Different Cytokine Production and Effector/Memory Dynamics of αβ+ or γδ+ T-Cell Subsets in the Peripheral Blood of Patients with Active Pulmonary Tuberculosis

Author:

Gioia C.,Agrati C.,Goletti D.1,Vincenti D.1,Carrara S.1,Amicosante M.,Casarinp M.2,Giosue S.2,Puglisi G.3,Rossi A.3,Colizzi V.4,Pucillo L. P.,Poccia F.

Affiliation:

1. Transnational Research Unit, Rome, Italy

2. Department of Cardiovascular and Respiratory Sciences, La Sapienza University, Roma, Italy

3. Carlo Forlanini Hospital, Roma, Italy

4. International Center for AIDS & Emerging Infections of the National Institute for Infectious Diseases (I.N.M.I.) “Lazzaro Spallanzani” I.R.C.C.S., Rome, Italy

Abstract

Immunity to M.tuberculosis (MTB) infection consists of interactions between various T-cell subsets that control the infection and prevent further reactivation. We analysed the effector/memory T-cell dynamics and cytokines production in the peripheral blood of patients with pulmonary tuberculosis (TB). We observed that the frequency of CD4+ T-cell effectors was significantly increased during active TB, confirming a major role of this T-cell subset in TB immunity. Pre-terminally differentiated CD8+ T-lymphocytes were increased in the peripheral blood as well. In contrast, we observed a reduced number of effector mycobacteria-reactive γδ+ T-lymphocytes with a specific defects in reacting to mycobacterial nonpeptidic antigens, suggesting that this innate response is rapidly lost during TB infection. Nevertheless, the frequency of γδ+ T-cells effectors in TB patients was higher than the αβ+ T-cell response to peptide from MTB-ESAT-6 protein and quantitatively similar to PPD reactivity. Thus, αβ+and γδ+ T-cell differentiation and function are differently triggered by active TB infection.

Publisher

SAGE Publications

Subject

Pharmacology,Immunology,Immunology and Allergy

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