T cells maintain an exhausted phenotype after antigen withdrawal and population reexpansion

Daniel T. Utzschneider; Amandine Legat; Silvia A. Fuertes Marraco; Lucie Carrié; Immanuel Luescher; Daniel E. Speiser; Dietmar Zehn

doi:10.1038/ni.2606

T cells maintain an exhausted phenotype after antigen withdrawal and population reexpansion

Daniel T. Utzschneider, Amandine Legat, Silvia A. Fuertes Marraco, Lucie Carrié, Immanuel Luescher, Daniel E. Speiser, Dietmar Zehn

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

224 Scopus citations

Abstract

During chronic infection, pathogen-specific CD8⁺ T cells upregulate expression of molecules such as the inhibitory surface receptor PD-1, have diminished cytokine production and are thought to undergo terminal differentiation into exhausted cells. Here we found that T cells with memory-like properties were generated during chronic infection. After transfer into naive mice, these cells robustly proliferated and controlled a viral infection. The reexpanded T cell populations continued to have the exhausted phenotype they acquired during the chronic infection. Thus, the cells underwent a form of differentiation that was stably transmitted to daughter cells. We therefore propose that during persistent infection, effector T cells stably differentiate into a state that is optimized to limit viral replication without causing overwhelming immunological pathology.

Original language	English
Pages (from-to)	603-610
Number of pages	8
Journal	Nature Immunology
Volume	14
Issue number	6
DOIs	https://doi.org/10.1038/ni.2606
State	Published - Jun 2013
Externally published	Yes

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@article{02569181bee34221a0b40fb5f491cee0,

title = "T cells maintain an exhausted phenotype after antigen withdrawal and population reexpansion",

abstract = "During chronic infection, pathogen-specific CD8+ T cells upregulate expression of molecules such as the inhibitory surface receptor PD-1, have diminished cytokine production and are thought to undergo terminal differentiation into exhausted cells. Here we found that T cells with memory-like properties were generated during chronic infection. After transfer into naive mice, these cells robustly proliferated and controlled a viral infection. The reexpanded T cell populations continued to have the exhausted phenotype they acquired during the chronic infection. Thus, the cells underwent a form of differentiation that was stably transmitted to daughter cells. We therefore propose that during persistent infection, effector T cells stably differentiate into a state that is optimized to limit viral replication without causing overwhelming immunological pathology.",

author = "Utzschneider, {Daniel T.} and Amandine Legat and {Fuertes Marraco}, {Silvia A.} and Lucie Carri{\'e} and Immanuel Luescher and Speiser, {Daniel E.} and Dietmar Zehn",

note = "Funding Information: We thank S. Enouz, S. Oberle and M. Prlic for discussions and critical review of the manuscript; A. Oxenius (Institute of Microbiology, Swiss Federal Institute of Technology Z{\"u}rich) for P14αβ mice; P. Fink (University of Washington, Seattle) for Vβ5 mice; and A. Wilson and H.R. MacDonald (Ludwig Center for Cancer Research, University of Lausanne) for antibodies specific to CD45.2 (clone 104) and CD45.1 (clone A20). Supported by the Swiss Vaccine Research Institute (D.Z.) and the Swiss National Science Foundation (CRSII3_141879 to D.Z. and D.E.S.).",

year = "2013",

month = jun,

doi = "10.1038/ni.2606",

language = "English",

volume = "14",

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journal = "Nature Immunology",

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T1 - T cells maintain an exhausted phenotype after antigen withdrawal and population reexpansion

AU - Utzschneider, Daniel T.

AU - Legat, Amandine

AU - Fuertes Marraco, Silvia A.

AU - Carrié, Lucie

AU - Luescher, Immanuel

AU - Speiser, Daniel E.

AU - Zehn, Dietmar

N1 - Funding Information: We thank S. Enouz, S. Oberle and M. Prlic for discussions and critical review of the manuscript; A. Oxenius (Institute of Microbiology, Swiss Federal Institute of Technology Zürich) for P14αβ mice; P. Fink (University of Washington, Seattle) for Vβ5 mice; and A. Wilson and H.R. MacDonald (Ludwig Center for Cancer Research, University of Lausanne) for antibodies specific to CD45.2 (clone 104) and CD45.1 (clone A20). Supported by the Swiss Vaccine Research Institute (D.Z.) and the Swiss National Science Foundation (CRSII3_141879 to D.Z. and D.E.S.).

PY - 2013/6

Y1 - 2013/6

N2 - During chronic infection, pathogen-specific CD8+ T cells upregulate expression of molecules such as the inhibitory surface receptor PD-1, have diminished cytokine production and are thought to undergo terminal differentiation into exhausted cells. Here we found that T cells with memory-like properties were generated during chronic infection. After transfer into naive mice, these cells robustly proliferated and controlled a viral infection. The reexpanded T cell populations continued to have the exhausted phenotype they acquired during the chronic infection. Thus, the cells underwent a form of differentiation that was stably transmitted to daughter cells. We therefore propose that during persistent infection, effector T cells stably differentiate into a state that is optimized to limit viral replication without causing overwhelming immunological pathology.

AB - During chronic infection, pathogen-specific CD8+ T cells upregulate expression of molecules such as the inhibitory surface receptor PD-1, have diminished cytokine production and are thought to undergo terminal differentiation into exhausted cells. Here we found that T cells with memory-like properties were generated during chronic infection. After transfer into naive mice, these cells robustly proliferated and controlled a viral infection. The reexpanded T cell populations continued to have the exhausted phenotype they acquired during the chronic infection. Thus, the cells underwent a form of differentiation that was stably transmitted to daughter cells. We therefore propose that during persistent infection, effector T cells stably differentiate into a state that is optimized to limit viral replication without causing overwhelming immunological pathology.

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JO - Nature Immunology

JF - Nature Immunology

IS - 6

ER -

T cells maintain an exhausted phenotype after antigen withdrawal and population reexpansion

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