Tc17 CD8 T cells: Functional plasticity and subset diversity

Hung Rong Yen; Timothy J. Harris; Satoshi Wada; Joseph F. Grosso; Derese Getnet; Monica V. Goldberg; Kai Li Liang; Tullia C. Bruno; Kristin J. Pyle; Siaw Li Chan; Robert A. Anders; Cornelia L. Trimble; Adam J. Adler; Tzou Yien Lin; Drew M. Pardoll; Ching Tai Huang; Charles G. Drake

doi:10.4049/jimmunol.0900368

Tc17 CD8 T cells: Functional plasticity and subset diversity

Hung Rong Yen
, Timothy J. Harris
, Satoshi Wada
, Joseph F. Grosso
, Derese Getnet
, Monica V. Goldberg
, Kai Li Liang
, Tullia C. Bruno
, Kristin J. Pyle
, Siaw Li Chan
, Robert A. Anders
, Cornelia L. Trimble
, Adam J. Adler
, Tzou Yien Lin
, Drew M. Pardoll
, Ching Tai Huang
, Charles G. Drake

School of Medicine

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

175 Scopus citations

Abstract

IL-17-secreting CD8 T cells (Tc17) have been described in several settings, but little is known regarding their functional characteristics. While Tc1 cells produced IFN-γ and efficiently killed targets, Tc17 cells lacked lytic function in vitro. Interestingly, the small numbers of IFN-γ-positive or IL-17/IFN-γ-double-positive cells generated under Tc17 conditions also lacked lytic activity and expressed a similar pattern of cell surface proteins to IL-17-producing cells. As is the case for Th17 (CD4) cells, STAT3 is important for Tc17 polarization, both in vitro and in vivo. Adoptive transfer of highly purified, Ag-specific IL-17-secreting Tc17 cells into Ag-bearing hosts resulted in near complete conversion to an IFN-γ-secreting phenotype and substantial pulmonary pathology, demonstrating functional plasticity. Tc17 also accumulated to a greater extent than did Tc1 cells, suggesting that adoptive transfer of CD8 T cells cultured in Tc17 conditions may have therapeutic potential for diseases in which IFN-γ-producing cells are desired.

Original language	English
Pages (from-to)	7161-7168
Number of pages	8
Journal	Journal of Immunology
Volume	183
Issue number	11
DOIs	https://doi.org/10.4049/jimmunol.0900368
State	Published - 01 12 2009

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10.4049/jimmunol.0900368

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Yen, H. R., Harris, T. J., Wada, S., Grosso, J. F., Getnet, D., Goldberg, M. V., Liang, K. L., Bruno, T. C., Pyle, K. J., Chan, S. L., Anders, R. A., Trimble, C. L., Adler, A. J., Lin, T. Y., Pardoll, D. M., Huang, C. T., & Drake, C. G. (2009). Tc17 CD8 T cells: Functional plasticity and subset diversity. Journal of Immunology, 183(11), 7161-7168. https://doi.org/10.4049/jimmunol.0900368

@article{a7e71dacd2124d798ccf7e4186ce11ad,

title = "Tc17 CD8 T cells: Functional plasticity and subset diversity",

abstract = "IL-17-secreting CD8 T cells (Tc17) have been described in several settings, but little is known regarding their functional characteristics. While Tc1 cells produced IFN-γ and efficiently killed targets, Tc17 cells lacked lytic function in vitro. Interestingly, the small numbers of IFN-γ-positive or IL-17/IFN-γ-double-positive cells generated under Tc17 conditions also lacked lytic activity and expressed a similar pattern of cell surface proteins to IL-17-producing cells. As is the case for Th17 (CD4) cells, STAT3 is important for Tc17 polarization, both in vitro and in vivo. Adoptive transfer of highly purified, Ag-specific IL-17-secreting Tc17 cells into Ag-bearing hosts resulted in near complete conversion to an IFN-γ-secreting phenotype and substantial pulmonary pathology, demonstrating functional plasticity. Tc17 also accumulated to a greater extent than did Tc1 cells, suggesting that adoptive transfer of CD8 T cells cultured in Tc17 conditions may have therapeutic potential for diseases in which IFN-γ-producing cells are desired.",

author = "Yen, \{Hung Rong\} and Harris, \{Timothy J.\} and Satoshi Wada and Grosso, \{Joseph F.\} and Derese Getnet and Goldberg, \{Monica V.\} and Liang, \{Kai Li\} and Bruno, \{Tullia C.\} and Pyle, \{Kristin J.\} and Chan, \{Siaw Li\} and Anders, \{Robert A.\} and Trimble, \{Cornelia L.\} and Adler, \{Adam J.\} and Lin, \{Tzou Yien\} and Pardoll, \{Drew M.\} and Huang, \{Ching Tai\} and Drake, \{Charles G.\}",

year = "2009",

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doi = "10.4049/jimmunol.0900368",

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T2 - Functional plasticity and subset diversity

AU - Yen, Hung Rong

AU - Harris, Timothy J.

AU - Wada, Satoshi

AU - Grosso, Joseph F.

AU - Getnet, Derese

AU - Goldberg, Monica V.

AU - Liang, Kai Li

AU - Bruno, Tullia C.

AU - Pyle, Kristin J.

AU - Chan, Siaw Li

AU - Anders, Robert A.

AU - Trimble, Cornelia L.

AU - Adler, Adam J.

AU - Lin, Tzou Yien

AU - Pardoll, Drew M.

AU - Huang, Ching Tai

AU - Drake, Charles G.

PY - 2009/12/1

Y1 - 2009/12/1

N2 - IL-17-secreting CD8 T cells (Tc17) have been described in several settings, but little is known regarding their functional characteristics. While Tc1 cells produced IFN-γ and efficiently killed targets, Tc17 cells lacked lytic function in vitro. Interestingly, the small numbers of IFN-γ-positive or IL-17/IFN-γ-double-positive cells generated under Tc17 conditions also lacked lytic activity and expressed a similar pattern of cell surface proteins to IL-17-producing cells. As is the case for Th17 (CD4) cells, STAT3 is important for Tc17 polarization, both in vitro and in vivo. Adoptive transfer of highly purified, Ag-specific IL-17-secreting Tc17 cells into Ag-bearing hosts resulted in near complete conversion to an IFN-γ-secreting phenotype and substantial pulmonary pathology, demonstrating functional plasticity. Tc17 also accumulated to a greater extent than did Tc1 cells, suggesting that adoptive transfer of CD8 T cells cultured in Tc17 conditions may have therapeutic potential for diseases in which IFN-γ-producing cells are desired.

AB - IL-17-secreting CD8 T cells (Tc17) have been described in several settings, but little is known regarding their functional characteristics. While Tc1 cells produced IFN-γ and efficiently killed targets, Tc17 cells lacked lytic function in vitro. Interestingly, the small numbers of IFN-γ-positive or IL-17/IFN-γ-double-positive cells generated under Tc17 conditions also lacked lytic activity and expressed a similar pattern of cell surface proteins to IL-17-producing cells. As is the case for Th17 (CD4) cells, STAT3 is important for Tc17 polarization, both in vitro and in vivo. Adoptive transfer of highly purified, Ag-specific IL-17-secreting Tc17 cells into Ag-bearing hosts resulted in near complete conversion to an IFN-γ-secreting phenotype and substantial pulmonary pathology, demonstrating functional plasticity. Tc17 also accumulated to a greater extent than did Tc1 cells, suggesting that adoptive transfer of CD8 T cells cultured in Tc17 conditions may have therapeutic potential for diseases in which IFN-γ-producing cells are desired.

UR - https://www.scopus.com/pages/publications/73349101421

U2 - 10.4049/jimmunol.0900368

DO - 10.4049/jimmunol.0900368

M3 - 文章

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AN - SCOPUS:73349101421

SN - 0022-1767

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SP - 7161

EP - 7168

JO - Journal of Immunology

JF - Journal of Immunology

IS - 11

ER -

Tc17 CD8 T cells: Functional plasticity and subset diversity

Abstract

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