HIV Clinical Trial
Official title:
Immune Response After Vaccination Against Pandemic A/H1N1 Influenza in the Immunocompromised Host. Vaccination Response in ImmunoCompromised Host
As recommended by the Dutch Health Council, certain risk groups and health care workers in
The Netherlands were vaccinated to prevent morbidity due to pandemic influenza A/H1N1.
Adults were vaccinated twice with the monovalent influenza A/California/2009(H1N1)
MF59-adjuvanted surface-antigen vaccine Focetria® (Novartis). The vaccination campaign was
executed by general practitioners.
The aim of the study is to verify whether HIV-infected individuals generate an adequate
immune response after the first and after the second vaccination.
AIM OF THIS STUDY:
Primary objective: Do HIV-infected individuals mount a protective humoral response following
vaccination for pandemic influenza A/H1N1 with the monovalent influenza
A/California/2009(H1N1) MF59-adjuvanted surface-antigen vaccine Focetria® (Novartis).
Secondary objective: 1) To evaluate the strength of the immune response in HIV-infected
individuals compared to healthy volunteers. 2) To evaluate whether a second dose,
administered at least 21 days after the first increases the proportion of HIV-infected
individuals that have a titer above the threshold associated with protection. 3) To assess
whether vaccination is associated with an increases in HIV-replication. 4) To assess whether
very early antibody responses occur, which may may indicate immunological memory, for
example due to cross reactivity from past influenza infection or vaccination.
STUDY DESIGN:
This is not an interventional study. In this single-centre observational study we will
monitor the immune response in a cohort of people who are to be vaccinated during the
national vaccination campaign.
Population: The population base for this study consists of HIV-infected adult outpatients at
our hospital and of healthy hospital employees. All Dutch and English speaking HIV-infected
LUMC outpatients above 18 years of age, on a stable antiretroviral regimen or not yet in
need of treatment, are sent a letter inviting them to take part. Healthy hospital employees
are invited to take part with a letter, which is handed out upon vaccination. Inclusion is
possible until three days after the first vaccination. Exclusion criteria are: use of
systemic immunosuppressive medication, an ongoing infection, recent flu-like symptoms and
pregnancy. The following characteristics are documented at baseline: age, gender,
co-morbidity, medication, year of prior influenza vaccinations and year of diagnosis of HIV
infection. All participants are requested to fill out standardized diary assessing flu-like
symptoms and use of new medication during the 60 day follow-up.
Laboratory analysis: Lymphocyte counts are determined at baseline, prior to vaccination. A
serum sample is taken prior to the first vaccination (day -30 to day 0), prior to the second
vaccination (day 17-20) and after the second vaccination (day 60). Viral load is determined
at baseline (day -30 to day 0) and after the second vaccination (day 5-7) in a subgroup of
10 persons with undetectable viral load at the preceding outpatient visit. Antibody
responses are detected in duplicate for each sample by means of hemagglutination-inhibition
(HI) assays according to standard methods at the Erasmus Medical Center in Rotterdam.
Statistical analysis: No formal sample-size calculation was performed. We intend to include
a maximum of 100 subjects with HIV and 50 healthy hospital employees. The crude outcome
estimates will be adjusted for variables that may influence the outcome (age, CD4 lymphocyte
count, use of HAART, viral load).
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