DUSP12 protects against hepatic ischemia–reperfusion injury dependent on ASK1-JNK/p38 pathway in vitro and in vivo

炎症 再灌注损伤 肝细胞生长因子 p38丝裂原活化蛋白激酶 肝细胞 细胞生物学 纤维化 转基因小鼠 肝纤维化 缺血 体内 细胞凋亡 ASK1 药理学 生物 体外 免疫学 医学 MAPK/ERK通路 肝损伤 转基因 信号转导 内科学 受体 生物化学 细胞周期 细胞周期蛋白依赖激酶2 生物技术 基因
作者
Tao Qiu,Tianyu Wang,Jiangqiao Zhou,Zhongbao Chen,Jilin Zou,Long Zhang,Xiaoxiong Ma
出处
期刊:Clinical Science [Portland Press]
卷期号:134 (17): 2279-2294 被引量:16
标识
DOI:10.1042/cs20191272
摘要

Abstract Hepatic ischemia–reperfusion (I/R) injury is an important risk factor resulting in liver failure during liver surgery. However, there is still lack of effective therapeutic methods to treat hepatic I/R injury. DUSP12 is a member of the dual specific phosphatase (DUSP) family. Some DUSPs have been identified as being involved in the regulation of hepatic I/R injury. However, the role of DUSP12 during hepatic I/R injury is still unclear. In the present study, we observed a significant decrease in DUSP12 expression in a hepatic I/R injury mouse model in vivo and in hypoxia/reoxygenation (H/R) model in vitro. Using hepatocyte-specific DUSP12 knockout mice and DUSP12 transgenic mice, we demonstrated that DUSP12 apparently relieved I/R-induced liver injury. Moreover, DUSP12 inhibited hepatic inflammatory responses and alleviated apoptosis both in vitro and in vivo. Furthermore, we demonstrated that JNK and p38 activity, but not ERK1/2, was increased in the DUSP12-deficient mice and decreased in the DUSP12 transgenic mice under I/R condition. ASK1 was required for DUSP12 function in hepatic I/R injury and inhibition of ASK1 prevented inflammation and apoptosis in DUSP12-deficient hepatocytes and mice. In conclusion, DUSP12 protects against hepatic I/R injury and related inflammation and apoptosis. This regulatory role of DUSP12 is primarily through ASK1-JNK/p38 signaling pathway. Taken together, DUSP12 could be a potential therapeutic target for hepatic I/R injury.
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