previously observed in pediatric treatment studies (see Table 4).
Table 4: Most Frequent Adverse Events Occurring in Children
Aged 1 to 12 Years in Studies in Naturally Acquired Influenza
| Treatment Trialsa | Household Prophylaxis Trialb | ||||
| Adverse Event | Placebo N=517 |
Oseltamivir 2 mg/kg bid N=515 |
No Prophylaxisc N=87 |
Prophylaxis with Oseltamivir QDc N=99 |
|
| Vomiting | 48 | (9%) | 77 (15%) | 2 (2%) | 10 (10%) |
| Diarrhea | 55 | (11%) | 49 (10%) | - | 1 (1%) |
| Otitis media | 58 | (11%) | 45 (9%) | 2 (2%) | 2 (2%) |
| Abdominal pain | 20 | (4%) | 24 (5%) | - | 3 (3%) |
| Asthma (including aggravated) | 19 | (4%) | 18 (3%) | 1 (1%) | 1 (1%) |
| Nausea | 22 | (4%) | 17 (3%) | 1 (1%) | 4 (4%) |
| Epistaxis | 13 | (3%) | 16 (3%) | - | 1 (1%) |
| Pneumonia | 17 | (3%) | 10 (2%) | 2 (2%) | - |
| Ear disorder | 6 | (1%) | 9 (2%) | - | - |
| Sinusitis | 13 | (3%) | 9 (2%) | - | - |
| Bronchitis | 11 | (2%) | 8 (2%) | 2 (2%) | - |
| Conjunctivitis | 2 | ( < 1%) | 5 (1%) | - | - |
| Dermatitis | 10 | (2%) | 5 (1%) | - | - |
| Lymphadenopathy | 8 | (2%) | 5 (1%) | - | - |
| Tympanic membrane disorder | 6 | (1%) | 5 (1%) | - | - |
| a Pooled data from Phase III
trials of TAMIFLU treatment of naturally acquired influenza. b A randomized, open-label study of household transmission in which household contacts received either prophylaxis orno prophylaxis but treatment if they became ill. Only contacts who received prophylaxis or who remained on noprophylaxis are included in this table. c Unit dose = age-based dosing |
|||||
| Age | Prophylaxis (10 days) |
| 1-2 years | 30 mg QD |
| 3-5 years | 45 mg QD |
| 6-12 years | 60 mg QD |
Adverse events included in Table 4 are: all events reported in the treatment studies with frequency ≥ 1% in the oseltamivir 75 mg bid group.
Observed During Clinical Practice
The following adverse reactions have been identified during postmarketing use of TAMIFLU. Because these reactions are reported voluntarily from a population of uncertain size, it is not possible to reliably estimate their frequency or establish a causal relationship to TAMIFLU exposure.
Body as a Whole: Swelling of the face or tongue, allergy, anaphylactic/anaphylactoid reactions
Dermatologic: Dermatitis, rash, eczema, urticaria, erythema multiforme, Stevens-Johnson Syndrome, toxic epidermal necrolysis (see PRECAUTIONS)
Digestive: Hepatitis, liver function tests abnormal
Cardiac: Arrhythmia
Gastrointestinal disorders: Gastrointestinal bleeding, hemorrhagic colitis
Neurologic: Seizure
Metabolic: Aggravation of diabetes
Psychiatric: Delirium, including symptoms such as altered level of consciousness, confusion, abnormal behavior, delusions, hallucinations, agitation, anxiety, nightmares (see PRECAUTIONS)
DRUG INTERACTIONS
The concurrent use of TAMIFLU with live attenuated influenza vaccine (LAIV) intranasal has not been evaluated. However, because of the potential for interference between these products, LAIV should not be administered within 2 weeks before or 48 hours after administration of TAMIFLU, unless medically indicated. The concern about possible interference arises from the potential for antiviral drugs to inhibit replication of live vaccine virus. Trivalent inactivated influenza vaccine can be administered at any time relative to use of TAMIFLU.
Information derived from pharmacology and pharmacokinetic studies of oseltamivir suggests that clinically significant drug interactions are unlikely.
Oseltamivir is extensively converted to oseltamivir carboxylate by esterases, located predominantly in the liver. Drug interactions involving competition for esterases have not been extensively reported in literature. Low protein binding of oseltamivir and oseltamivir carboxylate suggests that the probability of drug displacement interactions is low.
In vitro studies demonstrate that neither oseltamivir nor oseltamivir carboxylate is a good substrate for P450 mixed-function oxidases or for glucuronyl transferases.
Clinically important drug interactions involving competition for renal tubular secretion are unlikely due to the known safety margin for most of these drugs, the elimination characteristics of oseltamivir carboxylate (glomerular filtration and anionic tubular secretion) and the excretion capacity of these pathways. Coadministration of probenecid results in an approximate twofold increase in exposure to oseltamivir carboxylate due to a decrease in active anionic tubular secretion in the kidney. However, due to the safety margin of oseltamivir carboxylate, no dose adjustments are required when coadministering with probenecid.
No pharmacokinetic interactions have been observed when coadministering oseltamivir with amoxicillin, acetaminophen, cimetidine or with antacids (magnesium and aluminum hydroxides and calcium carbonates).
Generic Name: Oseltamivir Phosphate
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