Programmed death-1 receptor suppresses γ-IFN producing NKT cells in human tuberculosis

Amar Singh; Aparajit Ballav Dey; Anant Mohan; Dipendra Kumar Mitra

doi:10.1016/j.tube.2014.01.005

Programmed death-1 receptor suppresses γ-IFN producing NKT cells in human tuberculosis

Amar Singh, Aparajit Ballav Dey, Anant Mohan, Dipendra Kumar Mitra

Surgery

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30 Scopus citations

Abstract

IFN-γ biased Th1 effector immune response is crucial for containment of Mycobacterium tuberculosis infection. Various T cell subsets with regulatory function dictate the generation of Th1 like cells. NKT cells are a specialized T cell subset known to be activated early in immune response and control T cell response via release of immunoregulatory cytokines like IFN-γ, IL-4 and IL-10. M. tuberculosis, with abundance of its cell wall lipids may potently activate NKT cells resulting in cytokine production and PD-1 expression. In this study, among 49 treatment naive active pulmonary tuberculosis patients, we found a higher percentage of PD1⁺ NKT cells correlating with sputum bacillary load. Furthermore, blocking PD-1 increased the number of IFN-γ producing NKT cells by inhibiting their apoptosis. Moreover, peripheral frequency of NKT cells declined with therapy suggesting their role in host T cell response. In this study, we concluded that PD-1 preferentially induces apoptosis of IFN-γ producing NKT cells while sparing NKT cells that produce IL-4. Such a polarized NKT cell function may impose a Th2 bias on the ensuing effector T cell response leading to inefficient clearance of M. tuberculosis. Inhibiting PD-1 may therefore alter the T cell response in favor of the host by rescuing type 1 NKT cells from apoptosis and boosting Th1 effector T cell functions against M. tuberculosis.

Original language	English (US)
Pages (from-to)	197-206
Number of pages	10
Journal	Tuberculosis
Volume	94
Issue number	3
DOIs	https://doi.org/10.1016/j.tube.2014.01.005
State	Published - May 2014

Bibliographical note

Funding Information:
The study was supported by Indian Council of Medical Research (ICMR) and Department of Biotechnology (DBT), Govt. of India, New Delhi, India.

Funding Information:
The study was supported by Indian Council of Medical Research(ICMR) and Department of Biotechnology(DBT), Govt. of India, New Delhi, India.

Funding Information:
The authors thank all the patients and control subjects who voluntarily agreed to participate in this study. This work was supported by Department of Biotechnology & Indian Council of Medical Research Grant, Government of India. We are thankful to Drs. Ambak Rai and Ankit Saxena (Department of TI&I, AIIMS, New Delhi, India) for critical reading of this manuscript. We would like to thank Dr. U. Sengupta, (JALMA, Agra, India) for a kind gift of M. tuberculosis antigen.

Copyright:
Copyright 2014 Elsevier B.V., All rights reserved.

Keywords

Effector T cells
Inteferon-gamma
Natural killer T cell
Programmed death-1
T helper-1

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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title = "Programmed death-1 receptor suppresses γ-IFN producing NKT cells in human tuberculosis",

abstract = "IFN-γ biased Th1 effector immune response is crucial for containment of Mycobacterium tuberculosis infection. Various T cell subsets with regulatory function dictate the generation of Th1 like cells. NKT cells are a specialized T cell subset known to be activated early in immune response and control T cell response via release of immunoregulatory cytokines like IFN-γ, IL-4 and IL-10. M. tuberculosis, with abundance of its cell wall lipids may potently activate NKT cells resulting in cytokine production and PD-1 expression. In this study, among 49 treatment naive active pulmonary tuberculosis patients, we found a higher percentage of PD1+ NKT cells correlating with sputum bacillary load. Furthermore, blocking PD-1 increased the number of IFN-γ producing NKT cells by inhibiting their apoptosis. Moreover, peripheral frequency of NKT cells declined with therapy suggesting their role in host T cell response. In this study, we concluded that PD-1 preferentially induces apoptosis of IFN-γ producing NKT cells while sparing NKT cells that produce IL-4. Such a polarized NKT cell function may impose a Th2 bias on the ensuing effector T cell response leading to inefficient clearance of M. tuberculosis. Inhibiting PD-1 may therefore alter the T cell response in favor of the host by rescuing type 1 NKT cells from apoptosis and boosting Th1 effector T cell functions against M. tuberculosis.",

keywords = "Effector T cells, Inteferon-gamma, Natural killer T cell, Programmed death-1, T helper-1",

author = "Amar Singh and Dey, {Aparajit Ballav} and Anant Mohan and Mitra, {Dipendra Kumar}",

note = "Funding Information: The study was supported by Indian Council of Medical Research (ICMR) and Department of Biotechnology (DBT), Govt. of India, New Delhi, India. Funding Information: The study was supported by Indian Council of Medical Research(ICMR) and Department of Biotechnology(DBT), Govt. of India, New Delhi, India. Funding Information: The authors thank all the patients and control subjects who voluntarily agreed to participate in this study. This work was supported by Department of Biotechnology & Indian Council of Medical Research Grant, Government of India. We are thankful to Drs. Ambak Rai and Ankit Saxena (Department of TI&I, AIIMS, New Delhi, India) for critical reading of this manuscript. We would like to thank Dr. U. Sengupta, (JALMA, Agra, India) for a kind gift of M. tuberculosis antigen. Copyright: Copyright 2014 Elsevier B.V., All rights reserved.",

year = "2014",

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doi = "10.1016/j.tube.2014.01.005",

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AU - Singh, Amar

AU - Dey, Aparajit Ballav

AU - Mohan, Anant

AU - Mitra, Dipendra Kumar

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N2 - IFN-γ biased Th1 effector immune response is crucial for containment of Mycobacterium tuberculosis infection. Various T cell subsets with regulatory function dictate the generation of Th1 like cells. NKT cells are a specialized T cell subset known to be activated early in immune response and control T cell response via release of immunoregulatory cytokines like IFN-γ, IL-4 and IL-10. M. tuberculosis, with abundance of its cell wall lipids may potently activate NKT cells resulting in cytokine production and PD-1 expression. In this study, among 49 treatment naive active pulmonary tuberculosis patients, we found a higher percentage of PD1+ NKT cells correlating with sputum bacillary load. Furthermore, blocking PD-1 increased the number of IFN-γ producing NKT cells by inhibiting their apoptosis. Moreover, peripheral frequency of NKT cells declined with therapy suggesting their role in host T cell response. In this study, we concluded that PD-1 preferentially induces apoptosis of IFN-γ producing NKT cells while sparing NKT cells that produce IL-4. Such a polarized NKT cell function may impose a Th2 bias on the ensuing effector T cell response leading to inefficient clearance of M. tuberculosis. Inhibiting PD-1 may therefore alter the T cell response in favor of the host by rescuing type 1 NKT cells from apoptosis and boosting Th1 effector T cell functions against M. tuberculosis.

AB - IFN-γ biased Th1 effector immune response is crucial for containment of Mycobacterium tuberculosis infection. Various T cell subsets with regulatory function dictate the generation of Th1 like cells. NKT cells are a specialized T cell subset known to be activated early in immune response and control T cell response via release of immunoregulatory cytokines like IFN-γ, IL-4 and IL-10. M. tuberculosis, with abundance of its cell wall lipids may potently activate NKT cells resulting in cytokine production and PD-1 expression. In this study, among 49 treatment naive active pulmonary tuberculosis patients, we found a higher percentage of PD1+ NKT cells correlating with sputum bacillary load. Furthermore, blocking PD-1 increased the number of IFN-γ producing NKT cells by inhibiting their apoptosis. Moreover, peripheral frequency of NKT cells declined with therapy suggesting their role in host T cell response. In this study, we concluded that PD-1 preferentially induces apoptosis of IFN-γ producing NKT cells while sparing NKT cells that produce IL-4. Such a polarized NKT cell function may impose a Th2 bias on the ensuing effector T cell response leading to inefficient clearance of M. tuberculosis. Inhibiting PD-1 may therefore alter the T cell response in favor of the host by rescuing type 1 NKT cells from apoptosis and boosting Th1 effector T cell functions against M. tuberculosis.

KW - Effector T cells

KW - Inteferon-gamma

KW - Natural killer T cell

KW - Programmed death-1

KW - T helper-1

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Programmed death-1 receptor suppresses γ-IFN producing NKT cells in human tuberculosis

Abstract

Bibliographical note

Keywords

UN SDGs

Access

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