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非核糖体肽酶促装配线的结构见解

Structural insights into nonribosomal peptide enzymatic assembly lines.

作者信息

Koglin Alexander, Walsh Christopher T

机构信息

Department of Biological Chemistry & Molecular Pharmacology, Harvard Medical School, Boston, MA 02115, USA.

出版信息

Nat Prod Rep. 2009 Aug;26(8):987-1000. doi: 10.1039/b904543k. Epub 2009 May 22.

Abstract

Nonribosomal peptides have a variety of medicinal activities including activity as antibiotics, antitumor drugs, immunosuppressives, and toxins. Their biosynthesis on multimodular assembly lines as a series of covalently tethered thioesters, in turn covalently attached on pantetheinyl arms on carrier protein way stations, reflects similar chemical logic and protein machinery to fatty acid and polyketide biosynthesis. While structural information on excised or isolated catalytic adenylation (A), condensation (C), peptidyl carrier protein (PCP) and thioesterase (TE) domains had been gathered over the past decade, little was known about how the NRPS catalytic and carrier domains interact with each other both within and across elongation or termination modules. This Highlight reviews recent breakthrough achievements in both X-ray and NMR spectroscopic studies that illuminate the architecture of NRPS PCP domains, PCP-containing didomain-fragments and of a full termination module (C-A-PCP-TE).

摘要

非核糖体肽具有多种药用活性,包括作为抗生素、抗肿瘤药物、免疫抑制剂和毒素的活性。它们在多模块装配线上生物合成,形成一系列共价连接的硫酯,这些硫酯又以共价方式连接在载体蛋白中途站的泛酰巯基乙胺臂上,这反映出与脂肪酸和聚酮生物合成相似的化学逻辑和蛋白质机制。尽管在过去十年中已经收集了关于切除或分离的催化腺苷化(A)、缩合(C)、肽基载体蛋白(PCP)和硫酯酶(TE)结构域的结构信息,但对于非核糖体肽合成酶(NRPS)催化结构域和载体结构域在延伸或终止模块内以及跨模块如何相互作用却知之甚少。本综述重点介绍了X射线和核磁共振光谱研究方面的最新突破性成果,这些成果阐明了NRPS的PCP结构域、含PCP的双结构域片段以及完整终止模块(C-A-PCP-TE)的结构。

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Structural insights into nonribosomal peptide enzymatic assembly lines.非核糖体肽酶促装配线的结构见解
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