Sphingosine d18:1 promotes nonalcoholic steatohepatitis by inhibiting macrophage HIF-2α.
Jialin XiaHong ChenXiaoxiao WangWeixuan ChenJun LinFeng XuQixing NieChuan YeBitao ZhongMin ZhaoChuyu YunGuangyi ZengYuejian MaoYongping WenXuguang ZhangSen YanXuemei WangLulu SunFeng LiuChao ZhongPengyan XiaChang-Tao JiangHui-Ying RaoYanli PangPublished in: Nature communications (2024)
Non-alcoholic steatohepatitis (NASH) is a severe type of the non-alcoholic fatty liver disease (NAFLD). NASH is a growing global health concern due to its increasing morbidity, lack of well-defined biomarkers and lack of clinically effective treatments. Using metabolomic analysis, the most significantly changed active lipid sphingosine d18:1 [So(d18:1)] is selected from NASH patients. So(d18:1) inhibits macrophage HIF-2α as a direct inhibitor and promotes the inflammatory factors secretion. Male macrophage-specific HIF-2α knockout and overexpression mice verified the protective effect of HIF-2α on NASH progression. Importantly, the HIF-2α stabilizer FG-4592 alleviates liver inflammation and fibrosis in NASH, which indicated that macrophage HIF-2α is a potential drug target for NASH treatment. Overall, this study confirms that So(d18:1) promotes NASH and clarifies that So(d18:1) inhibits the transcriptional activity of HIF-2α in liver macrophages by suppressing the interaction of HIF-2α with ARNT, suggesting that macrophage HIF-2α may be a potential target for the treatment of NASH.
Keyphrases
- endothelial cells
- adipose tissue
- global health
- oxidative stress
- end stage renal disease
- public health
- gene expression
- emergency department
- chronic kidney disease
- ejection fraction
- type diabetes
- cell proliferation
- risk assessment
- liver fibrosis
- combination therapy
- drug induced
- heat shock
- heat shock protein
- replacement therapy