CDC Recommends against the Use of
Amantadine and Rimantadine for the Treatment or Prophylaxis of Influenza in the
United States during the 2005–06 Influenza Season
Recent evidence indicates that a
high proportion of currently circulating Influenza A viruses in this country
are resistant to these medications
While the primary strategy for preventing complications of
influenza infections is annual vaccination, antiviral medications with activity
against influenza viruses can be effective for the prophylaxis and treatment of
influenza. Two classes of antivirals are currently available—the M2 ion channel
inhibitors (i.e., the two adamantanes amantadine and rimantadine) and the
neuraminidase inhibitors (i.e., oseltamivir and zanamivir). The neuraminidase
inhibitors are effective for the treatment and prophylaxis of influenza A and
B, while the adamantanes are only active against influenza A viruses. This
alert provides new information about the resistance of influenza viruses
currently circulating in the United States to the adamantanes, and it makes an
interim recommendation that these drugs not be used during the 2005–06
influenza season. Amantadine is also used to treat the symptoms of Parkinson’s
disease, and should continue to be used for this indication.
Viral resistance to adamantanes can emerge rapidly during
treatment because a single point mutation at amino acid positions 26, 27, 30,
31, or 34 of the M2 protein can confer cross-resistance to both amantadine and
rimantadine. The transmissibility of adamantane-resistant viruses is not
impaired by any of these amino acid changes. A recent report on the global
prevalence of adamantane-resistant influenza viruses showed a significant
increase (from 1.9% to 12.3%) in drug resistance over the past 3 years. In the
United States, the frequency of drug resistance increased from 1.9% in 2004 to
14.5% during the first 6 months of the 2004–05 influenza season.
For the 2005–06 season, 120 influenza A (H3N2) viruses
isolated from patients in 23 states have been tested at CDC through January 12,
2006; 109 of the isolates (91%) contain an amino acid change at position 31 of
the M2 protein, which confers resistance to amantadine and rimantadine. Three
influenza A(H1N1) viruses have been tested and demonstrated susceptibility to
these drugs. All influenza viruses from the United States that have been
screened for antiviral resistance at CDC have demonstrated susceptibility to
the neuraminidase inhibitors.
On the basis of available antiviral testing results, CDC is
providing an interim recommendation that neither amantadine nor rimantadine be
used for the treatment or prophylaxis of influenza A in the United States for
the remainder of the 2005–06 influenza season. During this period, oseltamivir
or zanamivir should be selected if an antiviral medication is used for the
treatment and prophylaxis of influenza. Testing of influenza isolates for
resistance to antivirals will continue throughout the 2005–06 influenza season,
and recommendations will be updated as needed. Annual influenza vaccination
remains the primary means of preventing morbidity and mortality associated with
influenza.
Additional information about the prevention and control of
influenza is available at http://www.cdc.gov/flu/.
Specific information regarding the use of the neuraminidase inhibitors is
available at http://www.cdc.gov/flu/protect/antiviral/index.htm.
These websites will be updated as new information becomes available.
