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首页> 外文期刊>ChemMedChem >Discovery of a Histidine-Based Scaffold as an Inhibitor of Gut Microbial Choline Trimethylamine-Lyase
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Discovery of a Histidine-Based Scaffold as an Inhibitor of Gut Microbial Choline Trimethylamine-Lyase

机译:发现基于组氨酸的支架作为肠道微生物胆碱三甲胺 - 裂解酶的抑制剂

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摘要

Anaerobic choline metabolism by human gut microbiota to produce trimethylamine (TMA) has recently evolved as a potential therapeutic target because of its association with chronic kidney disease and increased cardiovascular risks. Limited examples of choline analogues have been reported as inhibitors of bacterial enzyme choline TMA-lyase (CutC), a key enzyme regulating choline anaerobic metabolism. We used a new workflow to discover CutC inhibitors based on focused screening of a diversified library of small molecules for intestinal metabolic stability followed by in vitro CutC inhibitory assay. This workflow identified a histidine-based scaffold as a CutC inhibitor with an IC_(50) value of 1.9±0.2 μM. Remarkably, the identified CutC inhibitor was able to reduce the production of TMA in whole-cell assays using various bacterial strains as well as in complex gut microbiota environment. The improved efficiency of the new scaffold identified in this study in comparison to previously reported CutC inhibitors would enable optimization of potential leads for in vivo screening and clinical translation. Finally, docking studies and moleculardynamic simulations were used to predict putative interactions created between inhibitor and CutC.
机译:由于其与慢性肾病和心血管风险增加,人体肠道微生物通过人体肠道微生物产生三甲胺(TMA)的厌氧胆碱代谢最近被演变为潜在的治疗目标。有限的胆碱类似物的实例已被报告为细菌酶胆碱TMA-Lyase(COFC)的抑制剂,一种关键酶调节胆碱厌氧代谢。我们使用了新的工作流程,以发现基于针对肠道代谢稳定性的小分子的多样化文库的聚焦筛选的COFC抑制剂,然后进行体外CUTC抑制测定。该工作流鉴定为基于组氨酸的支架作为COFC抑制剂,IC_(50)值为1.9±0.2μm。值得注意的是,所识别的CODC抑制剂能够使用各种细菌菌株以及复杂的肠道微生物菌环境来减少全细胞测定中TMA的产生。与先前报道的CUDC抑制剂相比,该研究中鉴定的新支架的提高效率将能够优化体内筛选和临床翻译的潜在铅。最后,使用对接研究和分子动力学模拟来预测抑制剂和CUTC之间产生的推定相互作用。

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