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工程调控级联和网络控制链霉菌抗生素生物合成。

Engineering of regulatory cascades and networks controlling antibiotic biosynthesis in Streptomyces.

机构信息

Area de Microbiología, Department of Molecular Biology, University of León, León, Spain.

出版信息

Curr Opin Microbiol. 2010 Jun;13(3):263-73. doi: 10.1016/j.mib.2010.02.008. Epub 2010 Mar 19.

Abstract

Engineering of regulatory mechanisms that control the biosynthesis of bioactive secondary metabolites is an approach to increase the production of valuable fermentation products. Two types of regulatory mechanisms have been studied in Streptomyces species: (1) pyramidal cascades of regulation that usually involve a butyrolactone and its receptor protein triggering the formation of pathway-associated regulatory proteins (SARP), and (2) global regulators that transduce protein phosphorylation signals responding to stress factors. Global regulators are frequently two-component systems; for example, the PhoR-PhoP system, the AsbA1-AsbA2, the orphan response regulator GlnR and the STAND-family regulator AfsR. Several strategies have been used to obtain overproducer strains, including: (i) obtention of phosphate-deregulated mutants by alteration of phoP, (ii) amplification and/or overexpression of pathway-associated positive regulators, and (iii) modification of butyrolactone receptor proteins. The success of these strategies is hampered by the poor knowledge of interactions between regulatory mechanisms.

摘要

工程调控机制,控制生物活性次生代谢物的生物合成是一种增加有价值的发酵产品的生产方法。两种类型的调控机制已经在链霉菌属中进行了研究:(1)调节的金字塔式级联,通常涉及丁内酯及其受体蛋白触发途径相关调节蛋白(SARP)的形成,和(2)全球调节蛋白,其转导对胁迫因子做出响应的蛋白质磷酸化信号。全局调节剂通常是双组分系统;例如,PhoR-PhoP 系统、AsbA1-AsbA2、孤儿响应调节剂 GlnR 和 STAND 家族调节剂 AfsR。已经使用了几种策略来获得高产菌株,包括:(i)通过改变 phoP 获得磷酸盐调节突变体,(ii)扩增和/或过表达途径相关的正调节因子,和(iii)丁内酯受体蛋白的修饰。这些策略的成功受到调控机制之间相互作用的知识匮乏的阻碍。

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