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第20章. 玫瑰孢链霉菌中脂肽的生物合成与基因工程

Chapter 20. Biosynthesis and genetic engineering of lipopeptides in Streptomyces roseosporus.

作者信息

Baltz Richard H

机构信息

Cubist Pharmaceuticals Inc, Lexington, Massachusetts, USA.

出版信息

Methods Enzymol. 2009;458:511-31. doi: 10.1016/S0076-6879(09)04820-4.

Abstract

Daptomycin is an acidic cyclic lipopeptide antibiotic approved for treatment of infections caused by Gram-positive pathogens, including Staphylococcus aureus strains resistant to other antibiotics. Daptomycin biosynthesis is carried out by a giant multisubunit, multienzyme nonribosomal peptide synthetase (NRPS). The daptomycin (dpt) biosynthetic genes have been cloned in a bacterial artificial chromosome (BAC) vector, sequenced, and expressed in Streptomyces lividans. Several of the dpt genes, including the three NRPS genes, are transcribed as a lengthy polycistronic message. The daptomycin-producing strain, Streptomyces roseosporus, can be genetically manipulated, and a number of deletion mutants encompassing one or more of the dpt genes have been constructed. Several of the dpt genes have been expressed from ectopic chromosomal loci (varphiC31 or IS117 attB sites) under the transcriptional control of the strong constitutive ermEp* promoter, and recombinant strains produced high levels of lipopeptides, thus establishing a trans-complementation system for combinatorial biosynthesis. A number of hybrid NRPS subunits have been generated by lambda-Red-mediated recombination, and combinatorial libraries of lipopeptides have been generated by NRPS subunit exchanges, module exchanges, multidomain exchanges, deletion mutagenesis, and multiple natural lipidations, using the ectopic trans-complementation system in S. roseosporus.

摘要

达托霉素是一种酸性环状脂肽抗生素,被批准用于治疗由革兰氏阳性病原体引起的感染,包括对其他抗生素耐药的金黄色葡萄球菌菌株。达托霉素的生物合成由一种巨大的多亚基、多酶非核糖体肽合成酶(NRPS)进行。达托霉素(dpt)生物合成基因已被克隆到细菌人工染色体(BAC)载体中,进行了测序,并在变铅青链霉菌中表达。包括三个NRPS基因在内的几个dpt基因被转录为一条长的多顺反子信息。产生达托霉素的菌株玫瑰孢链霉菌可以进行基因操作,并且已经构建了许多包含一个或多个dpt基因的缺失突变体。几个dpt基因已在强组成型ermEp*启动子的转录控制下从异位染色体位点(φC31或IS117 attB位点)表达,重组菌株产生了高水平的脂肽,从而建立了用于组合生物合成的反式互补系统。通过λ-Red介导的重组产生了许多杂合NRPS亚基,并利用玫瑰孢链霉菌中的异位反式互补系统,通过NRPS亚基交换、模块交换、多结构域交换、缺失诱变和多种天然脂化作用,产生了脂肽组合文库。

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