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林可霉素和克林霉素的构象。由TRNOE核糖体结合构象确定的大环内酯类、酮内酯类和林可酰胺类共有的一个片段。

Lincomycin and clindamycin conformations. A fragment shared by macrolides, ketolides and lincosamides determined from TRNOE ribosome-bound conformations.

作者信息

Verdier L, Bertho G, Gharbi-Benarous J, Girault J P

机构信息

Université René Descartes-Paris V, Laboratoire de Chimie et Biochimie Pharmacologiques et Toxicologiques (UMR 8601 CNRS), France.

出版信息

Bioorg Med Chem. 2000 Jun;8(6):1225-43. doi: 10.1016/s0968-0896(00)00081-x.

Abstract

Two important lincosamide antibiotics, lincomycin and clindamycin were studied in the complex state with the bacterial ribosome after a conformational analysis by 1H and 13C NMR spectroscopy and molecular modelling of the unbound molecules. Lincosamide-ribosome interactions were investigated using two-dimensional transferred nuclear Overhauser effect spectroscopy (TRNOESY), resulting in a bound structure compatible with the experimental NMR data. The results compared with the conformational analysis of the substrates in solution indicate that specific conformations are preferred in the bound state. Clindamycin, the more bioactive antibiotic studied, displayed a stronger NMR response than lincomycin showing that in lincosamide-ribosome interactions, a low affinity binding level is associated to the tight binding one and is related to biological activity. This study shows that conformation plays an essential role for the low affinity binding site. Superimposition of lincosamide, macrolide and ketolide bound structures exhibited conformational similarities in a particular fragment which is in agreement with a hypothesis of partial overlapping lincosamide and macrolide binding sites.

摘要

在通过¹H和¹³C NMR光谱对未结合分子进行构象分析以及分子建模后,研究了两种重要的林可酰胺类抗生素——林可霉素和克林霉素与细菌核糖体的复合物状态。使用二维转移核Overhauser效应光谱(TRNOESY)研究林可酰胺 - 核糖体相互作用,得到了与实验NMR数据相符的结合结构。与溶液中底物的构象分析结果相比,表明在结合状态下特定构象更受青睐。所研究的生物活性更强的抗生素克林霉素比林可霉素表现出更强的NMR响应,这表明在林可酰胺 - 核糖体相互作用中,低亲和力结合水平与紧密结合水平相关,并且与生物活性有关。这项研究表明构象对低亲和力结合位点起着至关重要的作用。林可酰胺、大环内酯和酮内酯结合结构的叠加在一个特定片段中表现出构象相似性,这与林可酰胺和大环内酯结合位点部分重叠的假设一致。

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