超越胆汁酸：用天然和合成配体靶向法尼醇X受体（FXR）

Beyond bile acids: targeting Farnesoid X Receptor (FXR) with natural and synthetic ligands.

作者信息

Carotti Andrea, Marinozzi Maura, Custodi Chiara, Cerra Bruno, Pellicciari Roberto, Gioiello Antimo, Macchiarulo Antonio

机构信息

Dipartimento di Scienze Farmaceutiche, Via del Liceo 1 06123 Perugia, Italy.

出版信息

Curr Top Med Chem. 2014;14(19):2129-42. doi: 10.2174/1568026614666141112094058.

DOI:10.2174/1568026614666141112094058

PMID:25388537

Abstract

The modulation of FXR receptor remains an attractive area in drug discovery to develop novel therapeutic opportunities for liver and metabolic disorders. Despite the large variety of FXR ligands reported so far, only a very restricted number of agonists have entered in clinical settings. In this review article we provide the reader with an overview on the different classes of natural and synthetic ligands that have been developed by academic groups and pharmaceutical companies to target FXR. We discuss their structure-activity relationships, analyzing the binding modes that some of these compounds adopt to interact with the receptor.

摘要

法尼醇X受体（FXR）的调节仍是药物研发中一个具有吸引力的领域，有望为肝脏和代谢紊乱开发新的治疗机会。尽管目前已报道了种类繁多的FXR配体，但只有极少数激动剂进入了临床阶段。在这篇综述文章中，我们向读者概述了学术团体和制药公司开发的针对FXR的不同类型的天然和合成配体。我们讨论它们的构效关系，分析其中一些化合物与受体相互作用所采用的结合模式。

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超越胆汁酸：用天然和合成配体靶向法尼醇X受体（FXR）

Beyond bile acids: targeting Farnesoid X Receptor (FXR) with natural and synthetic ligands.

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