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在大肠杆菌中,6-磷酸葡糖胺合酶GlmS表达的反馈控制依赖于小RNA GlmZ,并涉及新型蛋白质YhbJ。

Feedback control of glucosamine-6-phosphate synthase GlmS expression depends on the small RNA GlmZ and involves the novel protein YhbJ in Escherichia coli.

作者信息

Kalamorz Falk, Reichenbach Birte, März Walter, Rak Bodo, Görke Boris

机构信息

Department of General Microbiology, Institute of Microbiology and Genetics, Georg-August University, Grisebachstrasse 8, D-37077 Göttingen, Germany.

出版信息

Mol Microbiol. 2007 Sep;65(6):1518-33. doi: 10.1111/j.1365-2958.2007.05888.x.

DOI:10.1111/j.1365-2958.2007.05888.x
PMID:17824929
Abstract

Amino sugars are essential precursor molecules for the biosynthesis of bacterial cell walls. Their synthesis pathway is initiated by glucosamine-6-phosphate (GlcN-6-P) synthase (GlmS) which catalyses the rate limiting reaction. We report here that expression of the Escherichia coli glmS gene is negatively feedback regulated by its product GlcN-6-P at the post-transcriptional level. Initially, we observed that mutants defective for yhbJ, a gene of the rpoN operon, overproduce GlmS. Concomitantly, a glmS mRNA accumulates that is derived from processing of the primary glmUS transcript at the glmU stop codon by RNase E. A transposon mutagenesis screen in the yhbJ mutant identified the small RNA GlmZ (formerly RyiA or SraJ) to be required for glmS mRNA accumulation. GlmZ, which is normally processed, accumulates in its full-length form in the yhbJ mutant. In the wild type, a decrease of the intracellular GlcN-6-P concentration induces accumulation of the glmS transcript in a GlmZ-dependent manner. Concomitantly, GlmZ accumulates in its unprocessed form. Hence, we conclude that the biological function of GlmZ is to positively control the glmS mRNA in response to GlcN-6-P concentrations and that YhbJ negatively regulates GlmZ. As in yhbJ mutants GlcN-6-P has no effect, YhbJ is essential for sensing this metabolite.

摘要

氨基糖是细菌细胞壁生物合成的必需前体分子。它们的合成途径由氨基葡萄糖-6-磷酸(GlcN-6-P)合酶(GlmS)启动,该酶催化限速反应。我们在此报告,大肠杆菌glmS基因的表达在转录后水平受到其产物GlcN-6-P的负反馈调节。最初,我们观察到rpoN操纵子的一个基因yhbJ缺陷的突变体过量产生GlmS。同时,积累了一种glmS mRNA,它是由RNase E在glmU终止密码子处对初级glmUS转录本进行加工而产生的。在yhbJ突变体中进行的转座子诱变筛选确定小RNA GlmZ(以前称为RyiA或SraJ)是glmS mRNA积累所必需的。通常被加工的GlmZ在yhbJ突变体中以全长形式积累。在野生型中,细胞内GlcN-6-P浓度的降低以GlmZ依赖的方式诱导glmS转录本的积累。同时,GlmZ以未加工的形式积累。因此,我们得出结论,GlmZ的生物学功能是响应GlcN-6-P浓度对glmS mRNA进行正向调控,而YhbJ对GlmZ进行负向调控。由于在yhbJ突变体中GlcN-6-P没有作用,YhbJ对于感知这种代谢物至关重要。

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