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人肠道微生物群代谢对G蛋白偶联受体靶向药物活性的影响。

Activity of GPCR-targeted drugs influenced by human gut microbiota metabolism.

作者信息

Wu Qihao, Song Deguang, Zhao Yanyu, Verdegaal Andrew A, Turocy Tayah, Duncan-Lowey Brianna, Goodman Andrew L, Palm Noah W, Crawford Jason M

机构信息

Department of Chemistry, Yale University, New Haven, CT, USA.

Institute of Biomolecular Design and Discovery, Yale University, West Haven, CT, USA.

出版信息

Nat Chem. 2025 Apr 3. doi: 10.1038/s41557-025-01789-w.

Abstract

Microbiota-mediated drug metabolism can affect pharmacological efficacy. Here we conducted a systematic comparative metabolomics investigation of drug metabolism modes by evaluating the impacts of human gut commensal bacteria on 127 G-protein-coupled receptor (GPCR)-targeted drugs. For the most extensively metabolized drugs in our screen, we elucidated both conventional and unconventional drug transformations and the corresponding activities of generated metabolites. Comparisons of drug metabolism by a gut microbial community versus individual species revealed both taxon intrinsic and collaborative processes that influenced the activity of the metabolized drugs against target GPCRs. We also observed iloperidone inactivation by generating unconventional metabolites. The human gut commensal bacteria mixture incorporated sulfur in the form of a thiophene motif, whereas Morganella morganii used a cascade reaction to incorporate amino-acid-derived tricyclic systems into the drug metabolites. Our results reveal a broad impact of human gut commensal bacteria on GPCR-targeted drug structures and activities through diverse microbiota-mediated biotransformations.

摘要

微生物群介导的药物代谢会影响药理疗效。在此,我们通过评估人类肠道共生细菌对127种G蛋白偶联受体(GPCR)靶向药物的影响,对药物代谢模式进行了系统的比较代谢组学研究。对于我们筛选中代谢最广泛的药物,我们阐明了传统和非传统的药物转化以及生成代谢物的相应活性。肠道微生物群落与单个物种的药物代谢比较揭示了影响代谢药物对靶标GPCR活性的分类群内在和协同过程。我们还观察到通过生成非传统代谢物使伊潘立酮失活。人类肠道共生细菌混合物以噻吩基序的形式掺入硫,而摩根氏摩根菌则利用级联反应将氨基酸衍生的三环系统掺入药物代谢物中。我们的结果揭示了人类肠道共生细菌通过多种微生物群介导的生物转化对GPCR靶向药物结构和活性产生的广泛影响。

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