AUTHOR=Diao Yanyan , Jiang Jing , Zhang Shoude , Li Shiliang , Shan Lei , Huang Jin , Zhang Weidong , Li Honglin 

TITLE=Discovery of Natural Products as Novel and Potent FXR Antagonists by Virtual Screening

JOURNAL=Frontiers in Chemistry

VOLUME=6

YEAR=2018

URL=https://www.frontiersin.org/journals/chemistry/articles/10.3389/fchem.2018.00140

DOI=10.3389/fchem.2018.00140

ISSN=2296-2646

ABSTRACT=<p>Farnesoid X receptor (FXR) is a member of nuclear receptor family involved in multiple physiological processes through regulating specific target genes. The critical role of FXR as a transcriptional regulator makes it a promising target for diverse diseases, especially those related to metabolic disorders such as diabetes and cholestasis. However, the underlying activation mechanism of FXR is still a blur owing to the absence of proper FXR modulators. To identify potential FXR modulators, an in-house natural product database (NPD) containing over 4,000 compounds was screened by structure-based virtual screening strategy and subsequent hit-based similarity searching method. After the yeast two-hybrid (Y2H) assay, six natural products were identified as FXR antagonists which blocked the CDCA-induced SRC-1 association. The IC<sub>50</sub> values of compounds <bold>2a</bold>, a diterpene bearing polycyclic skeleton, and <bold>3a</bold>, named daphneone with chain scaffold, are as low as 1.29 and 1.79 μM, respectively. Compared to the control compound guggulsterone (IC<sub>50</sub> = 6.47 μM), compounds <bold>2a</bold> and <bold>3a</bold> displayed 5- and 3-fold higher antagonistic activities against FXR, respectively. Remarkably, the two representative compounds shared low topological similarities with other reported FXR antagonists. According to the putative binding poses, the molecular basis of these antagonists against FXR was also elucidated in this report.</p>