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A20 in hepatic stellate cells suppresses chronic hepatitis by inhibiting DCLK1 – JNK pathway‐dependent chemokines

趋化因子 肝星状细胞 炎症 细胞生物学 基因沉默 癌症研究 化学 生物 免疫学 基因 内分泌学 生物化学
作者
Keiya Watakabe,Masato Miyoshi,Sei Kakinuma,Ayako Sato,Jun Tsuchiya,Taro Shimizu,Tomohiro Mochida,Kento Inada,Shun Kaneko,Fukiko Kawai‐Kitahata,Miyako Murakawa,Sayuri Nitta,Mina Nakagawa,Shigeru Oshima,Mamoru Watanabe,Averil Ma,Yasuhiro Asahina,Ryuichi Okamoto
出处
期刊:The FASEB Journal [Wiley]
卷期号:38 (13): e23757-e23757 被引量:4
标识
DOI:10.1096/fj.202400109r
摘要

Hepatic stellate cells (HSCs) are responsible for liver fibrosis accompanied by its activation into myofibroblasts and the abundant production of extracellular matrix. However, the HSC contribution to progression of liver inflammation has been less known. We aimed to elucidate the mechanism in HSCs underlying the inflammatory response and the function of tumor necrosis factor α-related protein A20 (TNFAIP3). We established A20 conditional knockout (KO) mice crossing Twist2-Cre and A20 floxed mice. Using these mice, the effect of A20 was analyzed in mouse liver and HSCs. The human HSC line LX-2 was also used to examine the role and underlying molecular mechanism of A20. In this KO model, A20 was deficient in >80% of HSCs. Spontaneous inflammation with mild fibrosis was found in the liver of the mouse model without any exogenous agents, suggesting that A20 in HSCs suppresses chronic hepatitis. Comprehensive RNA sequence analysis revealed that A20-deficient HSCs exhibited an inflammatory phenotype and abnormally expressed chemokines. A20 suppressed JNK pathway activation in HSCs. Loss of A20 function in LX-2 cells also induced excessive chemokine expression, mimicking A20-deficient HSCs. A20 overexpression suppressed chemokine expression in LX-2. In addition, we identified DCLK1 in the genes regulated by A20. DCLK1 activated the JNK pathway and upregulates chemokine expression. DCLK1 inhibition significantly decreased chemokine induction by A20-silencing, suggesting that A20 controlled chemokine expression in HSCs via the DCLK1-JNK pathway. In conclusion, A20 suppresses chemokine induction dependent on the DCLK1-JNK signaling pathway. These findings demonstrate the therapeutic potential of A20 and the DCLK1-JNK pathway for the regulation of inflammation in chronic hepatitis.
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