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非核糖体肽合成酶合成β-内酰胺时酰基供体的严格性和去氢氨酰中间产物。

Acyl Donor Stringency and Dehydroaminoacyl Intermediates in β-Lactam Formation by a Non-ribosomal Peptide Synthetase.

机构信息

Department of Chemistry, Johns Hopkins University, Baltimore, Maryland 21218, United States.

出版信息

ACS Chem Biol. 2021 May 21;16(5):806-812. doi: 10.1021/acschembio.1c00117. Epub 2021 Apr 13.

Abstract

Condensation (C) domains in non-ribosomal peptide synthetases catalyze peptide elongation steps whereby activated amino acid or peptidyl acyl donors are coupled with specific amino acid acceptors. In the biosynthesis of the β-lactam antibiotic nocardicin A, an unusual C domain converts a seryl tetrapeptide into its pentapeptide product containing an integrated β-lactam ring. While indirect evidence for the intermediacy of a dehydroalanyl species has been reported, here we describe observation of the elusive enzyme-bound dehydroamino acyl intermediate generated from the corresponding -threonyl tetrapeptide and partitioned into pentapeptide products containing either a dehydrobutyrine residue or an embedded β-lactam. Contrary to trends in the literature where condensation domains have been deemed flexible as to acyl donor structure, this β-lactam synthesizing domain is highly discriminating. The observation of dehydrobutyrine formation links this C domain to related clades associated with natural products containing dehydroamino acid and d-configured residues, suggesting a common mechanistic link.

摘要

非核糖体肽合成酶中的 C 结构域催化肽延伸步骤,其中激活的氨基酸或肽酰基供体与特定的氨基酸受体结合。在β-内酰胺抗生素诺卡菌素 A 的生物合成中,一个不寻常的 C 结构域将丝氨酰四肽转化为含有整合β-内酰胺环的五肽产物。虽然已经报道了脱氢丙氨酰物种中间体的间接证据,但在这里我们描述了从相应的苏氨酰四肽生成的难以捉摸的酶结合的脱氢氨基酰中间产物的观察结果,并将其分配到含有脱氢丁酰基残基或嵌入β-内酰胺的五肽产物中。与文献中认为缩合结构域对酰基供体结构具有柔韧性的趋势相反,这个β-内酰胺合成结构域具有高度的选择性。脱氢丁酰基形成的观察结果将这个 C 结构域与与含有脱氢氨基酸和 d-构型残基的天然产物相关的相关分支联系起来,表明存在共同的机制联系。

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