PX-478对低剪应力诱导血管内皮细胞炎性反应的效应机制

目的:探讨低氧诱导因子-1α(HIF-1α)特异性抑制剂PX-478能否抑制低剪应力(LWSS)诱导的动脉粥样硬化。方法:人脐静脉内皮细胞分为:高剪应力组(HWSS)、LWSS组和LWSS+PX-478组,检测HIF-1α和下游基因表达。C57BL6雄性小鼠腹腔注射PX-478,检测动脉内皮细胞HIF-1α表达。对Apoe^(-/-)小鼠部分(颈内动脉、颈外动脉、枕动脉)颈动脉结扎,腹腔注射PX-478,观察颈动脉HIF-1α和炎症分子表达以及颈动脉粥样硬化。组间比较采用t检验。结果:PX-478组HIF-1α表达(3.380±0.388比22.200±1.458,t=6.057,P<0.01)低于DMSO组。PCAL组内皮细胞炎症(955.661±172.953比15.200±3.384,t=5.437,P<0.01)和动脉粥样硬化程度(39.739±1.683比6.020±0.766,t=18.24,P<0.01)重于对照组,PCAL+PX-478组动脉内皮细胞炎症(163.978±15.035比955.661±172.953,t=4.560,P<0.01)与动脉粥样硬化程度(16.847±1.584比39.739±1.683,t=9.905,P<0.01)轻于PCAL组。结论:PX-478降低LWSS诱导的HIF-1α表达,缓解内皮细胞炎症,抑制动脉粥样硬化的发生。

Disruption of adipocyte HIF-1α improves atherosclerosis through the inhibition of ceramide generation

Atherosclerosis is a chronic multifactorial cardiovascular disease.Western diets have been reported to affect atherosclerosis through regulating adipose function.In high cholesterol diet-fed ApoE^(−/−)mice,adipocyte HIF-1αdeficiency or direct inhibition of HIF-1αby the selective pharmacological HIF-1αinhibitor PX-478 alleviates high cholesterol diet-induced atherosclerosis by reducing adipose ceramide generation,which lowers cholesterol levels and reduces inflammatory responses,resulting in improved dyslipidemia and atherogenesis.Smpd3,the gene encoding neutral sphingomyelinase,is identified as a new target gene directly regulated by HIF-1αthat is involved in ceramide generation.Injection of lentivirus-SMPD3 in epididymal adipose tissue reverses the decrease in ceramides in adipocytes and eliminates the improvements on atherosclerosis in the adipocyte HIF-1α-deficient mice.Therefore,HIF-1αinhibition may constitute a novel approach to slow atherosclerotic progression.