Date: Fri, 21 Apr 1995 10:14:35 +0500
From: ghmcleaf{CONTRACTOR/ASPEN/ghmcleaf}%NAC-GATEWAY.ASPEN@ace.aspensys.com
Subject: MMWR 04/21/95


MORBIDITY AND MORTALITY WEEKLY REPORT
Centers for Disease Control and Prevention
April 21, 1995
Vol. 44, No. 15


Update: Influenza Activity -- United States and Worldwide, 1994-95
Season, and Composition of the 1995-96 Influenza Vaccine
     In collaboration with the World Health Organization (WHO) and
the international network of collaborating laboratories and with
state and local health departments in the United States, CDC
conducts surveillance to monitor influenza activity and to detect
antigenic changes in the circulating strains of influenza viruses.
This report summarizes surveillance for influenza in the United
States and worldwide during the 1994-95 season and describes the
composition of the 1995-96 influenza vaccine.
United States
     Influenza activity began in the Northeast in late November
1994 and from late January to early February spread to other
regions of the country. Activity peaked during March and continues
to decline.
     From November 27, 1994, through January 14, 1995, regional or
widespread influenza activity* was reported only from northeastern
states. Regional activity was first reported outside this area for
the week ending January 21, and by February 11 regional or
widespread activity had been reported from every region in the
country. Based on reports from state and territorial
epidemiologists, peak activity occurred the week ending March 11,
1995, when 26 states reported either regional or widespread
activity. The number of states reporting regional or widespread
activity has declined every week since March 12. For the week
ending April 8, four states reported regional activity, and none
reported widespread activity.
     Of total deaths reported through CDC's 121-city mortality
surveillance system, the proportion attributed to pneumonia and
influenza exceeded the epidemic threshold** for 11 of the 27 weeks
from October 2, 1994, through April 8, 1995. Pneumonia and
influenza deaths exceeded the epidemic threshold for 2 consecutive
weeks twice during this interval.
     Of the 3423 influenza virus isolates reported to CDC from WHO
collaborating laboratories in the United States through April 8, a
total of 2654 (78%) were type A and 769 (22%) were type B. Of the
1337 type A viruses that have been subtyped, 1318 (99%) were type
A(H3N2) and 19 (1%) were type A(H1N1).
Worldwide
     Influenza activity has occurred at low to moderate levels in
most parts of the world. Although a few countries reported epidemic
activity, sporadic activity or localized outbreaks were reported
more frequently. Influenza activity was usually associated with
cocirculation of influenza A(H3N2) and influenza B viruses.
Influenza A(H1N1) activity was reported only in association with
sporadic cases. Influenza A(H3N2) viruses were first detected
during October in Europe and North America. Outbreaks associated
with influenza A(H3N2) were subsequently reported in the People's
Republic of China, Finland, Hungary, Italy, Spain, the United
Kingdom, and the United States. Although influenza A and influenza
B cocirculated, influenza A(H3N2) viruses predominated in Canada,
Finland, France, Italy, Spain, and the United States.
     Influenza type B viruses were first detected this season in
Europe in association with a secondary school outbreak in Portugal
during October. Outbreaks caused by influenza B were reported
subsequently in China, Iran, Italy, and the United States. Epidemic
activity associated with influenza B was reported in Italy and
Russia. In Germany, the Netherlands, Portugal, Russia, and the
United Kingdom, influenza B viruses were isolated more frequently
than influenza A(H3N2) viruses.
     Influenza A(H1N1) viruses have been reported in association
with sporadic activity from Canada, China, Hong Kong, the
Netherlands, Norway, Poland, Singapore, Switzerland, Thailand, the
United Kingdom, and the United States during the 1994-95 season.
Composition of the 1995-96 Vaccine
     The Food and Drug Administration Vaccines and Related
Biologicals Advisory Committee (VRBAC) has recommended that the
1995-96 trivalent influenza vaccine for the United States contain
A/Johannesburg/33/94-like (H3N2), A/Texas/36/91-like (H1N1) and
B/Beijing/184/93-like viruses. This recommendation was based on the
antigenic analysis of recently isolated influenza viruses and the
antibody responses of persons vaccinated with the 1994-95 vaccine.
     Although many of the influenza type A(H3N2) viruses that have
been antigenically characterized are similar to the
A/Shangdong/09/93 strain, some recently isolated A(H3N2) strains
from Asia, Europe, and North America are more similar to the
antigenic variant A/Johannesburg/33/94 (Table 1). Vaccines
containing the A/Shangdong/09/93(H3N2)-like virus induced a good
antibody response to the vaccine strain but induced lower and less
frequent antibody responses to recent type A(H3N2) strains such as
A/Johannesburg/33/94 (1). Therefore, VRBAC recommended changing the
influenza type A(H3N2) vaccine component to an
A/Johannesburg/33/94-like strain for the 1995-96 season.
     Many recent influenza B viruses isolated from Asia, Europe,
and North America are antigenically distinguishable from the
B/Panama/45/90 strain included in the 1994-95 vaccine. These recent
viruses are similar to the B/Beijing/184/93, B/Shanghai/04/94, and
B/Harbin/07/94 strains. These strains, which are themselves
antigenically indistinguishable, have been used as reference
strains for antigenic analysis (Table 2). Although vaccines
containing B/Panama/45/90 virus induced antibodies at a similar
frequency and titer as the vaccine virus for some recent influenza
B strains, in some studies the antibody response in adults and the
elderly was reduced to the B/Beijing/ 184/93-like strain,
B/Shanghai/04/94. VRBAC recommended changing the influenza B
component to a B/Beijing/184/93-like virus for the 1995-96 season.
The actual strain used by U.S. vaccine manufacturers will be
B/Harbin/07/94 because of its growth properties.
     Since the 1992-93 influenza season, isolation of influenza
type A(H1N1) virus has been sporadic worldwide (2). Nine recent
viruses from China and the United States have been characterized as
being related to the reference strains A/Taiwan/01/86 and
A/Texas/36/91. Vaccines containing the A/Texas/36/91 strain induced
antibodies with similar frequency and titer to the vaccine virus
and to type A(H1N1) strains isolated in 1993 and 1994. Therefore,
VRBAC recommended retaining an A/Texas/36/91-like strain in the
1995-96 vaccine.
Reported by: Participating state and territorial health dept
epidemiologists and state public health laboratory directors. M
Chakraverty, PhD, Central Public Health Laboratory, A Hay, PhD,
National Institute for Medical Research, London; G Schild, PhD, J
Wood, PhD, National Institute for Biological Standards and Control,
Hertfordshire, England. I Gust, MD, A Hampson, Commonwealth Serum
Laboratories, Parkville, Australia. J Weber, Laboratory Center for
Disease Control, Ottawa, Ontario. J Kim, PhD, K Park, PhD, National
Institute of Health, Seoul, Korea. E Claas, PhD, Eramus University,
Rotterdam, The Netherlands. World Health Organization National
Influenza Centers, Program on Bacterial, Viral Diseases, and
Immunology, Geneva. Div of Virology, Center for Biologics
Evaluation and Research, Food and Drug Administration. Influenza
Br, Div of Viral and Rickettsial Diseases, National Center for
Infectious Diseases, CDC.
Editorial Note: During the 1994-95 season, the impact of influenza
in most parts of the United States and in most other countries in
the Northern Hemisphere was less severe than during the previous
season, when A/Beijing/32/92-like (H3N2) viruses predominated.
Although approximately 75% of influenza viruses circulating in the
United States during the 1994-95 season have been type A(H3N2),
compared with the 1993-94 season, influenza spread more slowly and
was associated with less severe illness. The results of mortality
surveillance based on the 121-city system suggest relatively low
influenza-associated mortality in the United States this season and
are consistent with other influenza surveillance findings.
     Strains to be included in next season's influenza vaccine are
selected usually during the preceding January through March because
of scheduling requirements for production, quality control,
packaging, and distribution of vaccine for administration before
onset of the next influenza season. Recommendations of the Advisory
Committee on Immunization Practices for the use of vaccine and
antiviral agents for prevention and control of influenza have been
published in the MMWR Recommendations and Reports (3).
References
1. World Health Organization. Recommended composition of influenza
virus vaccines for use in the 1995-96 season. Wkly Epidemiol Rec
1995;70:53-6.
2. CDC. Update: influenza activity--United States and worldwide,
1993-94 season, and composition of the 1994-95 influenza vaccine.
MMWR 1994;43:179-83.
3. CDC. Prevention and control of influenza: recommendations of the
Advisory Committee on Immunization Practices (ACIP). MMWR
1995;44(no. RR-3).

* Levels of activity are 1) sporadic--sporadically occurring
influenza-like illness (ILI) or culture-confirmed influenza, with
no outbreaks detected; 2) regional--outbreaks of ILI or
culture-confirmed influenza in counties having a combined
population of less than 50% of the state's total population; and 3)
widespread--outbreaks of ILI or culture-confirmed influenza in
counties having a combined population of greater than or equal to
50% of the state's total population.
** The epidemic threshold is 1.645 standard deviations above the
seasonal baseline. The expected seasonal baseline is projected
using a robust regression procedure in which a periodic regression
model is applied to observed percentages of deaths from pneumonia
and influenza since 1983.


Notice to Readers
National Notifiable Diseases Reporting -- United States, 1995
     Beginning with the April 28, 1995, MMWR, the following
modifications will be incorporated in Tables I and II, Cases of
Notifiable Diseases, United States, and Figure I, Notifiable
Disease Reports: 1) diseases recently deleted from the nationally
notifiable diseases list by the Council of State and Territorial
Epidemiologists will no longer appear in Tables I and II and Figure
I (i.e., aseptic meningitis, primary and postinfectious
encephalitis, unspecified hepatitis, leptospirosis, and tularemia)
and 2) the column in Table II labeled NA,NB hepatitis will be
relabeled "C/NA,NB" hepatitis.