孕烷X受体
核受体
药理学
受体
炎症
配体(生物化学)
异型生物质的
化学
药品
消炎药
医学
生物化学
基因
酶
内科学
转录因子
作者
Xiaojuan Wang,Guohui Zhang,Zhiwei Bian,Vimanda Chow,Marina Grimaldi,Coralie Carivenc,Savannah Sirounian,Hao Li,Lucia Sládeková,Stefano Motta,Yulia Luperi,Yufeng Gong,Cait M. Costello,Linhao Li,Matthew Jachimowicz,Miao Guo,Shian Hu,Derek J. Wilson,Patrick Balaguer,William Bourguet
标识
DOI:10.1038/s41467-025-56624-0
摘要
The literature documenting the value of drug-like molecules found in natural products is vast. Although many dietary and herbal remedies have been found to be effective for treating intestinal inflammation, the identification of their active components has lagged behind. In this study, we find that a major ginger component, furanodienone (FDN), is a selective pregnane X receptor (PXR) ligand with agonistic transcriptional outcomes. We show that FDN binds within a sub-pocket of the PXR ligand binding domain (LBD), with subsequent alterations in LBD structure. Using male mice, we show that orally provided FDN has potent PXR-dependant anti-inflammatory outcomes that are colon-specific. Increased affinity and target gene activation in the presence of synergistically acting agonists indicates further opportunities for augmenting FDN activity, efficacy and safety. Collectively, these results support the translational potential of FDN as a therapeutic agent for the treatment and prevention of colonic diseases. Here the authors discover that furanodienone (FDN), a small molecule derived from ginger, exhibits PXR agonist activity selective for the intestine and show that when FDN is administered orally in pharmacological doses ameliorates induced colitis in male mice.
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