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Pharmacological Applications of Bile Acids and Their Derivatives in the Treatment of Metabolic Syndrome

机译:胆汁酸及其衍生物在代谢综合征治疗中的药理应用

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摘要

Apart from well-known functions of bile acids in digestion and solubilization of lipophilic nutrients and drugs in the small intestine, the emerging evidence from the past two decades identified the role of bile acids as signaling, endocrine molecules that regulate the glucose, lipid, and energy metabolism through complex and intertwined pathways that are largely mediated by activation of nuclear receptor farnesoid X receptor (FXR) and cell surface G protein-coupled receptor 1, TGR5 (also known as GPBAR1). Interactions of bile acids with the gut microbiota that result in the altered composition of circulating and intestinal bile acids pool, gut microbiota composition and modified signaling pathways, are further extending the complexity of biological functions of these steroid derivatives. Thus, bile acids signaling pathways have become attractive targets for the treatment of various metabolic diseases and metabolic syndrome opening the new potential avenue in their treatment. In addition, there is a significant effort to unveil some specific properties of bile acids relevant to their intrinsic potency and selectivity for particular receptors and to design novel modulators of these receptors with improved pharmacokinetic and pharmacodynamic profiles. This resulted in synthesis of few semi-synthetic bile acids derivatives such as 6α-ethyl-chenodeoxycholic acid (obeticholic acid, OCA), norursodeoxycholic acid (norUDCA), and 12-monoketocholic acid (12-MKC) that are proven to have positive effect in metabolic and hepato-biliary disorders. This review presents an overview of the current knowledge related to bile acids implications in glucose, lipid and energy metabolism, as well as a potential application of bile acids in metabolic syndrome treatment with future perspectives.
机译:除了胆汁酸在小肠中脂溶性营养物质和药物的消化和增溶中的众所周知的功能外,过去二十年来的新证据还表明胆汁酸的作用是调节葡萄糖,脂质和脂肪的内分泌分子的信号传导。通过复杂且相互缠绕的途径进行能量代谢,这些途径主要由核受体法呢类X受体(FXR)和细胞表面G蛋白偶联受体1 TGR5(也称为GPBAR1)的激活介导。胆汁酸与肠道菌群的相互作用导致循环和肠道胆汁酸池组成的改变,肠道菌群组成和信号通路的改变,进一步扩大了这些类固醇衍生物的生物学功能的复杂性。因此,胆汁酸信号传导途径已成为治疗各种代谢疾病和代谢综合症的有吸引力的靶标,从而在其治疗中打开了新的潜在途径。此外,还付出了巨大的努力来揭示胆汁酸的某些特定特性,这些特性与其对特定受体的内在效力和选择性有关,并设计具有改善的药代动力学和药效学特征的这些受体的新型调节剂。这导致合成了半合成的胆汁酸衍生物,如6α-乙基-去氧胆酸(obticholic acid,OCA),去甲去氧胆酸(norUDCA)和12-单酮胆酸(12-MKC)在代谢和肝胆疾病中。这篇综述概述了与胆汁酸在葡萄糖,脂质和能量代谢中的意义有关的当前知识,以及胆汁酸在代谢综合征治疗中的潜在应用。

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