CTLA-4 suppresses the pathogenicity of self antigen-specific T cells by cell-intrinsic and cell-extrinsic mechanisms

Wataru Ise; Masako Kohyama; Katherine M. Nutsch; Hyang Mi Lee; Anish Suri; Emil R. Unanue; Theresa L. Murphy; Kenneth M. Murphy

doi:10.1038/ni.1835

CTLA-4 suppresses the pathogenicity of self antigen-specific T cells by cell-intrinsic and cell-extrinsic mechanisms

Wataru Ise
, Masako Kohyama
, Katherine M. Nutsch
, Hyang Mi Lee
, Anish Suri
, Emil R. Unanue
, Theresa L. Murphy
, Kenneth M. Murphy

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

154 Scopus citations

Abstract

The inhibitory immunoregulatory receptor CTLA-4 is critical in maintaining self-tolerance, but the mechanisms of its actions have remained controversial. Here we examined the antigen specificity of tissue-infiltrating CD4⁺ T cells in Ctla4^-/- mice. After adoptive transfer, T cells isolated from tissues of Ctla4^/ mice showed T cell antigen receptor (TCR)-dependent accumulation in the tissues from which they were derived, which suggested reactivity to tissue-specific antigens. We identified the pancreas-specific enzyme PDIA2 as an autoantigen in Ctla4^/ mice. CTLA-4 expressed either on PDIA2-specific effector cells or on regulatory T cells was sufficient to control tissue destruction mediated by PDIA2-specific T cells. Our results demonstrate that both cell-intrinsic and non-cell-autonomous actions of CTLA-4 operate to maintain T cell tolerance to a self antigen.

Original language	English
Pages (from-to)	129-135
Number of pages	7
Journal	Nature immunology
Volume	11
Issue number	2
DOIs	https://doi.org/10.1038/ni.1835
State	Published - Feb 2010

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title = "CTLA-4 suppresses the pathogenicity of self antigen-specific T cells by cell-intrinsic and cell-extrinsic mechanisms",

abstract = "The inhibitory immunoregulatory receptor CTLA-4 is critical in maintaining self-tolerance, but the mechanisms of its actions have remained controversial. Here we examined the antigen specificity of tissue-infiltrating CD4+ T cells in Ctla4-/- mice. After adoptive transfer, T cells isolated from tissues of Ctla4/ mice showed T cell antigen receptor (TCR)-dependent accumulation in the tissues from which they were derived, which suggested reactivity to tissue-specific antigens. We identified the pancreas-specific enzyme PDIA2 as an autoantigen in Ctla4/ mice. CTLA-4 expressed either on PDIA2-specific effector cells or on regulatory T cells was sufficient to control tissue destruction mediated by PDIA2-specific T cells. Our results demonstrate that both cell-intrinsic and non-cell-autonomous actions of CTLA-4 operate to maintain T cell tolerance to a self antigen.",

author = "Wataru Ise and Masako Kohyama and Nutsch, \{Katherine M.\} and Lee, \{Hyang Mi\} and Anish Suri and Unanue, \{Emil R.\} and Murphy, \{Theresa L.\} and Murphy, \{Kenneth M.\}",

year = "2010",

month = feb,

doi = "10.1038/ni.1835",

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pages = "129--135",

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T1 - CTLA-4 suppresses the pathogenicity of self antigen-specific T cells by cell-intrinsic and cell-extrinsic mechanisms

AU - Ise, Wataru

AU - Kohyama, Masako

AU - Nutsch, Katherine M.

AU - Lee, Hyang Mi

AU - Suri, Anish

AU - Unanue, Emil R.

AU - Murphy, Theresa L.

AU - Murphy, Kenneth M.

PY - 2010/2

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AB - The inhibitory immunoregulatory receptor CTLA-4 is critical in maintaining self-tolerance, but the mechanisms of its actions have remained controversial. Here we examined the antigen specificity of tissue-infiltrating CD4+ T cells in Ctla4-/- mice. After adoptive transfer, T cells isolated from tissues of Ctla4/ mice showed T cell antigen receptor (TCR)-dependent accumulation in the tissues from which they were derived, which suggested reactivity to tissue-specific antigens. We identified the pancreas-specific enzyme PDIA2 as an autoantigen in Ctla4/ mice. CTLA-4 expressed either on PDIA2-specific effector cells or on regulatory T cells was sufficient to control tissue destruction mediated by PDIA2-specific T cells. Our results demonstrate that both cell-intrinsic and non-cell-autonomous actions of CTLA-4 operate to maintain T cell tolerance to a self antigen.

UR - https://www.scopus.com/pages/publications/75649095238

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DO - 10.1038/ni.1835

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SN - 1529-2908

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JO - Nature immunology

JF - Nature immunology

IS - 2

ER -

CTLA-4 suppresses the pathogenicity of self antigen-specific T cells by cell-intrinsic and cell-extrinsic mechanisms

Abstract

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