Hypoxia induces an immunodominant target of tuberculosis specific T cells absent from common BCG vaccines

M. tuberculosis (MTB) species-specific antigenic determinants of the human T cell response are important for immunodiagnosis and vaccination. As hypoxia is a stimulus in chronic tuberculosis infection, we analyzed transcriptional profiles of MTB subject to 168 hours of hypoxia to test the hypothesis...

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Bibliographic Details
Published in:PLoS pathogens 2010-12, Vol.6 (12), p.e1001237-e1001237
Main Authors: Gideon, Hannah Priyadarshini, Wilkinson, Katalin Andrea, Rustad, Tige R, Oni, Tolu, Guio, Heinner, Kozak, Robert Andrew, Sherman, David R, Meintjes, Graeme, Behr, Marcel A, Vordermeier, Hans Martin, Young, Douglas Brownlee, Wilkinson, Robert John
Format: Article
Language:English
Subjects:
Antigens
Antigens, Bacterial - genetics
Antigens, Bacterial - immunology
BCG
BCG Vaccine - immunology
BCG vaccines
Colleges & universities
Cytokines
Experiments
Gene Expression Profiling
Genetic aspects
Humans
Hypoxia
Hypoxia - immunology
Immunodominant Epitopes - biosynthesis
Immunodominant Epitopes - genetics
Immunologic Memory
Immunology/Antigen Processing and Recognition
Immunology/Immune Response
Immunology/Immunity to Infections
Infectious Diseases/Bacterial Infections
Lymphocytes
Microbiology/Immunity to Infections
Mycobacterium tuberculosis
Physiological aspects
T cells
T-Cell Antigen Receptor Specificity
T-Lymphocytes - immunology
Transcriptional Activation
Tuberculosis
Tuberculosis - immunology
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Summary:M. tuberculosis (MTB) species-specific antigenic determinants of the human T cell response are important for immunodiagnosis and vaccination. As hypoxia is a stimulus in chronic tuberculosis infection, we analyzed transcriptional profiles of MTB subject to 168 hours of hypoxia to test the hypothesis that upregulation by hypoxia might result in gene products being recognized as antigens. We identified upregulation of two region of difference (RD) 11 (Rv2658C and Rv2659c), and one RD2 (Rv1986) absent from commonly used BCG strains. In MTB infected persons, the IL-2 ELISpot response to Rv1986 peptides was several times greater than the corresponding IFN-γ response to the reference immunodominant ESAT-6 or CFP-10 antigens. The IL-2 response was confined to two epitopic regions containing residues 61-80 and 161-180. The biggest population of IL-2 secreting T cells was single cytokine positive central memory T cells. The IL-2 response to live MTB bacilli lacking Rv1986 was significantly lower than the response to wild type or mutant complemented with Rv1986. In addition, the IL-2 response to Rv1986 was significantly lower in HIV-TB co-infected persons than in HIV uninfected persons, and significantly increased during antiretroviral therapy. These findings demonstrate that Rv1986 is an immunodominant target of memory T cells and is therefore of relevance when considering the partial efficacy of currently used BCG vaccines and provide evidence for a clinical trial comparing BCG strains.
ISSN:1553-7374
1553-7366
1553-7374
DOI:10.1371/journal.ppat.1001237