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结核菌脂酰基辅酶 A 脱氢酶的全细胞活性抑制剂通过紧密结合相互作用提供对人酶的选择性。

Whole Cell Active Inhibitors of Mycobacterial Lipoamide Dehydrogenase Afford Selectivity over the Human Enzyme through Tight Binding Interactions.

机构信息

Tri-Institutional Therapeutics Discovery Institute, New York, New York 10065, United States.

Structural Biology Program, Sloan Kettering Institute, New York, New York 10065, United States.

出版信息

ACS Infect Dis. 2021 Feb 12;7(2):435-444. doi: 10.1021/acsinfecdis.0c00788. Epub 2021 Feb 2.

Abstract

Tuberculosis remains a leading cause of death from a single bacterial infection worldwide. Efforts to develop new treatment options call for expansion into an unexplored target space to expand the drug pipeline and bypass resistance to current antibiotics. Lipoamide dehydrogenase is a metabolic and antioxidant enzyme critical for mycobacterial growth and survival in mice. Sulfonamide analogs were previously identified as potent and selective inhibitors of mycobacterial lipoamide dehydrogenase but lacked activity against whole mycobacteria. Here we present the development of analogs with improved permeability, potency, and selectivity, which inhibit the growth of in axenic culture on carbohydrates and within mouse primary macrophages. They increase intrabacterial pyruvate levels, supporting their on-target activity within mycobacteria. Distinct modalities of binding between the mycobacterial and human enzymes contribute to improved potency and hence selectivity through induced-fit tight binding interactions within the mycobacterial but not human enzyme, as indicated by kinetic analysis and crystallography.

摘要

结核病仍然是全球范围内由单一细菌感染导致的主要死亡原因。为了开发新的治疗方法,我们需要开拓一个尚未开发的目标领域,以扩大药物研发管线并规避现有抗生素耐药性的问题。脂酰脱氢酶是一种代谢和抗氧化酶,对于分枝杆菌在小鼠中的生长和存活至关重要。磺胺类似物先前被鉴定为分枝杆菌脂酰脱氢酶的有效且选择性抑制剂,但对完整分枝杆菌缺乏活性。在这里,我们提出了具有改善的通透性、效力和选择性的类似物的开发,这些类似物可抑制在碳水化合物中以及在小鼠原代巨噬细胞内的纯培养物中的生长。它们增加了细菌内丙酮酸的水平,支持其在分枝杆菌内的靶标活性。分枝杆菌和人酶之间的结合模式的差异通过在分枝杆菌而不是人酶内的诱导契合紧密结合相互作用导致了效力的提高,从而提高了选择性,这一点通过动力学分析和晶体学得到了证实。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0aa4/7888283/f9c79e0ee48c/id0c00788_0001.jpg

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