Treatment with oseltamivir or zanamivir is
recommended for all persons with suspected or confirmed influenza requiring
hospitalization.
Early empiric
treatment with oseltamivir or zanamivir
should be considered for persons with suspected or confirmed influenza who are
at higher risk for complications including:
Children younger
than 2 years old;
Persons aged 65
years or older
Pregnant women
Persons of any age
with certain chronic medical or immunosuppressive conditions (see page 3); and,
Persons younger than 19 years of age who are receiving long-term aspirin
therapy.
Children 2 year to
4 years old are more likely to require hospitalization or urgent medical
evaluation for influenza compared with older children, although the risk is
much lower than for children younger than 2 years old. Children aged 2 years to 4 years without high
risk conditions and with mild illness do not necessarily require antiviral
treatment.
Treatment, when
indicated, should be initiated as early as possible because studies show that
treatment initiated early (i.e., within 48 hours of illness onset) is more
likely to provide benefit.
Actions that should
be taken to reduce delays in treatment initiation include:
Informing persons
at higher risk for influenza complications of signs and symptoms of influenza
and need for early treatment after onset of symptoms of influenza (i.e., fever,
respiratory symptoms);
Ensuring rapid
access to telephone consultation and clinical evaluation for these patients as
well as patients who report severe illness;
Considering empiric
treatment of patients at higher risk for influenza complications based on
telephone contact if hospitalization is not indicated and if this will
substantially reduce delay before treatment is initiated.
Treatment should
not wait for laboratory confirmation of influenza because laboratory testing
can delay treatment and because a negative rapid test for influenza does not
rule out influenza. The sensitivity of rapid tests in detecting 2009 H1N1 has
ranged from 10% to 70%. Information on the use of rapid influenza diagnostic tests
(RIDTs) can be found at
http://www.cdc.gov/h1n1flu/guidance/rapid_testing.htm.
Testing for 2009
H1N1 influenza infection with real-time reverse transcriptase-polymerase chain
reaction (rRT-PCR) should be prioritized for persons
with suspected or confirmed influenza requiring hospitalization and based on
guidelines from local and state health departments.
Consideration for
antiviral chemoprophylaxis should generally be reserved for persons at higher
risk for influenza-related complications who have had contact with someone
likely to have been infected with influenza. However, early treatment is an
emphasized alternative to chemoprophylaxis after a suspected exposure.
Household or close contacts (with risk factors for influenza complications) of
confirmed or suspected cases can be counseled about the early signs and
symptoms of influenza, and advised to immediately contact their health care
provider for evaluation and possible early treatment if clinical signs or
symptoms develop.
Based on global
experience to date, 2009 H1N1 influenza viruses likely will be the most common
influenza viruses among those circulating in the coming season, particularly
those causing influenza among younger age groups. Circulation of seasonal influenza viruses
during the 2009-10 season is also expected. Influenza
seasons are unpredictable, however, and the timing and intensity of seasonal
influenza virus activity versus 2009 H1N1 circulation cannot be predicted in
advance.
Currently
circulating 2009 H1N1 viruses are susceptible to oseltamivir
and zanamivir, but resistant to amantadine
and rimantadine; however, antiviral treatment
regimens might change according to new antiviral resistance or viral
surveillance information.
Information on the
dose and dosing schedule for oseltamivir and zanamivir is provided in this document. An April 2009
Emergency Use Authorization authorizes the emergency use of oseltamivir
in children younger than 1 year old (http://www.cdc.gov/h1n1flu/eua/), subject
to the terms and conditions of the EUA
Background
As of September 12,
2009, 99% of circulating influenza viruses in the United States were 2009 H1N1
influenza (previously referred to as novel influenza A (H1N1)). Among people
who become infected with 2009 H1N1, certain groups appear to be at increased
risk of complications and may benefit most from early treatment with antiviral
medications. Approximately 70% of persons hospitalized with 2009 H1N1 influenza
have had a recognized high risk condition. These groups are similar to those
who are at increased risk for seasonal influenza-related complications:
Children younger
than 2 years old;
Adults 65 years of
age or older
Pregnant women
Persons with the
following conditions:
Chronic pulmonary
(including asthma), cardiovascular (except hypertension), renal, hepatic,
hematological (including sickle cell disease), or metabolic disorders
(including diabetes mellitus);
Disorders that that
can compromise respiratory function or the handling of respiratory secretions
or that can increase the risk for aspiration (e.g., cognitive dysfunction,
spinal cord injuries, seizure disorders, or other neuromuscular disorders)
Immunosuppression, including that caused by medications or by HIV;
Persons younger than 19 years of age who are receiving long-term aspirin
therapy, because of an increased risk for Reye syndrome.
Among children,
rates of influenza-associated hospitalization from 2009 H1N1 have varied by age
group. The risk of influenza-associated hospitalizations in healthy children
younger than 2 years old is equal to or greater than the risk of other
high-risk groups. During April to August 2009 hospitalization rates for
laboratory-confirmed 2009 H1N1 influenza among children younger than 2 years
old were 2.5 times higher than rates for children 2 year to 4 years old.
Children 2 years to 4 years old had slightly (20%) higher rates of
hospitalization compared with children 5 years to 17 years old. In studies of
seasonal influenza, the risk for hospitalization is also highest for infants,
with the risk decreasing as age increases. Given this increased risk for
hospitalization, children younger than 2 years old are generally recommended
for antiviral treatment. Children ages 2 through 4 years old without high risk
conditions (see above) and who are not severely ill do not necessarily require
antiviral treatment. Health care providers should use clinical judgment to
guide treatment decisions. Children of any age presenting with suspected
influenza and symptoms of lower respiratory tract illness or clinical deterioration
should receive prompt empiric antiviral therapy in addition to other indicated
treatment (e.g. antibiotics if bacterial co-infection is suspected). Updated
information on hospitalization rates by age group can be found at
www.cdc.gov/flu/weekly.
Persons 65 years and older are less likely to become ill with 2009 H1N1
influenza compared to younger persons. However, when persons aged 65 years or older
acquire influenza, they are at higher risk for severe influenza-related
complications.
Preliminary studies
suggest that people who are morbidly obese (body mass index equal to or greater
than 40) and perhaps people who are obese (body mass index 30 to 39) may be at
increased risk of hospitalization and death due to 2009 H1N1 influenza
infection. Additional studies to determine the risk of morbid obesity and /or
obesity for these complications of 2009 H1N1 virus infection are underway.
Patients with morbid obesity, and perhaps obesity, often have underlying
conditions that put them at increased risk for complications due to 2009 H1N1
influenza infection, such as diabetes, asthma, chronic respiratory illness or
liver disease. Patients with obesity or morbid obesity should be carefully
evaluated for the presence of underlying medical conditions that are known to
increase the risk for influenza complications, and receive empiric treatment
when these conditions are present, or if signs of lower respiratory tract
infection are present
Transmission of
2009 H1N1 influenza is being studied as part of the ongoing epidemiologic
investigation, but data available indicate that this virus appears to be
transmitted in ways similar to other influenza viruses. All respiratory
secretions and bodily fluids (including diarrheal stool) of 2009 H1N1 cases
should be considered potentially infectious.
Close contact, for
the purposes of this document, is defined as having cared for or lived with a
person who is a confirmed, probable, or suspected case of influenza, or having
been in a setting where there was a high likelihood of contact with respiratory
droplets and/or body fluids of such a person. Examples of close contact include
sharing eating or drinking utensils, physical examination, or any other contact
between persons likely to result in exposure to respiratory droplets. Close
contact typically does not include activities such as walking by an infected
person or sitting across from a symptomatic patient in a waiting room or
office.
Special
Considerations for Children
Aspirin or aspirin-containing
products (e.g. bismuth subsalicylate – Pepto Bismol) should not be administered to any confirmed or
suspected ill case of influenza aged 18 years old and younger due to the risk
of Reye syndrome. For relief of fever, other anti-pyretic medications such as
acetaminophen or non-steroidal anti-inflammatory drugs are recommended.
Children younger
than 4 years of age should not be given over-the-counter cold medications
without first speaking with a health care provider.
Antiviral Treatment
Recommendations for
use of antiviral medications may change as data on antiviral effectiveness,
clinical spectrum of illness, adverse events from antiviral use, or resistance
among circulating viruses become available. As of September 12, 2009, 99% of circulating
influenza viruses were 2009 H1N1 viruses susceptible
to both oseltamivir and zanamivir.
These treatment guidelines therefore focus on use of antiviral medications
effective against 2009 H1N1 viruses. For antiviral treatment of 2009 H1N1 virus
infection, either oseltamivir or zanamivir
are recommended (Table 1).
Clinical judgment
is an important factor in treatment decisions. Most patients who have had 2009
H1N1 virus infection have had a self-limited respiratory illness similar to
typical seasonal influenza. Most healthy persons who develop suspected or
confirmed 2009 H1N1 influenza or seasonal influenza who
present with an uncomplicated febrile illness generally do not require
antiviral treatment. In addition, persons who appear to be recovering from
influenza generally do not require antiviral treatment. However, some groups
appear to be at increased risk of influenza-related complications. Local public
health authorities might provide additional guidance about prioritizing
treatment within groups at higher risk for severe infection.
Treatment is
recommended for all hospitalized patients with confirmed, probable or suspected
2009 H1N1 or seasonal influenza.
Early empiric
treatment should be considered for outpatients who are at higher risk for influenza-related
complications (see above). Clinical judgment should be used in deciding whether
outpatients with risk factors for influenza-related complications require
treatment.
Treatment with oseltamivir or zanamivir is
recommended for persons with suspected or confirmed influenza who are severely
ill or who are showing evidence of rapid clinical deterioration. Signs and
symptoms of severe illness due to suspected influenza are in indication for
immediate treatment, regardless of previous health or age.
Treatment should be
initiated empirically when the decision is made to treat patients who have
illnesses that are clinically compatible with influenza. Treatment should not
await laboratory confirmation because laboratory-based testing could delay
treatment and because a negative rapid test does not rule out influenza. (See
“Evaluation of Rapid Influenza Diagnostic Tests for Detection of Novel
Influenza A (H1N1) Virus --- United States, 2009” for more information about
the sensitivity of rapid tests.)
These
recommendations should be used together with clinical judgment in making
treatment decisions for both patients who are at higher risk for
influenza-related complications and patients who are not at higher risk. When
evaluating previously healthy children with possible influenza, clinicians
should be aware that, similar to seasonal influenza, the risk for developing
severe disease is likely to be highest among infants and younger children. Once
the decision to administer antiviral treatment is made by the health care
provider, treatment with zanamivir or oseltamivir should be initiated as soon as possible after
the onset of symptoms.
Evidence for
benefits from antiviral treatment in studies of uncomplicated seasonal
influenza is strongest when treatment is started within 48 hours of illness
onset. Initiating treatment as soon as possible after illness onset is also
thought likely to reduce the risk of severe outcomes including severe illness
or death. However, some studies of hospitalized patients with seasonal
influenza treated with oseltamivir have suggested
benefit, including reductions in mortality or duration of hospitalization, even
for patients whose treatment was started more than 48 hours after illness
onset. The recommended duration of treatment is five days. Hospitalized
patients with severe infections (such as those with prolonged infection or who
require intensive unit care admission) might require longer treatment courses.
Antiviral doses recommended for treatment of 2009 H1N1 influenza virus infection
in adults or children 1 year of age or older are the same as those recommended
for seasonal influenza (Table 1). Some experts have advocated use of increased
(doubled) doses of oseltamivir for some severely ill
patients, although there are no published data demonstrating that higher doses
are more effective. Oseltamivir use for children
younger than 1 year old was recently authorized by the U.S. Food and Drug
Administration (FDA) under an Emergency Use Authorization (EUA).
These EUA provisions apply only when the product is
provided in accordance with the local public health authority's response plans.
Dosing for children younger than 1 year old is age-based in the EUA guidance. However, some experts who are currently
conducting studies on oseltamivir use in this age
group prefer weight based dosing for this age group, particularly for premature
or underweight infants. (Table 2) (See Emergency Use Authorization of Tamiflu (oseltamivir) ).
Persons at higher
risk for complications from influenza or who have already developed severe
illness should be treated as quickly as possible after signs or symptoms
develop. To reduce delays in starting treatment, health care providers should:
Provide information
for patients at higher risk for influenza complications about signs and
symptoms of influenza and need for early treatment after symptom onset when ill
with influenza;
Ensure rapid access
to telephone consultation and clinical evaluation for these patients as well as
patients who report severe illness;
Consider empiric
treatment of patients who have illnesses compatible with influenza and are at
higher risk for influenza complications based on telephone contact if
hospitalization is not indicated and if this will substantially reduce delay
before treatment is initiated and additional medical evaluation can be arranged
if needed;
Request that
patients at higher risk for influenza complications contact the provider if
signs or symptoms of influenza develop, obtain
medication as quickly as possible if prescribed by the provider, and initiate
treatment. Providers should take into account patient reliability, ability to
understand the information about symptoms of influenza, and access to a
pharmacy when considering ways to reduce treatment delays.
Counsel patients about influenza antiviral benefits and adverse effects,
the potential for continued susceptibility to influenza virus infection after
treatment is completed (because of other circulating influenza viruses or if
illness was due to another cause), and the need to again seek early access to
health care consultation if symptoms recur.
Patients receiving
treatment should be advised that they remain potentially infectious to others
while on treatment. Despite treatment with antiviral agents, including treatment
with the neuraminidase inhibitors, patients may continue to shed influenza
virus for up to four or more days after beginning therapy. Therefore, patients
should continue good hand washing and respiratory hygiene practices during the
entire period on therapy to prevent the transmission of virus to close
contacts. View information about homecare of ill persons for providers and
patients is available at: Taking Care of a Sick Person in Your Home and
Physician Directions to Patient/Parent.
Treatment of influenza
when oseltamivir-resistant viruses are circulating
Oseltamivir resistance is
common among seasonal influenza A (H1N1) viruses. These viruses typically
remain susceptible to rimantadine and amantadine. However, since April 2009, very few seasonal H1N1
viruses have circulated in the United States. Therefore, treatment, when
indicated, with either oseltamivir or zanamivir is appropriate. However, if viral surveillance
data indicate that oseltamivir-resistant seasonal
H1N1 viruses have become more common or are associated with identified
community outbreaks, zanamivir or a combination of oseltamivir and rimantadine or amantadine should be considered for use as empiric
treatment for patients who might have oseltamivir-resistant
seasonal human influenza A (H1N1) virus infection. National surveillance data
on influenza viruses circulating in the United States is available and is
updated weekly. State and local health departments are also a source of viral
surveillance data in some areas. Guidance on empiric treatment recommendations
when multiple influenza strains are circulating is available at
http://www2a.cdc.gov/HAN/ArchiveSys/ViewMsgV.asp?AlertNum=00279.
Antiviral
Chemoprophylaxis
The infectious
period for persons infected with the 2009 H1N1 virus appears to be similar to
that observed in studies of seasonal influenza. Infected persons may shed
influenza virus, and potentially be infectious to others, beginning one day
before they develop symptoms to up to 7 days after they become ill. Children,
especially younger children, and persons who are immune compromised can shed
influenza virus for longer periods. However, the amount of virus shed generally
correlates with magnitude of fever and for these recommendations,
the infectious period for influenza is defined as one day before until 24 hours
after fever ends.
Post exposure
antiviral chemoprophylaxis with either oseltamivir or
zanamivir can be considered for the following:
Persons who are at higher risk for complications of influenza and are a
close contact of a person with confirmed, probable, or suspected 2009 H1N1 or
seasonal influenza during that person’s infectious period.
Health care
personnel, public health workers, or first responders who have had a
recognized, unprotected close contact exposure to a person with confirmed,
probable, or suspected 2009 H1N1 or seasonal influenza during that person’s
infectious period. Information on appropriate personal protective equipment is
available at: Infection Control for Patients in a Healthcare Setting and might
be updated frequently as additional information on transmission becomes
available.
Antiviral agents
should not be used for post exposure chemoprophylaxis in healthy children or
adults based on potential exposures in the community, school, camp or other
settings.
Chemoprophylaxis
generally is not recommended if more than 48 hours have elapsed since the last
contact with an infectious person.
Chemoprophylaxis is
not indicated when contact occurred before or after, but not during, the ill
person’s infectious period as defined above.
Patients given
post-exposure chemoprophylaxis should be informed that the chemoprophylaxis
lowers but does not eliminate the risk of influenza and that protection stops
when the medication course is stopped. Patients receiving chemoprophylaxis
should be encouraged to seek medical evaluation as soon as they develop a
febrile respiratory illness that might indicate influenza. For antiviral
chemoprophylaxis of 2009 H1N1 influenza virus infection, either oseltamivir or zanamivir is
recommended (Table 1). Duration of post-exposure chemoprophylaxis is 10 days
after the last known exposure to 2009 H1N1 influenza.
Oseltamivir was authorized for
use for chemoprophylaxis under the EUA for children
younger than 1 year of age, subject to the terms and conditions of the EUA. (See Treatment and Chemoprophylaxis
for Children Younger than 1 Year of Age, below.) Age-based dosing
recommendations are provided in the fact sheetsincluded
with the EUA letter of authorization, however
weight-based dosing is an alternative preferred by some experts who are
currently conducting studies of oseltamivir use in
this age group.
An emphasis on
early treatment is an alternative to chemoprophylaxis after a suspected
exposure. Persons with risk factors for influenza complications who are
household or close contacts of confirmed or suspected cases, and health care personnel who have occupational exposures, can be counseled
about the early signs and symptoms of influenza, and advised to immediately
contact their health care provider for evaluation and possible early treatment
if clinical signs or symptoms develop. Health care providers should use
clinical judgment regarding situations where early recognition of illness and
treatment might be an appropriate alternative to chemoprophylaxis.
Persons at ongoing
occupational risk for exposure (e.g., health care personnel, public health
workers, or first responders who are working in communities with influenza
outbreaks) should carefully follow guidelines for appropriate personal
protective equipment. Efforts to reduce the risk of exposure or infection for
healthcare personnel should include appropriate administrative controls (e.g.
having health care personnel stay home from work when ill, and triaging for
identification of potentially infectious patients), cough and hand hygiene,
personal protective equipment, and vaccination when available.
Antiviral
Resistance
2009 H1N1 influenza
viruses are susceptible to the neuraminidase inhibitor antiviral medications, oseltamivir and zanamivir, but
are resistant to the adamantane antiviral
medications, amantadine and rimantadine.
This susceptibility pattern is the same as that observed among seasonal influenza
A (H3N2) and B viruses in recent years. Oseltamivir
resistance appears to be rare at this time. However, oseltamivir-resistant
2009 H1N1 viruses have been identified, typically among persons who develop
illness while receiving oseltamivir for chemoprophylaxis
or immunocompromised patients with influenza who are
being treated.These findings underscore the
importance of careful and limited use of antiviral medications for
chemoprophylaxis and the need for persons taking antiviral medications to
continue to follow recommendations for hand and respiratory hygiene to prevent
the spread of antiviral resistant viruses. Additional information on oseltamivir resistance among 2009 H1N1 viruses is available
at http://www.cdc.gov/h1n1flu/HAN/070909.htm. Monitoring for antiviral
resistance is ongoing and clinicians and state health departments should
continue to follow state and national guidance for submission and testing of
clinical specimens from persons with suspected 2009 H1N1 virus infection,
particularly from those who develop influenza while taking chemoprophylaxis or
who have prolonged viral shedding while on treatment.
Antiviral Use for
Control of 2009 H1N1 Influenza Outbreaks
Use of antiviral
drugs for treatment and chemoprophylaxis of influenza has been a cornerstone
for the control of seasonal influenza outbreaks in nursing homes and other
long-term care facilities that house large numbers of patients at higher risk
for influenza complications. (See MMWR: Prevention
and Control of Influenza: Recommendations of the Advisory Committee on
Immunization Practices (ACIP), 2008). At this time,
no outbreaks of 2009 H1N1 have been reported in such settings. This may be the
result of some level of immunity among persons 65 years and older and/or
possibly fewer exposures of such persons to 2009 H1N1 thus far. However, if
such outbreaks were to occur, it is recommended that ill patients be treated
with oseltamivir or zanamivir
and that chemoprophylaxis with either oseltamivir or zanamivir be started as early as possible to reduce the
spread of the virus as is recommended for seasonal influenza outbreaks in such
settings. Additional guidance for infection control measures in long-term care
facilities can be found at: Using Antiviral Medications to Control Influenza
Outbreaks in Institutions.
In addition to use
in nursing homes, antiviral chemoprophylaxis also can be considered for
controlling influenza outbreaks in other closed or semi-closed settings (e.g.,
correctional facilities, or other settings in which persons live in close
proximity) where large numbers of persons at higher risk for influenza
complications are housed. For more information about influenza outbreaks in
facilities see:
Prevention and
Control of Influenza: Recommendations of the Advisory Committee on Immunization
Practices (ACIP), 2009
Seasonal Influenza
in Adults and Children—Diagnosis, Treatment, Chemoprophylaxis, and
Institutional Outbreak Management: Clinical Practice Guidelines of the
Infectious Diseases Society of America (available at: http://www.journals.uchicago.edu/doi/pdf/10.1086/598513).
Interim Guidance
for Correctional and Detention Facilities on Novel Influenza A (H1N1) Virus
Interim Guidance
for Homeless and Emergency Shelters on the Novel Influenza A (H1N1) Virus
Outbreaks in
schools, camps, workplaces and other group settings should not be managed by
providing chemoprophylaxis to all persons potentially exposed to influenza
viruses. The healthy populations typically present in these settings should be
educated about the signs and symptoms of influenza, and urged to consult their
health care provider if severe illness develops. Post-exposure chemoprophylaxis
can be considered for those who meet the above criteria for exposure and who
have a medical condition or are of an age that confers a higher risk for
influenza complications. An emphasis on early evaluation and treatment, as
described above, is an alternative. Persons in these settings also should be
educated about hygiene and infection control measures that can reduce
transmission of influenza viruses.
Table 1.Antiviral medication dosing recommendations for treatment or
chemoprophylaxis of 2009 H1N1 infection.
(Table extracted
from product information for Tamiflu® and Relenza®)
MedicationTreatment
(5
days)Chemoprophylaxis
(10 days)
Oseltamivir
Adults
75-mg capsule twice per day75-mg capsule once
per day
Children ≥ 12
months
Body Weight (kg)Body Weight (lbs)
≤15 kg≤33lbs30
mg twice daily30 mg once per day
> 15 kg to 23
kg>33 lbs to 51 lbs45 mg twice daily45 mg once per day
>23 kg to 40
kg>51 lbs to 88 lbs60 mg twice daily60 mg once per day
>40 kg>88
lbs75 mg twice daily75 mg once per day
Zanamivir
Adults
10 mg (two 5-mg inhalations) twice daily10 mg
(two 5-mg inhalations) once daily
Children (≥7
years or older for treatment, ≥5 years for chemoprophylaxis)
10 mg (two 5-mg inhalations) twice daily 10 mg (two 5-mg
inhalations) once daily
Health care
providers and pharmacists should be aware that an oral dosing dispenser with 30
mg, 45 mg, and 60 mg graduations is provided with TAMIFLU®
for Oral Suspension, rather than graduations in milliliters (mL) or teaspoons (tsp). There have been cases where the
units of measure on the prescription instructions (mL,
tsp) do not match the units on the dosing device (mg), which has lead to patient
or caregiver confusion and dosing errors. When dispensing commercially
manufactured TAMIFLU® for Oral Suspension,
pharmacists should ensure the units of measure on the prescription instructions
match the dosing device. If prescription instructions specify administration
using millilters (mL) or
teaspoons (tsp), then the device included in the Tamiflu®
product package should be removed and replaced with an appropriate measuring
device, such as an oral syringe if the prescribed dose is in milliliters (mL).
Treatment and
Chemoprophylaxis for Children younger than 1 Year of Age
Children younger
than 1 year of age are at higher risk for influenza-related complications and
have a higher rate of hospitalization compared to older children. Oseltamivir is not approved for use in children younger
than 1 year of age. However, limited safety data on oseltamivir
treatment of seasonal influenza in children younger than 1 year of age suggest
that severe adverse events are rare. Oseltamivir is
authorized for emergency use in children younger than 1 year of age under an EUA issued by FDA, subject to
the terms and conditions of the EUA.
Because infants
experience high rates of morbidity and mortality from influenza, infants with
2009 H1N1 influenza virus infections may benefit from treatment using oseltamivir. (Table 2 and Emergency Use
Authorization of Tamiflu (oseltamivir)).
Table 2. Dosing
recommendations for antiviral treatment or chemoprophylaxis of children younger
than 1 year using oseltamivir.
Age Recommended treatment dose for 5 daysRecommended
prophylaxis dose for 10 days
Younger than 3
months12 mg twice dailyNot recommended unless
situation judged critical due to limited data on use in this age group
3-5 months20 mg
twice daily20 mg once daily
6-11 months25 mg
twice daily25 mg once daily
When dispensing TAMIFLU® for Oral Suspension for children younger than 1
year of age, the oral dosing dispenser that is included in the Tamiflu package should always be removed. Pharmacists and health care providers should provide
an oral syringe that is capable of accurately measuring the prescribed
milliliter (mL) dose, and counsel the caregiver how
to administer the prescribed dose.
Some experts prefer
weight-based dosing for children aged younger than 1 year, particularly for
very young or premature infants based on preliminary data from a National
Institutes of Health-funded Collaborative Antiviral Study Group (CASG). When using
weight-based dosing for infants aged younger than 1 year for treatment, those 9
months or older should receive 3.5 mg/kg/dose BID, and those aged younger than
9 months should receive 3.0 mg/kg/dose BID. When using weight-based dosing for
infants aged younger than 1 year for chemoprophylaxis, those 9 months or older
should receive 3.5 mg/kg/dose QD, and those aged
younger than 9 months should receive 3.0 mg/kg/dose QD
(Source: D Kimberlin et al. Oseltamivir
(OST) and OST Carboxylate (CBX)
Pharmacokinetics (PK) in Infants: Interim Results
from a Multicenter Trial. Abstract accepted to Infectious Diseases Society of
America meeting, October 2009). Health care providers should be aware of the
lack of data on safety and dosing when considering oseltamivir
use in a seriously ill young infant with confirmed 2009 H1N1 influenza virus
infection or who has been exposed to a confirmed 2009 H1N1 influenza case, and
carefully monitor infants for adverse events when oseltamivir
is used. Additional information on oseltamivir for
this age group can be found at:
http://www.fda.gov/downloads/Drugs/DrugSafety/InformationbyDrugClass/UCM153547.pdf
Pregnant Women
Pregnant women are
known to be at higher risk for complications from infection with seasonal
influenza viruses, and severe disease among pregnant women was reported during
past pandemics. Hospitalizations and deaths have been reported among pregnant
women with 2009 H1N1 influenza virus infection, and one study estimated that
the risk for hospitalization for 2009 H1N1 influenza was four times higher for
pregnant women than for the general population. While oseltamivir
and zanamivir are "Pregnancy Category C"
medications, indicating that no clinical studies have been conducted to assess
the safety of these medications for pregnant women, the available risk-benefit
data indicate pregnant women with suspected or confirmed influenza should
receive prompt antiviral therapy. Pregnancy should not be considered a
contraindication to oseltamivir or zanamivir use. Because of its systemic activity, oseltamivir is preferred for treatment of pregnant women.
The drug of choice for chemoprophylaxis is less clear. Zanamivir
may be preferable because of its limited systemic absorption; however,
respiratory complications that may be associated with zanamivir
because of its inhaled route of administration need to be considered, especially
in women at risk for respiratory problems.