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缬草属植物缬草的环烯醚萜通过脂噬作用缓解肥胖小鼠的肝脂肪变性。

Iridoids of Valeriana fauriei contribute to alleviating hepatic steatosis in obese mice by lipophagy.

机构信息

Research Division of Food Functionality, Korea Food Research Institute, Wanju-gun, Jeollabuk-do, 55365, Republic of Korea; Department of Food Biotechnology, University of Science and Technology, Daejoen, 34113, Republic of Korea.

Center for Electron Microscopy Research, Korea Basic Science Institute, Cheongju, 28119, Republic of Korea.

出版信息

Biomed Pharmacother. 2020 May;125:109950. doi: 10.1016/j.biopha.2020.109950. Epub 2020 Feb 10.

Abstract

Nonalcoholic fatty liver disease (NAFLD) is a common risk factor for metabolic syndrome that increases the risk of future cardiovascular disease, stroke, and diabetes. Recently, autophagy has been proposed as a means to prevent NAFLD. We investigated whether substances with autophagy-inducing activity alleviate NAFLD. The Valeriana fauriei (V. fauriei) was selected as a potential autophagy inducer among various natural materials using a Cyto-ID autophagy detection kit. V. fauriei 70 % ethanol extract (VFE) increased LC3II levels in the presence of the lysosomal inhibitor and reduced the GFP/mCherry puncta ratio, suggesting that VFE enhanced autophagy. VFE reduced oleic acid (OA)-induced lipid accumulation and increased the number of autophagosome in hepatocytes. Autophagy induction by VFE is due to inhibition of mTORC1 activity. VFE supplementation reduced fatty liver by downregulating lipogenesis-related genes and increased the autophagy, as revealed by TEM and IHC analysis in the fatty liver. We identified iridoids as main compounds of VFE; didrovaltrate (DI), valeriotriate B (VAL B), valeriotetrate C (VAL C), valtrate (VAL), and valechlorine (VC) were shown to enhance autophagy. These compounds also reduced OA-induced lipid accumulation in an Atg5-dependent manner. Taken together, VFE and its iridoids might be effective in alleviating fatty liver by acting as autophagy enhancers to break down LDs.

摘要

非酒精性脂肪性肝病(NAFLD)是代谢综合征的一个常见危险因素,会增加未来患心血管疾病、中风和糖尿病的风险。最近,自噬被认为是预防 NAFLD 的一种方法。我们研究了具有自噬诱导活性的物质是否可以缓解 NAFLD。使用 Cyto-ID 自噬检测试剂盒,从各种天然材料中选择缬草(V. fauriei)作为潜在的自噬诱导剂。V. fauriei 70%乙醇提取物(VFE)在溶酶体抑制剂存在的情况下增加了 LC3II 水平,并降低了 GFP/mCherry 斑点的比值,表明 VFE 增强了自噬。VFE 减少了油酸(OA)诱导的脂质积累,并增加了肝细胞中的自噬体数量。VFE 通过抑制 mTORC1 活性诱导自噬。VFE 通过下调脂肪生成相关基因来减少脂肪肝,并通过 TEM 和 IHC 分析在脂肪肝中增加自噬,从而减少脂肪肝。我们确定了 VFE 的主要化合物为裂环烯醚萜;二氢缬草三酯(DI)、缬草三酯 B(VAL B)、缬草四酯 C(VAL C)、缬草酯(VAL)和缬草氯(VC)均显示出增强自噬的作用。这些化合物还以 Atg5 依赖的方式减少了 OA 诱导的脂质积累。总之,VFE 及其裂环烯醚萜类化合物可能通过作为自噬增强剂来分解 LD,从而有效缓解脂肪肝。

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