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来自变形菌门的套索肽:利用异源表达和质谱的基因组挖掘

Lasso peptides from proteobacteria: Genome mining employing heterologous expression and mass spectrometry.

作者信息

Hegemann Julian D, Zimmermann Marcel, Zhu Shaozhou, Klug Dennis, Marahiel Mohamed A

机构信息

Department of Chemistry, Philipps-University Marburg, Hans-Meerwein-Strasse 4 and LOEWE-Center for Synthetic Microbiology, Marburg, D-35032, Germany.

出版信息

Biopolymers. 2013 Sep;100(5):527-42. doi: 10.1002/bip.22326.

DOI:10.1002/bip.22326
PMID:23897438
Abstract

Lasso peptides are natural products with a unique three dimensional structure resembling a lariat knot. They are from ribosomal origin and are post-translationally modified by two enzymes (B and C), one of which shares little similarity to enzymes outside of lasso peptide biosynthetic gene clusters and as such is a useful target for genome mining. In this study, we demonstrate a B protein-centric genome mining approach through which we were able to identify 102 putative lasso peptide biosynthetic gene clusters from a total of 87 different proteobacterial strains. Ten of these clusters were cloned into the pET41a expression vector, optimized through incorporation of a ribosomal binding site and heterologously expressed in Escherichia coli BL21(DE3). All 12 predicted lasso peptides (namely burhizin, caulonodin I, caulonodin II, caulonodin III, rhodanodin, rubrivinodin, sphingonodin I, sphingonodin II, syanodin I, sphingopyxin I, sphingopyxin II, and zucinodin) were detected by high-resolution Fourier transform mass spectrometry and their proposed primary structure was confirmed through tandem mass spectrometry. High yields (ranging from 0.4 to 5.2 mg/L) were observable for eight of these compounds, while thermostability assays revealed five new representatives of heat labile lasso peptides.

摘要

套索肽是一类天然产物,具有独特的三维结构,形似套索结。它们起源于核糖体,由两种酶(B和C)进行翻译后修饰,其中一种酶与套索肽生物合成基因簇之外的酶几乎没有相似性,因此是基因组挖掘的一个有用靶点。在本研究中,我们展示了一种以B蛋白为中心的基因组挖掘方法,通过该方法我们能够从总共87种不同的变形杆菌菌株中鉴定出102个假定的套索肽生物合成基因簇。其中10个基因簇被克隆到pET41a表达载体中,通过引入核糖体结合位点进行优化,并在大肠杆菌BL21(DE3)中进行异源表达。通过高分辨率傅里叶变换质谱法检测到了所有12种预测的套索肽(即burhizin、caulonodin I、caulonodin II、caulonodin III、rhodanodin、rubrivinodin、sphingonodin I、sphingonodin II、syanodin I、sphingopyxin I、sphingopyxin II和zucinodin),并通过串联质谱法确认了它们的一级结构。其中8种化合物的产量较高(范围为0.4至5.2 mg/L),而热稳定性分析揭示了5种新的热不稳定套索肽代表。

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