橙皮素通过靶向线粒体调控肝细胞焦亡在缓解酒精性肝损伤中的作用及机制OA
Effects and mechanisms of hesperetin in attenuating alcoholic liver injury by targeting mitochondria to regulate hepatocyte pyroptosis
该研究通过体外实验探讨橙皮素(hesperetin,HST)靶向线粒体调控肝细胞焦亡,缓解酒精性肝损伤的作用及潜在机制.以人永生化肝细胞(THLE-2)为研究对象,用 200 mmol·L-1乙醇建立体外酒精性肝损伤模型;通过 MTT 法确定 HST 的有效作用剂量(40、80、160 μmol·L-1),并采用光学显微镜观察、乳酸脱氢酶(LDH)释放实验、流式细胞术分析 HST 对肝细胞焦亡的影响,结合尼罗红染色及胆固醇、甘油三酯试剂盒检测评估其对脂质堆积的作用.进一步用高剂量 HST 干预,通过Western blot 和 PCR 实验检测焦亡相关分子半胱氨酸蛋白酶-1(caspase-1)、消皮素 D(GSDMD)、白细胞介素-18(IL-18)、白细胞介素-1β(IL-1β)的表达;联合 caspase-1抑制剂(Z-YVAD FMK)反向验证 HST 对经典焦亡途径的调控作用.通过激光共聚焦显微镜观察内质网、溶酶体以及线粒体的形态,试剂盒检测超氧化物歧化酶(SOD)含量,流式细胞术分析线粒体膜电位,PCR 法检测线粒体膜转运蛋白电压依赖性阴离子通道 1(VDAC1)、线粒体膜转运蛋白电压依赖性阴离子通道 2(VDAC2)、线粒体外膜转位酶 20(TOM20)、线粒体外膜转位酶 34(TOM34)的基因表达;联合线粒体活性氧(mtROS)诱导剂鱼藤酮(rote-none),验证 HST 对线粒体功能的靶向调控效应.实验结果显示,HST 可剂量依赖性提高肝细胞活力、降低 LDH 水平,显著缓解细胞焦亡并改善脂质堆积,同时下调 caspase-1、GSDMD、IL-18、IL-1β 的表达;加入 caspase-1 抑制剂后,HST 对细胞焦亡的抑制作用进一步得到证实.机制探索发现,HST 可靶向线粒体,清除 mtROS、上调 SOD 表达、恢复线粒体膜电位,并下调线粒体膜相关转运蛋白 VDAC1、VDAC2、TOM20、TOM34 的表达;加入 mtROS 诱导剂 rotenone,反向验证了 HST 靶向线粒体缓解细胞焦亡.综上所述,HST 可通过靶向线粒体、调控经典焦亡途径减轻肝细胞焦亡损伤并改善脂质代谢紊乱,最终缓解酒精性肝损伤,为 HST 在酒精性肝损伤治疗中的临床应用提供理论依据.
This study investigated the effects and potential mechanisms of hesperetin(HST)in targeting mitochondria to regulate hepatocyte pyroptosis and alleviate alcoholic liver injury through in vitro experiments.Human immortalized hepatocytes(THLE-2)were used to establish an in vitro alcoholic liver injury model induced by 200 mmol·L-1 ethanol.The effective concentrations of HST(40,80,and 160 μmol·L-1)were determined using the MTT assay.The effects of HST on hepatocyte pyroptosis were evaluated by optical microscopy,lactate dehydrogenase(LDH)release assay,and flow cytometry,and its effects on lipid accumulation were assessed using Nile red staining and cholesterol and triglyceride assay kits.Further intervention with a high dose of HST was performed,and the expression levels of pyroptosis-related molecules,including caspase-1,gasdermin D(GSDMD),interleukin-18(IL-18),and interleukin-1β(IL-1β),were detected by Western blot and PCR.In addition,a caspase-1 inhibitor(Z-YVAD-FMK)was used to reversely validate the regulatory effect of HST on the classical pyroptosis pathway.The morphology of the endoplasmic reticulum,lysosomes,and mitochondria was observed using confocal laser scanning microscopy.Superoxide dismutase(SOD)levels were measured using a commercial assay kit,mitochondrial membrane potential was analyzed by flow cytometry,and the gene expression levels of mitochondrial membrane transport proteins,including voltage-dependent anion channel 1(VDAC1),voltage-dependent anion channel 2(VDAC2),translocase of the outer mitochondrial membrane 20(TOM20),and translocase of the outer mitochondrial membrane 34(TOM34),were determined by PCR.Meanwhile,the mitochondrial reactive oxygen species(mtROS)inducer rotenone was employed to validate the mitochondria-targeted regulatory effects of HST on mitochondrial function.The experimental results showed that HST concentration-dependently increased hepatocyte viability,reduced LDH levels,significantly alleviated hepatocyte pyroptosis,and improved lipid accumulation,while downregulating the expression of caspase-1,GSDMD,IL-18,and IL-1β.After the addition of a caspase-1 inhibitor,the inhibitory effect of HST on hepatocyte pyroptosis was further confirmed.Mechanistic investigations revealed that HST targeted mitochondria by scavenging mtROS,upregulating SOD expression,restoring mitochondrial membrane potential,and downregulating the expression of mitochondrial membrane-associated transport proteins VDAC1,VDAC2,TOM20,and TOM34.Furthermore,the addition of the mtROS inducer rotenone reversely validated the role of HST in alleviating hepatocyte pyroptosis through mitochondrial targeting.In summary,HST alleviates hepatocyte pyroptosis and improves lipid metabolism disorders by targeting mitochondria and regulating the classical pyroptosis pathway,thereby mitigating alcoholic liver injury.These findings provide a theoretical basis for the potential clinical application of HST in the treatment of alcoholic liver injury.
张卫东;华丰;赵权;黄玮;张晶;王访;王飞虾;陈薇;张晓鸣
常州市中医医院,江苏 常州 213000常州市中医医院,江苏 常州 213000常州市中医医院,江苏 常州 213000常州市中医医院,江苏 常州 213000常州市中医医院,江苏 常州 213000常州市中医医院,江苏 常州 213000南京中医药大学,江苏 南京 210000常州市中医医院,江苏 常州 213000常州市中医医院,江苏 常州 213000
橙皮素酒精性肝损伤细胞焦亡线粒体靶向脂代谢
hesperetinalcoholic liver injurypyroptosismitochondria-targetedlipid metabolism
《中国中药杂志》 2026 (8)
2310-2322,13
国家中药炮制技术传承基地建设项目(财社[2022]45号)全国老药工传承工作室建设项目(国中医药人教函[2024]255号)江苏省老药工传承工作室建设项目(苏中医科教[2024]4号)江苏省中药骨干人才高级研修项目(苏中医科教[2022]11号)常州市第五批科技计划(社会发展科技支撑)项目(CE20235068)常州市科技计划(应用基础研究指导性)项目(CJ20229029,CJ20239042,CJ20242049,CJ20253125,CJ20219020,CJ20219011)常州市"龙城强医"工程中医药人才培育项目-张冰岐黄学者工作室项目(常财社[2024]55号)2024年度省中医药学会科研项目(苏中会[2024]62号)2024年度常州市卫健委科技项目(WZ202405)江苏省中医疫病研究中心开放课题(JSYB2024KF30)南京中医药大学自然科学基金项目(XZR2024162)江苏省自然科学基金青年项目(BK20230758)
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