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海绵共生菌 MB037 中 III 类硫肽的异源表达及其与 Labionin 偶联交叉连接的特性分析。

Heterologous Expression Facilitates the Production and Characterization of a Class III Lanthipeptide with Coupled Labionin Cross-Links in Sponge-Associated MB037.

机构信息

Marine Biotechnology Laboratory, State Key Laboratory of Microbial Metabolism and School of Life Sciences and Biotechnology, Shanghai Jiao Tong University, Shanghai 200240, China.

Yazhou Bay Institute of Deepsea Science and Technology, Shanghai Jiao Tong University, Shanghai 200240, P.R. China.

出版信息

ACS Chem Biol. 2024 Sep 20;19(9):2060-2069. doi: 10.1021/acschembio.4c00428. Epub 2024 Aug 15.

DOI:10.1021/acschembio.4c00428
PMID:39145437
Abstract

Cyclic peptides, with remarkable stability, cellular permeability, and proteolysis resistance, display promising potential in pharmaceutical applications. Labionin (Lab), a unique bicyclic cross-link containing both C-C and C-S bonds, provides high rigidity and better control of conformation compared to monocyclic cross-links. To discover more Lab-containing scaffolds with highly rigid conformation for cyclic peptide drug development, herein, a cryptic class III lanthipeptide biosynthetic gene cluster (BGC) (i.e., ) was identified in the sponge-associated MB037 and expressed in , incorporating an N-terminal SUMO-tag on the RcsA precursor peptide to prevent proteolysis. Subsequently, a novel class III lanthipeptide, i.e., rochsin A, exhibiting a highly rigid conformation with coupled Lab cross-links crowded by bulky aromatic amino acids, was produced. Three AplP-like proteases outside the BGC were proven to remove the leader peptide of rochsin A through their dual endo- and aminopeptidase activities, resulting in mature rochsin A . Ala mutation experiments revealed the C to N cyclization direction, like most class III lanthipeptides. However, RcsKC displays a high substrate breadth, enabling various ring topologies that are rarely observed in other class III lanthipeptides. Overall, the established expression system broadens the chemical diversity of cyclic peptides with unique Lab cross-links and offers a highly rigid scaffold for cyclic peptide drug development.

摘要

环肽具有显著的稳定性、细胞通透性和抗蛋白水解性,在药物应用方面显示出巨大的潜力。Labionin(Lab)是一种独特的双环交联物,含有 C-C 和 C-S 键,与单环交联物相比,它提供了更高的刚性和更好的构象控制。为了发现更多具有高度刚性构象的 Lab 含有支架用于环状肽药物开发,本文在海绵相关的 MB037 中鉴定了一个隐蔽的 III 类硫肽生物合成基因簇(BGC)(即 ),并在 中表达,在 RcsA 前体肽的 N 端添加 SUMO 标签以防止蛋白水解。随后,产生了一种新型的 III 类硫肽,即 Rochsin A,其具有高度刚性的构象,带有耦合的 Lab 交联,被大的芳香族氨基酸拥挤。证明 BGC 外的三个 AplP 样蛋白酶通过其双重内切和氨肽酶活性去除 Rochsin A 的前导肽,生成成熟的 Rochsin A。Ala 突变实验揭示了 C 到 N 的环化方向,与大多数 III 类硫肽一样。然而,RcsKC 表现出较高的底物广谱性,能够实现各种在其他 III 类硫肽中很少观察到的环拓扑结构。总的来说,建立的表达系统拓宽了具有独特 Lab 交联的环状肽的化学多样性,并为环状肽药物开发提供了一个高度刚性的支架。

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