| Literature DB >> 25631937 |
Nadia Caccamo1, Gabriella Pietra, Lucy C Sullivan, Andrew G Brooks, Teresa Prezzemolo, Marco P La Manna, Diana Di Liberto, Simone A Joosten, Krista E van Meijgaarden, Paola Di Carlo, Lucina Titone, Lorenzo Moretta, Maria C Mingari, Tom H M Ottenhoff, Francesco Dieli.
Abstract
CD8 T cells contribute to protective immunity against Mycobacterium tuberculosis. In humans, M. tuberculosis reactive CD8 T cells typically recognize peptides associated to classical MHC class Ia molecules, but little information is available on CD8 T cells recognizing M. tuberculosis Ags presented by nonclassical MHC class Ib molecules. We show here that CD8 T cells from tuberculosis (TB) patients recognize HLA-E-binding M. tuberculosis peptides in a CD3/TCR αβ mediated and CD8-dependent manner, and represent an additional type of effector cells playing a role in immune response to M. tuberculosis during active infection. HLA-E-restricted recognition of M. tuberculosis peptides is detectable by a significant enhanced ex vivo frequency of tetramer-specific circulating CD8 T cells during active TB. These CD8 T cells produce type 2 cytokines upon antigenic in vitro stimulation, help B cells for Ab production, and mediate limited TRAIL-dependent cytolytic and microbicidal activity toward M. tuberculosis infected target cells. Our results, together with the finding that HLA-E/M. tuberculosis peptide specific CD8 T cells are detected in TB patients with or without HIV coinfection, suggest that this is a new human T-cell population that participates in immune response in TB.Entities:
Keywords: CD8 T lymphocytes; HLA-E; Mycobacterium tuberculosis; TB; Tetramers; Type 2 cytokines
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Year: 2015 PMID: 25631937 DOI: 10.1002/eji.201445193
Source DB: PubMed Journal: Eur J Immunol ISSN: 0014-2980 Impact factor: 6.688