The RIG-I-like Receptor LGP2 Controls CD8+ T Cell Survival and Fitness

Mehul S. Suthar; Hilario J. Ramos; Margaret M. Brassil; Jason Netland; Craig P. Chappell; Gabriele Blahnik; Aimee McMillan; Michael S. Diamond; Edward A. Clark; Michael J. Bevan; Michael Gale

doi:10.1016/j.immuni.2012.07.004

The RIG-I-like Receptor LGP2 Controls CD8⁺ T Cell Survival and Fitness

Mehul S. Suthar
, Hilario J. Ramos
, Margaret M. Brassil
, Jason Netland
, Craig P. Chappell
, Gabriele Blahnik
, Aimee McMillan
, Michael S. Diamond
, Edward A. Clark
, Michael J. Bevan
, Michael Gale

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

110 Scopus citations

Abstract

The RIG-I-like receptors (RLRs) signal innate immune defenses upon RNA virus infection, but their roles in adaptive immunity have not been clearly defined. Here, we showed that the RLR LGP2 was not essential for induction of innate immune defenses, but rather was required for controlling antigen-specific CD8⁺ T cell survival and fitness during peripheral T cell-number expansion in response to virus infection. Adoptive transfer and biochemical studies demonstrated that T cell-receptor signaling induced LGP2 expression wherein LGP2 operated to regulate death-receptor signaling and imparted sensitivity to CD95-mediated cell death. Thus, LGP2 promotes an essential prosurvival signal in response to antigen stimulation to confer CD8⁺ T cell-number expansion and effector functions against divergent RNA viruses, including West Nile virus and lymphocytic choriomeningitis virus.

Original language	English (US)
Pages (from-to)	235-248
Number of pages	14
Journal	Immunity
Volume	37
Issue number	2
DOIs	https://doi.org/10.1016/j.immuni.2012.07.004
State	Published - Aug 24 2012
Externally published	Yes

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

SDG 3 Good Health and Well-being

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10.1016/j.immuni.2012.07.004

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title = "The RIG-I-like Receptor LGP2 Controls CD8+ T Cell Survival and Fitness",

abstract = "The RIG-I-like receptors (RLRs) signal innate immune defenses upon RNA virus infection, but their roles in adaptive immunity have not been clearly defined. Here, we showed that the RLR LGP2 was not essential for induction of innate immune defenses, but rather was required for controlling antigen-specific CD8+ T cell survival and fitness during peripheral T cell-number expansion in response to virus infection. Adoptive transfer and biochemical studies demonstrated that T cell-receptor signaling induced LGP2 expression wherein LGP2 operated to regulate death-receptor signaling and imparted sensitivity to CD95-mediated cell death. Thus, LGP2 promotes an essential prosurvival signal in response to antigen stimulation to confer CD8+ T cell-number expansion and effector functions against divergent RNA viruses, including West Nile virus and lymphocytic choriomeningitis virus.",

author = "Suthar, \{Mehul S.\} and Ramos, \{Hilario J.\} and Brassil, \{Margaret M.\} and Jason Netland and Chappell, \{Craig P.\} and Gabriele Blahnik and Aimee McMillan and Diamond, \{Michael S.\} and Clark, \{Edward A.\} and Bevan, \{Michael J.\} and Michael Gale",

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AU - Suthar, Mehul S.

AU - Ramos, Hilario J.

AU - Brassil, Margaret M.

AU - Netland, Jason

AU - Chappell, Craig P.

AU - Blahnik, Gabriele

AU - McMillan, Aimee

AU - Diamond, Michael S.

AU - Clark, Edward A.

AU - Bevan, Michael J.

AU - Gale, Michael

PY - 2012/8/24

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AB - The RIG-I-like receptors (RLRs) signal innate immune defenses upon RNA virus infection, but their roles in adaptive immunity have not been clearly defined. Here, we showed that the RLR LGP2 was not essential for induction of innate immune defenses, but rather was required for controlling antigen-specific CD8+ T cell survival and fitness during peripheral T cell-number expansion in response to virus infection. Adoptive transfer and biochemical studies demonstrated that T cell-receptor signaling induced LGP2 expression wherein LGP2 operated to regulate death-receptor signaling and imparted sensitivity to CD95-mediated cell death. Thus, LGP2 promotes an essential prosurvival signal in response to antigen stimulation to confer CD8+ T cell-number expansion and effector functions against divergent RNA viruses, including West Nile virus and lymphocytic choriomeningitis virus.

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