Augmentation of Vα14 Nkt Cell–Mediated Cytotoxicity by Interleukin 4 in an Autocrine Mechanism Resulting in the Development of Concanavalin a–Induced Hepatitis

The administration of concanavalin A (Con A) induces a rapid severe injury of hepatocytes in mice. Although the Con A–induced hepatitis is considered to be an experimental model of human autoimmune hepatitis, the precise cellular and molecular mechanisms that induce hepatocyte injury remain unclear....

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Autores principales: Kaneko, Yoshikatsu, Harada, Michishige, Kawano, Tetsu, Yamashita, Masakatsu, Shibata, Youichi, Gejyo, Fumitake, Nakayama, Toshinori, Taniguchi, Masaru
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 2000
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2195789/
https://www.ncbi.nlm.nih.gov/pubmed/10620609
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author Kaneko, Yoshikatsu
Harada, Michishige
Kawano, Tetsu
Yamashita, Masakatsu
Shibata, Youichi
Gejyo, Fumitake
Nakayama, Toshinori
Taniguchi, Masaru
author_facet Kaneko, Yoshikatsu
Harada, Michishige
Kawano, Tetsu
Yamashita, Masakatsu
Shibata, Youichi
Gejyo, Fumitake
Nakayama, Toshinori
Taniguchi, Masaru
author_sort Kaneko, Yoshikatsu
collection PubMed
description The administration of concanavalin A (Con A) induces a rapid severe injury of hepatocytes in mice. Although the Con A–induced hepatitis is considered to be an experimental model of human autoimmune hepatitis, the precise cellular and molecular mechanisms that induce hepatocyte injury remain unclear. Here, we demonstrate that Vα14 NKT cells are required and sufficient for induction of this hepatitis. Moreover, interleukin (IL)-4 produced by Con A–activated Vα14 NKT cells is found to play a crucial role in disease development by augmenting the cytotoxic activity of Vα14 NKT cells in an autocrine fashion. Indeed, short-term treatment with IL-4 induces an increase in the expression of granzyme B and Fas ligand (L) in Vα14 NKT cells. Moreover, Vα14 NKT cells from either perforin knock-out mice or FasL-mutant gld/gld mice fail to induce hepatitis, and hence perforin–granzyme B and FasL appear to be effector molecules in Con A–induced Vα14 NKT cell–mediated hepatocyte injury.
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spelling pubmed-21957892008-04-16 Augmentation of Vα14 Nkt Cell–Mediated Cytotoxicity by Interleukin 4 in an Autocrine Mechanism Resulting in the Development of Concanavalin a–Induced Hepatitis Kaneko, Yoshikatsu Harada, Michishige Kawano, Tetsu Yamashita, Masakatsu Shibata, Youichi Gejyo, Fumitake Nakayama, Toshinori Taniguchi, Masaru J Exp Med Original Article The administration of concanavalin A (Con A) induces a rapid severe injury of hepatocytes in mice. Although the Con A–induced hepatitis is considered to be an experimental model of human autoimmune hepatitis, the precise cellular and molecular mechanisms that induce hepatocyte injury remain unclear. Here, we demonstrate that Vα14 NKT cells are required and sufficient for induction of this hepatitis. Moreover, interleukin (IL)-4 produced by Con A–activated Vα14 NKT cells is found to play a crucial role in disease development by augmenting the cytotoxic activity of Vα14 NKT cells in an autocrine fashion. Indeed, short-term treatment with IL-4 induces an increase in the expression of granzyme B and Fas ligand (L) in Vα14 NKT cells. Moreover, Vα14 NKT cells from either perforin knock-out mice or FasL-mutant gld/gld mice fail to induce hepatitis, and hence perforin–granzyme B and FasL appear to be effector molecules in Con A–induced Vα14 NKT cell–mediated hepatocyte injury. The Rockefeller University Press 2000-01-03 /pmc/articles/PMC2195789/ /pubmed/10620609 Text en © 2000 The Rockefeller University Press This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 4.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/4.0/).
spellingShingle Original Article
Kaneko, Yoshikatsu
Harada, Michishige
Kawano, Tetsu
Yamashita, Masakatsu
Shibata, Youichi
Gejyo, Fumitake
Nakayama, Toshinori
Taniguchi, Masaru
Augmentation of Vα14 Nkt Cell–Mediated Cytotoxicity by Interleukin 4 in an Autocrine Mechanism Resulting in the Development of Concanavalin a–Induced Hepatitis
title Augmentation of Vα14 Nkt Cell–Mediated Cytotoxicity by Interleukin 4 in an Autocrine Mechanism Resulting in the Development of Concanavalin a–Induced Hepatitis
title_full Augmentation of Vα14 Nkt Cell–Mediated Cytotoxicity by Interleukin 4 in an Autocrine Mechanism Resulting in the Development of Concanavalin a–Induced Hepatitis
title_fullStr Augmentation of Vα14 Nkt Cell–Mediated Cytotoxicity by Interleukin 4 in an Autocrine Mechanism Resulting in the Development of Concanavalin a–Induced Hepatitis
title_full_unstemmed Augmentation of Vα14 Nkt Cell–Mediated Cytotoxicity by Interleukin 4 in an Autocrine Mechanism Resulting in the Development of Concanavalin a–Induced Hepatitis
title_short Augmentation of Vα14 Nkt Cell–Mediated Cytotoxicity by Interleukin 4 in an Autocrine Mechanism Resulting in the Development of Concanavalin a–Induced Hepatitis
title_sort augmentation of vα14 nkt cell–mediated cytotoxicity by interleukin 4 in an autocrine mechanism resulting in the development of concanavalin a–induced hepatitis
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2195789/
https://www.ncbi.nlm.nih.gov/pubmed/10620609
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