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链霉菌中次生代谢和细胞分化的调控:A因子作为一种微生物激素,而AfsR蛋白作为双组分调控系统的一个组成部分。

Regulation of secondary metabolism and cell differentiation in Streptomyces: A-factor as a microbial hormone and the AfsR protein as a component of a two-component regulatory system.

作者信息

Horinouchi S, Beppu T

机构信息

Department of Agricultural Chemistry, University of Tokyo, Japan.

出版信息

Gene. 1992 Jun 15;115(1-2):167-72. doi: 10.1016/0378-1119(92)90555-4.

Abstract

A-factor is a microbial hormone that functions as a key switch for secondary metabolite formation and morphogenesis in Streptomyces griseus. Genetic and biochemical studies on the A-factor-binding protein have implied that the binding protein present in the cytoplasm plays a role in repressing streptomycin (Sm) production and sporulation while the binding of A-factor to the binding protein releases this repression. The A-factor signal is transferred, probably via some additional regulatory proteins in the A-factor-regulatory cascade, to the strR gene, a regulator for Sm biosynthesis. A positive regulatory protein binds about 430-330 bp upstream from the transcription start point of the strR promoter and activates its transcription. The StrR product, in turn, activates the other Sm-biosynthesis genes. A global regulatory gene, afsR, of Streptomyces coelicolor A3(2) encodes a 993-amino acid protein that is phosphorylated by a specific phosphokinase, AfsK, encoded by the region just upstream from the afsR gene. Site-directed mutagenesis of afsR has revealed that phosphorylated AfsR globally stimulates transcription of antibiotic-production genes. It is most likely that AfsR and AfsK compose a two-component regulatory system. Although AfsR shows no significant homology with typical regulators of the two-component systems in other prokaryotes, such as OmpR and PhoB of Escherichia coli, it shows considerable homology with regulatory proteins in antibiotic biosynthetic gene clusters of Streptomyces spp., such as actII ORF4, dnrR1 ORF1 and redD ORF1.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

A因子是一种微生物激素,在灰色链霉菌中作为次生代谢产物形成和形态发生的关键开关。对A因子结合蛋白的遗传和生化研究表明,存在于细胞质中的结合蛋白在抑制链霉素(Sm)产生和孢子形成中起作用,而A因子与结合蛋白的结合则解除这种抑制。A因子信号可能通过A因子调节级联中的一些其他调节蛋白传递到strR基因,strR基因是Sm生物合成的调节因子。一种正向调节蛋白结合在strR启动子转录起始点上游约430 - 330 bp处,并激活其转录。StrR产物进而激活其他Sm生物合成基因。天蓝色链霉菌A3(2)的一个全局调节基因afsR编码一种993个氨基酸的蛋白质,该蛋白质被afsR基因上游区域编码的特定磷酸激酶AfsK磷酸化。对afsR的定点诱变表明,磷酸化的AfsR全局刺激抗生素产生基因的转录。很可能AfsR和AfsK组成一个双组分调节系统。尽管AfsR与其他原核生物中双组分系统的典型调节因子(如大肠杆菌的OmpR和PhoB)没有显著同源性,但它与链霉菌属抗生素生物合成基因簇中的调节蛋白(如actII ORF4、dnrR1 ORF1和redD ORF1)有相当的同源性。(摘要截短于250字)

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