Cutting edge: Compartmentalization of Th1-like noninvariant CD1d-reactive T cells in hepatitis C virus-infected liver

Mark A. Exley; Qi He; Olivia Cheng; Ruo Jie Wang; Catherine P. Cheney; Steven P. Balk; Margaret J. Koziel

Cutting edge: Compartmentalization of Th1-like noninvariant CD1d-reactive T cells in hepatitis C virus-infected liver

Mark A. Exley, Qi He, Olivia Cheng, Ruo Jie Wang, Catherine P. Cheney, Steven P. Balk, Margaret J. Koziel

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

Abstract

Murine intrahepatic lymphocytes (IHL) are dominated by invariant TCR α-chain expressing CD1d-reactive NKT cells, which can cause model hepatitis. Invariant NKT (CD56+/-CD161+) and recently identified noninvariant CD1d-reactive T cells rapidly produce large amounts of IL-4 and/or IFN-γ and can regulate Th1/Th2 responses. Haman liver contains large numbers of CD56+ NKT cells but few invariant NKT. Compared with matched peripheral blood T cell lines, primary IHL lines from patients with chronic hepatitis C had high levels of CD161 and CD1d reactivity, but the invariant TCR was rare. CD1d-reactive IHL were strikingly Th1 biased. IHL also demonstrated CD1d-specific cytotoxic activity. Hepatocytes and other liver cells express CD1d. These results identify a novel population of human T cells that could contribute to destructive as well as protective immune responses in the liver. CD1d-reactive T cells may have distinct roles in different tissues.

Original language	English
Pages (from-to)	1519-1523
Number of pages	4
Journal	Journal of Immunology
Volume	168
Issue number	4
Publication status	Published - 15 Feb 2002

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title = "Cutting edge: Compartmentalization of Th1-like noninvariant CD1d-reactive T cells in hepatitis C virus-infected liver",

abstract = "Murine intrahepatic lymphocytes (IHL) are dominated by invariant TCR α-chain expressing CD1d-reactive NKT cells, which can cause model hepatitis. Invariant NKT (CD56+/-CD161+) and recently identified noninvariant CD1d-reactive T cells rapidly produce large amounts of IL-4 and/or IFN-γ and can regulate Th1/Th2 responses. Haman liver contains large numbers of CD56+ NKT cells but few invariant NKT. Compared with matched peripheral blood T cell lines, primary IHL lines from patients with chronic hepatitis C had high levels of CD161 and CD1d reactivity, but the invariant TCR was rare. CD1d-reactive IHL were strikingly Th1 biased. IHL also demonstrated CD1d-specific cytotoxic activity. Hepatocytes and other liver cells express CD1d. These results identify a novel population of human T cells that could contribute to destructive as well as protective immune responses in the liver. CD1d-reactive T cells may have distinct roles in different tissues.",

author = "Exley, {Mark A.} and Qi He and Olivia Cheng and Wang, {Ruo Jie} and Cheney, {Catherine P.} and Balk, {Steven P.} and Koziel, {Margaret J.}",

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language = "English",

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T1 - Cutting edge: Compartmentalization of Th1-like noninvariant CD1d-reactive T cells in hepatitis C virus-infected liver

AU - Exley, Mark A.

AU - He, Qi

AU - Cheng, Olivia

AU - Wang, Ruo Jie

AU - Cheney, Catherine P.

AU - Balk, Steven P.

AU - Koziel, Margaret J.

N1 - AI41563, NIAID NIH HHS, United StatesAI42955, NIAID NIH HHS, United StatesCA89567, NCI NIH HHS, United States

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N2 - Murine intrahepatic lymphocytes (IHL) are dominated by invariant TCR α-chain expressing CD1d-reactive NKT cells, which can cause model hepatitis. Invariant NKT (CD56+/-CD161+) and recently identified noninvariant CD1d-reactive T cells rapidly produce large amounts of IL-4 and/or IFN-γ and can regulate Th1/Th2 responses. Haman liver contains large numbers of CD56+ NKT cells but few invariant NKT. Compared with matched peripheral blood T cell lines, primary IHL lines from patients with chronic hepatitis C had high levels of CD161 and CD1d reactivity, but the invariant TCR was rare. CD1d-reactive IHL were strikingly Th1 biased. IHL also demonstrated CD1d-specific cytotoxic activity. Hepatocytes and other liver cells express CD1d. These results identify a novel population of human T cells that could contribute to destructive as well as protective immune responses in the liver. CD1d-reactive T cells may have distinct roles in different tissues.

AB - Murine intrahepatic lymphocytes (IHL) are dominated by invariant TCR α-chain expressing CD1d-reactive NKT cells, which can cause model hepatitis. Invariant NKT (CD56+/-CD161+) and recently identified noninvariant CD1d-reactive T cells rapidly produce large amounts of IL-4 and/or IFN-γ and can regulate Th1/Th2 responses. Haman liver contains large numbers of CD56+ NKT cells but few invariant NKT. Compared with matched peripheral blood T cell lines, primary IHL lines from patients with chronic hepatitis C had high levels of CD161 and CD1d reactivity, but the invariant TCR was rare. CD1d-reactive IHL were strikingly Th1 biased. IHL also demonstrated CD1d-specific cytotoxic activity. Hepatocytes and other liver cells express CD1d. These results identify a novel population of human T cells that could contribute to destructive as well as protective immune responses in the liver. CD1d-reactive T cells may have distinct roles in different tissues.

M3 - Article

C2 - 11823474

SN - 1550-6606

VL - 168

SP - 1519

EP - 1523

JO - Journal of Immunology

JF - Journal of Immunology

IS - 4

ER -

Cutting edge: Compartmentalization of Th1-like noninvariant CD1d-reactive T cells in hepatitis C virus-infected liver

Abstract

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