Efficacy Safety Study of Flu Vaccine in Immunodepression Patients

Assistance Publique - Hôpitaux de Paris228 enrolled

Overview

The primary purpose of the study is to compare the efficacy and safety of influenza vaccine in patients with inflammatory bowel disease (IBD) receiving immunosuppressive therapy with patients not receiving immunosuppressants . The main objective of the study is to evaluate the humoral immunogenicity of influenza vaccination in patients with IBD

Annual vaccination against influenza is recommended for those at high risk of complications, particularly among patients with immunodeficiency including those resulting from immunosuppressive treatments administered for a chronic inflammatory bowel disease (IBD). However, published data showing that influenza vaccination coverage is low in this population (\<30%) due to lack of data on the effectiveness of vaccination in these patients and the theoretical risk of negative impact on the evolution of IBD. To improve influenza vaccination coverage of the population treated by immunosuppressants for a chronic IBD, it is essential to have data on the effectiveness of vaccination in these populations. The research aims to evaluate the immunogenicity of influenza vaccination in patients followed for a chronic IBD. Factors in choice of study population were as follows: 1. IBD is a common disease. Among the inflammatory diseases treated with immunosuppressants and reaching patients under 65 years, IBD are among the most frequent. They result from an abnormal immune response to gut flora and their management often requires the prescription of immunosuppressive drugs (azathioprine, methotrexate, in particular) and more recently TNF-blockers; 2. the existence of vaccine recommendations published recently for specific patients on immunosuppressive therapy at greatest risk of complications related to influenza; 3. the fact that vaccinations have not been implicated in the pathogenesis of the disease; 4. data showing that vaccination recommendations are poorly followed in this population. A recently published work found vaccination coverage against influenza of only 28% in a cohort of 169 patients treated for IBD; The methodology chosen is a phase III, prospective, open, vaccine trial. The primary endpoint is the humoral immunogenicity induced by the vaccine. The study is scheduled on 2 successive years to assess the value of annual vaccination repeated in this population treated with immunosuppressants. There is a benefit for patients to participate in this study because they are all vaccinated against influenza and will benefit from a clinical and laboratory monitoring in this study. Moreover, these patients are taken to be vaccinated in the event of a pandemic influenza

Study Type

INTERVENTIONAL

Allocation

NON_RANDOMIZED

Purpose

TREATMENT

Masking

NONE

Enrollment

228

Conditions

Inflammatory Bowel Disease (IBD)

Interventions

VaccineDRUG

MUTAGRIP (2009-2010 winter) VAXIGRIP (2010-2011 winter)

Vaccine anti-H1N1BIOLOGICAL

patients who received the vaccine anti-H1N1

Eligibility

Sex: ALLMin age: 18 YearsMax age: 64 Years

Medical Language ↔ Plain English

Inclusion criteria : * informed consent signed * Age between 18 to 64 * Patient suffering from chronic inflammatory bowel disease (Crohn's disease, ulcerative colitis, or indeterminate colitis) * For patients receiving at least one immunosuppressive or anti-TNF therapy: treatment introduced for at least 3 months * Patient willing to participate in the study throughout its duration and acceptance procedures related to the study (blood samples, self questionnaires, nasal swab and telephone follow-up) Exclusion criteria : * Patient treated by corticosteroid alone without immunosuppressive or anti-TNF * For women, being pregnant or positive pregnancy test * Known allergy to any component of the study vaccine or a history of hypersensitivity reaction to influenza vaccination * Fever (at least 37.5°C measured orally) or acute infection in the week prior to vaccination * Received influenza vaccination in the 6 months preceding enrollment * Known history of progressive neuropathy or Guillain-Barre * Known infection with HIV and/or HBV (Ag-HBs positive) and/or HCV * Other causes of severe immune deficiency * Cellular therapy, immunoglobulin infusions, of blood products or monoclonal antibodies (except anti-TNF) in the 3 months prior to vaccination * Patient deprived of freedom by an administrative or court order * Patient non affiliated to a health social security system

Locations (1)

CIC Vaccinologie Hopital Cochin

Paris, France

Outcomes

Primary Outcomes

Seroconversion rate

Seroconversion rate in the overall population, defined as the geometric mean titers ratio post / pre-vaccination for each of the three vaccine strains

Time frame: 3-4 weeks after vaccination

Secondary Outcomes

Seroconversion factor

The seroconversion factor obtained for each of the three vaccine strains will be compared between each of the three groups (patients not receiving treatment, patients receiving immunosuppressants and patients receiving immunosuppressants including TNF) defined as the geometric mean titers ratio post / pre-vaccination for each of the three vaccine strains

Time frame: 3 weeks and 6 months after vaccination

Seroprotection rate against the three vaccine strains

The seroprotection rate (defined as the proportion of subjects attaining an anti-hemagglutinin titer ≥1:40) obtained 3-4 weeks after flu vaccination, against the three vaccine strains

Time frame: 3 or 4 weeks after of vaccination

Seroprotection rate in the general population

The seroprotection rate in the general population and according to the three groups of patients

Time frame: 3 weeks and 6 months after vaccination

Seroconversion rate, geometric mean titers ratio before and after vaccination by haemagglutination inhibition assay

The seroconversion rate, geometric mean titers ratio before and after vaccination by haemagglutination inhibition (HI) assay before and after vaccination

Time frame: after 3 weeks of vaccination

Comparison of seroprotection rates for each of the three vaccine strains obtained in each of three groups

Comparison of seroprotection rates for each of the three vaccine strains obtained in each of three groups (patients not receiving treatment, patients receiving immunosuppressants and patients, receiving immunosuppressants including TNF)

Data from ClinicalTrials.gov

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