H1N1 Influenza Clinical Trial
Official title:
The Safety of GSK Biological's H1N1 Pandemic Vaccine in Manitoba, Canada
Many people worldwide received the monovalent adjuvanted H1N1 vaccine. However, very little is known about the safety of the vaccine, particularly beyond the first few weeks after vaccination. This study will combine data from a well-established immunization registry in Manitoba with data from hospitalization and physician records, to examine the safety of the vaccine in the six month period post-vaccination. Studies on vaccine safety are important as the public's perception of the safety of a vaccine has a major role in its uptake.
The objective of this study is to examine the safety of the H1N1 vaccine administered in
Manitoba during the second wave of the pandemic (Oct 2009-Mar 2010) by describing the age
sex specific and age standardized incidence rates of certain vaccination adverse events in
the vaccinated populations during the first 6 months of follow-up and to compare the rates
with those in the non-vaccinated population and the general Manitoba population.
Study design The proposed study will be a retrospective analysis of population based cohorts
of subjects whose vaccination status and health events before and after H1N1 vaccination are
recorded in various Manitoba databases. All H1N1 vaccinated and unvaccinated individuals are
eligible to be included in the study population. There will be no exclusion criteria. The
list of specific adverse events of special interest (AESIs) includes: anaphylaxis, Bell's
palsy, convulsions, demyelination, encephalitis, Guillain-Barré syndrome, neuritis,
vasculitis and various pregnancy outcomes.
Vaccinated individuals will be identified using the Manitoba Immunization Monitoring System
(MIMS). Unvaccinated individuals will be identified using the Population Registry. AESIs and
other clinically relevant information will be determined using hospital, physician claim and
DPIN databases.
The primary statistical analysis will be a comparison of the overall and age specific rates
of deaths and AESIs in the vaccinated cohort relative to the non-vaccinated cohort. The two
cohorts will be matched on age (month and year of birth), sex and postal code of residence.
The analyses will be stratified by specific subgroups: (e.g. pregnant women, persons who are
immune suppressed or with autoimmune disorders).
The observed number of events will be determined from the date of first vaccination for each
subject and the matched control until the first occurrence of a specific event. Information
on events for each person will be derived from the medical claims and hospitalization
databases. The person years at risk will be calculated from the date of first vaccination
until the first occurrence of the specific event, emigration from Manitoba, or until 6
months after vaccination. Incidence rate ratios and 95% confidence intervals will be
calculated by comparing the standardized incidence rates in the vaccinated cohort with those
in the matched non vaccinated cohort.
In addition, the observed number of deaths and AESIs in the total vaccinated population and
in specific subgroups (as above) will be compared to the expected numbers based on the age
sex specific rates in the general Manitoba population. Similar to the matched cohort
component, the observed number of events will be determined for the vaccinated individuals
from the date of first vaccination until the first occurrence of a specific event, and the
person years at risk will be calculated from the date of first vaccination until the first
occurrence of the specific event, emigration from Manitoba, or until 6 months after
vaccination. The background rate of targeted events will be calculated utilizing information
from the mortality, physician claims and hospitalization databases for the total population
in Manitoba for the period 2004 2008. Since the risk of some of the events is low,
calculating the age sex specific rates based on five years of data will increase the
stability of the rates. The expected number of events will be calculated by multiplying the
person years at risk by the age sex specific background rate of each targeted event.
Standardized incidence ratios (SIRs) or mortality ratios (SMRs) will be calculated as the
number of observed events over the number of expected events, with 95% confidence intervals.
To assess the absolute burden of an eventual excess in observed number of events the
absolute difference between the observed and expected number of events for certain AESIs
will also be calculated.
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Observational Model: Cohort, Time Perspective: Retrospective
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