Delaying BCG Vaccination Until 8 Weeks of Age Results in Robust BCG-Specific T-Cell Responses in HIV-Exposed Infants

Background. BCG vaccination prevents disseminated tuberculosis in children, but it is contraindicated for persons with human immunodeficiency virus (HIV) infection because it can result in severe disease in this population. In tuberculosis-endemic regions, BCG vaccine is administered soon after birt...

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Bibliographic Details
Published in:The Journal of infectious diseases 2015-02, Vol.211 (3), p.338-346
Main Authors: Tchakoute, Christophe Toukam, Hesseling, Anneke C., Kidzeru, Elvis B., Gamieldien, Hoyam, Passmore, Jo-Ann S., Jones, Christine E., Gray, Clive M., Sodora, Donald L., Jaspan, Heather B.
Format: Article
Language:English
Subjects:
BCG Vaccine - immunology
CD4-Positive T-Lymphocytes - immunology
CD8-Positive T-Lymphocytes - immunology
Female
HIV - immunology
HIV Infections - immunology
HIV/AIDS
Human immunodeficiency virus
Humans
Immunization Schedule
Infant
Interferon-gamma - immunology
Lymphocyte Activation - immunology
Major and Brief Reports
Male
Mycobacterium
Tuberculosis - immunology
Tuberculosis - prevention & control
Vaccination - methods
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Summary:Background. BCG vaccination prevents disseminated tuberculosis in children, but it is contraindicated for persons with human immunodeficiency virus (HIV) infection because it can result in severe disease in this population. In tuberculosis-endemic regions, BCG vaccine is administered soon after birth, before in utero and peripartum HIV infection is excluded. We therefore assessed the immunogenicity of BCG vaccine in HIV-exposed infants who received BCG at birth or at 8 weeks of age. Methods. HIV-exposed, uninfected infants were randomly assigned to receive BCG vaccination at birth (the early vaccination arm) or 8 weeks of age (the delayed vaccination arm). BCG-specific proliferative and intracellular cytokine responses were assessed in 28 infants per arm at 6, 8, and 14 weeks of life. Results. There was no difference in BCG-specific T-cell proliferation between the study arms 6 weeks after vaccination. However, at 14 weeks of age, the frequency of interferon γ–expressing CD4⁺ T cells and multifunctional BCG-specific responses in the delayed vaccinated arm were significantly higher than those in the early vaccination arm (P = .021 and P = .011, respectively). Conclusions. The immunogenicity of BCG vaccination in HIV-exposed, uninfected infants is not compromised when delayed until 8 weeks of age and results in robust BCG-specific T-cell responses at 14 weeks of age. These findings support further evaluation of this modified BCG vaccination strategy for HIV-exposed infants. Clinical Trials Registration. NCT02062580.
ISSN:0022-1899
1537-6613
DOI:10.1093/infdis/jiu434