Inhibitory IL-10-producing CD4 + T cells are T-bet-dependent and facilitate cytomegalovirus persistence via coexpression of arginase-1

Mathew Clement; Kristin Ladell; Kelly L Miners; Morgan Marsden; Lucy Chapman; Anna Cardus Figueras; Jake Scott; Robert Andrews; Simon Clare; Valeriia V Kriukova; Ksenia R Lupyr; Olga V Britanova; David R Withers; Simon A Jones; Dmitriy M Chudakov; David A Price; Ian R Humphreys; Stipan Jonjic; Satyajit Rath

doi:10.7554/elife.79165

Inhibitory IL-10-producing CD4 + T cells are T-bet-dependent and facilitate cytomegalovirus persistence via coexpression of arginase-1

Mathew Clement^*, Kristin Ladell, Kelly L Miners, Morgan Marsden, Lucy Chapman, Anna Cardus Figueras, Jake Scott, Robert Andrews, Simon Clare, Valeriia V Kriukova, Ksenia R Lupyr, Olga V Britanova, David R Withers, Simon A Jones, Dmitriy M Chudakov, David A Price, Ian R Humphreys, Stipan Jonjic (Editor), Satyajit Rath

^*Corresponding author for this work

Immunology and Immunotherapy

Research output: Contribution to journal › Article › peer-review

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Abstract

Inhibitory CD4+ T cells have been linked with suboptimal immune responses against cancer and pathogen chronicity. However, the mechanisms that underpin the development of these regulatory cells, especially in the context of ongoing antigen exposure, have remained obscure. To address this knowledge gap, we undertook a comprehensive functional, phenotypic, and transcriptomic analysis of interleukin (IL)-10-producing CD4+ T cells induced by chronic infection with murine cytomegalovirus (MCMV). We identified these cells as clonally expanded and highly differentiated TH1-like cells that developed in a T-bet-dependent manner and coexpressed arginase-1 (Arg1), which promotes the catalytic breakdown of L-arginine. Mice lacking Arg1-expressing CD4+ T cells exhibited more robust antiviral immunity and were better able to control MCMV. Conditional deletion of T-bet in the CD4+ lineage suppressed the development of these inhibitory cells and also enhanced immune control of MCMV. Collectively, these data elucidated the ontogeny of IL-10-producing CD4+ T cells and revealed a previously unappreciated mechanism of immune regulation, whereby viral persistence was facilitated by the site-specific delivery of Arg1.

Original language	English
Article number	e79165
Journal	eLife
Volume	12
DOIs	https://doi.org/10.7554/elife.79165
Publication status	Published - 13 Jul 2023

Keywords

arginase-1
IL-10
T-bet
cytomegalovirus
Mice
Viruses
CD4+ T cells

UN SDGs

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

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10.7554/elife.79165Licence: Creative Commons: Attribution (CC BY)

ClementM2023InhibitoryFinal published version, 21.2 MBLicence: Creative Commons: Attribution (CC BY)

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Clement, M., Ladell, K., Miners, K. L., Marsden, M., Chapman, L., Cardus Figueras, A., Scott, J., Andrews, R., Clare, S., Kriukova, V. V., Lupyr, K. R., Britanova, O. V., Withers, D. R., Jones, S. A., Chudakov, D. M., Price, D. A., Humphreys, I. R., Jonjic, S. (Ed.), & Rath, S. (2023). Inhibitory IL-10-producing CD4 + T cells are T-bet-dependent and facilitate cytomegalovirus persistence via coexpression of arginase-1. eLife, 12, Article e79165. https://doi.org/10.7554/elife.79165

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title = "Inhibitory IL-10-producing CD4 + T cells are T-bet-dependent and facilitate cytomegalovirus persistence via coexpression of arginase-1",

abstract = "Inhibitory CD4+ T cells have been linked with suboptimal immune responses against cancer and pathogen chronicity. However, the mechanisms that underpin the development of these regulatory cells, especially in the context of ongoing antigen exposure, have remained obscure. To address this knowledge gap, we undertook a comprehensive functional, phenotypic, and transcriptomic analysis of interleukin (IL)-10-producing CD4+ T cells induced by chronic infection with murine cytomegalovirus (MCMV). We identified these cells as clonally expanded and highly differentiated TH1-like cells that developed in a T-bet-dependent manner and coexpressed arginase-1 (Arg1), which promotes the catalytic breakdown of L-arginine. Mice lacking Arg1-expressing CD4+ T cells exhibited more robust antiviral immunity and were better able to control MCMV. Conditional deletion of T-bet in the CD4+ lineage suppressed the development of these inhibitory cells and also enhanced immune control of MCMV. Collectively, these data elucidated the ontogeny of IL-10-producing CD4+ T cells and revealed a previously unappreciated mechanism of immune regulation, whereby viral persistence was facilitated by the site-specific delivery of Arg1.",

keywords = "arginase-1, IL-10, T-bet, cytomegalovirus, Mice, Viruses, CD4+ T cells",

author = "Mathew Clement and Kristin Ladell and Miners, {Kelly L} and Morgan Marsden and Lucy Chapman and {Cardus Figueras}, Anna and Jake Scott and Robert Andrews and Simon Clare and Kriukova, {Valeriia V} and Lupyr, {Ksenia R} and Britanova, {Olga V} and Withers, {David R} and Jones, {Simon A} and Chudakov, {Dmitriy M} and Price, {David A} and Humphreys, {Ian R} and Stipan Jonjic and Satyajit Rath",

year = "2023",

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Clement, M, Ladell, K, Miners, KL, Marsden, M, Chapman, L, Cardus Figueras, A, Scott, J, Andrews, R, Clare, S, Kriukova, VV, Lupyr, KR, Britanova, OV, Withers, DR, Jones, SA, Chudakov, DM, Price, DA, Humphreys, IR, Jonjic, S (ed.) & Rath, S 2023, 'Inhibitory IL-10-producing CD4 + T cells are T-bet-dependent and facilitate cytomegalovirus persistence via coexpression of arginase-1', eLife, vol. 12, e79165. https://doi.org/10.7554/elife.79165

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AU - Clement, Mathew

AU - Ladell, Kristin

AU - Miners, Kelly L

AU - Marsden, Morgan

AU - Chapman, Lucy

AU - Cardus Figueras, Anna

AU - Scott, Jake

AU - Andrews, Robert

AU - Clare, Simon

AU - Kriukova, Valeriia V

AU - Lupyr, Ksenia R

AU - Britanova, Olga V

AU - Withers, David R

AU - Jones, Simon A

AU - Chudakov, Dmitriy M

AU - Price, David A

AU - Humphreys, Ian R

AU - Rath, Satyajit

A2 - Jonjic, Stipan

PY - 2023/7/13

Y1 - 2023/7/13

N2 - Inhibitory CD4+ T cells have been linked with suboptimal immune responses against cancer and pathogen chronicity. However, the mechanisms that underpin the development of these regulatory cells, especially in the context of ongoing antigen exposure, have remained obscure. To address this knowledge gap, we undertook a comprehensive functional, phenotypic, and transcriptomic analysis of interleukin (IL)-10-producing CD4+ T cells induced by chronic infection with murine cytomegalovirus (MCMV). We identified these cells as clonally expanded and highly differentiated TH1-like cells that developed in a T-bet-dependent manner and coexpressed arginase-1 (Arg1), which promotes the catalytic breakdown of L-arginine. Mice lacking Arg1-expressing CD4+ T cells exhibited more robust antiviral immunity and were better able to control MCMV. Conditional deletion of T-bet in the CD4+ lineage suppressed the development of these inhibitory cells and also enhanced immune control of MCMV. Collectively, these data elucidated the ontogeny of IL-10-producing CD4+ T cells and revealed a previously unappreciated mechanism of immune regulation, whereby viral persistence was facilitated by the site-specific delivery of Arg1.

AB - Inhibitory CD4+ T cells have been linked with suboptimal immune responses against cancer and pathogen chronicity. However, the mechanisms that underpin the development of these regulatory cells, especially in the context of ongoing antigen exposure, have remained obscure. To address this knowledge gap, we undertook a comprehensive functional, phenotypic, and transcriptomic analysis of interleukin (IL)-10-producing CD4+ T cells induced by chronic infection with murine cytomegalovirus (MCMV). We identified these cells as clonally expanded and highly differentiated TH1-like cells that developed in a T-bet-dependent manner and coexpressed arginase-1 (Arg1), which promotes the catalytic breakdown of L-arginine. Mice lacking Arg1-expressing CD4+ T cells exhibited more robust antiviral immunity and were better able to control MCMV. Conditional deletion of T-bet in the CD4+ lineage suppressed the development of these inhibitory cells and also enhanced immune control of MCMV. Collectively, these data elucidated the ontogeny of IL-10-producing CD4+ T cells and revealed a previously unappreciated mechanism of immune regulation, whereby viral persistence was facilitated by the site-specific delivery of Arg1.

KW - arginase-1

KW - IL-10

KW - T-bet

KW - cytomegalovirus

KW - Mice

KW - Viruses

KW - CD4+ T cells

U2 - 10.7554/elife.79165

DO - 10.7554/elife.79165

M3 - Article

SN - 2050-084X

VL - 12

JO - eLife

JF - eLife

M1 - e79165

ER -

Inhibitory IL-10-producing CD4 + T cells are T-bet-dependent and facilitate cytomegalovirus persistence via coexpression of arginase-1

Abstract

Keywords

UN SDGs

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