Ubiquitously specific protease 4 inhibitor‐Vialinin A attenuates inflammation and fibrosis in S100‐induced hepatitis mice through Rheb/mTOR signalling

Inflammation and fibrosis are major consequences of autoimmune hepatitis, however, the therapeutic mechanism remains to be investigated. USP4 is a deubiquitinating enzyme and plays an important role in tissue fibrosis and immune disease. Vialinin A is an extract from mushroom and is a specific USP4...

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Autores principales: Xu, Jie, Chen, Dazhi, Jin, Lanling, Chen, Zhengkang, Tu, Yulu, Huang, Xiaozhe, Xue, Feiben, Xu, Jialu, Chen, Mingzhuan, Wang, Xiaodong, Chen, Yongping
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2020
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Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7812299/
https://www.ncbi.nlm.nih.gov/pubmed/33295107
http://dx.doi.org/10.1111/jcmm.16180
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author Xu, Jie
Chen, Dazhi
Jin, Lanling
Chen, Zhengkang
Tu, Yulu
Huang, Xiaozhe
Xue, Feiben
Xu, Jialu
Chen, Mingzhuan
Wang, Xiaodong
Chen, Yongping
author_facet Xu, Jie
Chen, Dazhi
Jin, Lanling
Chen, Zhengkang
Tu, Yulu
Huang, Xiaozhe
Xue, Feiben
Xu, Jialu
Chen, Mingzhuan
Wang, Xiaodong
Chen, Yongping
author_sort Xu, Jie
collection PubMed
description Inflammation and fibrosis are major consequences of autoimmune hepatitis, however, the therapeutic mechanism remains to be investigated. USP4 is a deubiquitinating enzyme and plays an important role in tissue fibrosis and immune disease. Vialinin A is an extract from mushroom and is a specific USP4 inhibitor. However, there is lack of evidences that Vialinin A plays a role in autoimmune hepatitis. By employing S100‐induced autoimmune hepatitis in mice and AML12 cell line, therapeutic mechanism of Vialinin A was examined. Inflammation was documented by liver histological staining and inflammatory cytokines. Fibrosis was demonstrated by Masson, Sirius red staining and fibrotic cytokines with western blot and real‐time RT‐PCR. In experimental animal, there were increases in inflammation and fibrosis as well as USP4, and which were reduced after treatment of Vialinin A. Vialinin A also reduced Rheb and phosphorylated mTOR. Moreover, in LPS‐treated AML12 cells, LPS‐induced USP4, inflammatory and fibrotic cytokines, phosphorylated mTOR and Rheb. Specific inhibitory siRNA of USP4 reduced USP4 level and the parameters mentioned above. In conclusion, USP4 was significantly elevated in autoimmune hepatitis mice and Vialinin A reduced USP4 level and attenuate inflammation and fibrosis in the liver. The mechanism may be related to regulation of Rheb/mTOR signalling.
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spelling pubmed-78122992021-01-22 Ubiquitously specific protease 4 inhibitor‐Vialinin A attenuates inflammation and fibrosis in S100‐induced hepatitis mice through Rheb/mTOR signalling Xu, Jie Chen, Dazhi Jin, Lanling Chen, Zhengkang Tu, Yulu Huang, Xiaozhe Xue, Feiben Xu, Jialu Chen, Mingzhuan Wang, Xiaodong Chen, Yongping J Cell Mol Med Original Articles Inflammation and fibrosis are major consequences of autoimmune hepatitis, however, the therapeutic mechanism remains to be investigated. USP4 is a deubiquitinating enzyme and plays an important role in tissue fibrosis and immune disease. Vialinin A is an extract from mushroom and is a specific USP4 inhibitor. However, there is lack of evidences that Vialinin A plays a role in autoimmune hepatitis. By employing S100‐induced autoimmune hepatitis in mice and AML12 cell line, therapeutic mechanism of Vialinin A was examined. Inflammation was documented by liver histological staining and inflammatory cytokines. Fibrosis was demonstrated by Masson, Sirius red staining and fibrotic cytokines with western blot and real‐time RT‐PCR. In experimental animal, there were increases in inflammation and fibrosis as well as USP4, and which were reduced after treatment of Vialinin A. Vialinin A also reduced Rheb and phosphorylated mTOR. Moreover, in LPS‐treated AML12 cells, LPS‐induced USP4, inflammatory and fibrotic cytokines, phosphorylated mTOR and Rheb. Specific inhibitory siRNA of USP4 reduced USP4 level and the parameters mentioned above. In conclusion, USP4 was significantly elevated in autoimmune hepatitis mice and Vialinin A reduced USP4 level and attenuate inflammation and fibrosis in the liver. The mechanism may be related to regulation of Rheb/mTOR signalling. John Wiley and Sons Inc. 2020-12-09 2021-01 /pmc/articles/PMC7812299/ /pubmed/33295107 http://dx.doi.org/10.1111/jcmm.16180 Text en © 2020 The Authors. Journal of Cellular and Molecular Medicine published by Foundation for Cellular and Molecular Medicine and John Wiley & Sons Ltd. This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Articles
Xu, Jie
Chen, Dazhi
Jin, Lanling
Chen, Zhengkang
Tu, Yulu
Huang, Xiaozhe
Xue, Feiben
Xu, Jialu
Chen, Mingzhuan
Wang, Xiaodong
Chen, Yongping
Ubiquitously specific protease 4 inhibitor‐Vialinin A attenuates inflammation and fibrosis in S100‐induced hepatitis mice through Rheb/mTOR signalling
title Ubiquitously specific protease 4 inhibitor‐Vialinin A attenuates inflammation and fibrosis in S100‐induced hepatitis mice through Rheb/mTOR signalling
title_full Ubiquitously specific protease 4 inhibitor‐Vialinin A attenuates inflammation and fibrosis in S100‐induced hepatitis mice through Rheb/mTOR signalling
title_fullStr Ubiquitously specific protease 4 inhibitor‐Vialinin A attenuates inflammation and fibrosis in S100‐induced hepatitis mice through Rheb/mTOR signalling
title_full_unstemmed Ubiquitously specific protease 4 inhibitor‐Vialinin A attenuates inflammation and fibrosis in S100‐induced hepatitis mice through Rheb/mTOR signalling
title_short Ubiquitously specific protease 4 inhibitor‐Vialinin A attenuates inflammation and fibrosis in S100‐induced hepatitis mice through Rheb/mTOR signalling
title_sort ubiquitously specific protease 4 inhibitor‐vialinin a attenuates inflammation and fibrosis in s100‐induced hepatitis mice through rheb/mtor signalling
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7812299/
https://www.ncbi.nlm.nih.gov/pubmed/33295107
http://dx.doi.org/10.1111/jcmm.16180
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