泛素连接酶
非酒精性脂肪肝
基因沉默
发病机制
调节器
泛素
炎症
脂肪性肝炎
生物
脂肪肝
癌症研究
细胞生物学
下调和上调
疾病
胰岛素抵抗
SOCS3
蛋白酶体
医学
过度活跃
信号转导
福克斯O1
体内
调解人
肝病
化学
MAPK/ERK通路
生物信息学
免疫学
RNA干扰
转染
氧化应激
分解代谢
非酒精性脂肪性肝炎
基因表达调控
促炎细胞因子
多不饱和脂肪酸
内分泌学
HEK 293细胞
小发夹RNA
脂肪变性
作者
Feng Juan Yan,Han Ding,Ning Zhang,Shi-Ran Yan,Mei Xin Huang,Jing-Wei Lu,Yong-Jian Wang,Yu-Jie Yan,Rong-peng Li,Qun Wang,Feng Juan Yan,Han Ding,Ning Zhang,Shi-Ran Yan,Mei Xin Huang,Jing-Wei Lu,Yong-Jian Wang,Yu-Jie Yan,Rong-peng Li,Qun Wang
标识
DOI:10.1038/s41467-025-65415-6
摘要
Non-alcoholic fatty liver disease (NAFLD) and its more severe form, nonalcoholic steatohepatitis (NASH), have emerged as a burgeoning global epidemic and impose an enormous socioeconomic burden. However, the lack of effective pharmacotherapies is due to incomplete understanding of the molecular mechanisms of NASH. In the present study, we observe that E3 ligase TRIM7 expression is significantly increased in both liver tissues and hepatocytes from NAFLD models. In vivo gain- and loss-of-function experiments reveal that hepatic-specific TRIM7 deletion significantly alleviates hepatic steatosis, inflammation and insulin resistance in diet-induced male mouse models, whereas overexpression of wild-type TRIM7 (but not its E3-deficient mutant) shows diametrically opposite effects. Mechanistic studies reveal that TRIM7 interacts with and catalyzes DUSP10 ubiquitination and proteasomal degradation, thus leading to hyperactivation of IKKβ-NF-κB and JNK/p38 MAPK signaling pathways. Importantly, silencing DUSP10 expression abrogates the protective effects of hepatic TRIM7 deficiency on NAFLD-related pathological phenotypes. Collectively, our findings identify TRIM7 as a key regulator of the pathogenesis of NAFLD/NASH and provide a promising therapeutic strategy for NAFLD by targeting the TRIM7-DUSP10 axis.
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