Department of Biological Chemistry and Molecular Pharmacology, Harvard Medical School, Boston, MA, USA.
Department of Cancer Biology, Department of Oncologic Pathology, Blais Proteomics Center, Dana-Farber Cancer Institute, Boston, MA, USA.
Nat Chem Biol. 2020 Mar;16(3):318-326. doi: 10.1038/s41589-020-0467-3. Epub 2020 Feb 10.
Bile salt hydrolase (BSH) enzymes are widely expressed by human gut bacteria and catalyze the gateway reaction leading to secondary bile acid formation. Bile acids regulate key metabolic and immune processes by binding to host receptors. There is an unmet need for a potent tool to inhibit BSHs across all gut bacteria to study the effects of bile acids on host physiology. Here, we report the development of a covalent pan-inhibitor of gut bacterial BSHs. From a rationally designed candidate library, we identified a lead compound bearing an alpha-fluoromethyl ketone warhead that modifies BSH at the catalytic cysteine residue. This inhibitor abolished BSH activity in conventional mouse feces. Mice gavaged with a single dose of this compound displayed decreased BSH activity and decreased deconjugated bile acid levels in feces. Our studies demonstrate the potential of a covalent BSH inhibitor to modulate bile acid composition in vivo.
胆盐水解酶(BSH)广泛存在于人类肠道细菌中,并催化通向次级胆汁酸形成的关键反应。胆汁酸通过与宿主受体结合来调节关键的代谢和免疫过程。目前迫切需要一种有效的工具来抑制所有肠道细菌中的 BSH,以研究胆汁酸对宿主生理学的影响。在这里,我们报告了一种共价的肠道细菌 BSH 泛抑制剂的开发。从一个合理设计的候选文库中,我们鉴定出一种先导化合物,其带有α-氟甲基酮弹头,可修饰 BSH 的催化半胱氨酸残基。这种抑制剂可消除常规小鼠粪便中的 BSH 活性。单次给予该化合物的小鼠显示 BSH 活性降低,粪便中去结合胆汁酸水平降低。我们的研究证明了共价 BSH 抑制剂在体内调节胆汁酸组成的潜力。
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