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多个结合位点和效应器独立结合对枯草芽孢杆菌 CodY 介导的调控的贡献。

Contributions of multiple binding sites and effector-independent binding to CodY-mediated regulation in Bacillus subtilis.

机构信息

Department of Molecular Biology and Microbiology, Tufts University School of Medicine, Boston, MA 02111, USA.

出版信息

J Bacteriol. 2011 Jan;193(2):473-84. doi: 10.1128/JB.01151-10. Epub 2010 Nov 19.

Abstract

CodY is a branched-chain amino acid-responsive transcriptional regulator that controls, directly or indirectly, the expression of more than 100 genes and operons in Bacillus subtilis. Using DNase I footprinting and gel-shift experiments, we identified two CodY-binding regions upstream of a B. subtilis gene (bcaP, previously known as yhdG) that encodes a transporter of branched-chain amino acids. Mutational analysis revealed that both CodY-binding regions contribute to repression in vivo and do so independently of each other. Thus, a single CodY-binding site is apparently sufficient for substantial CodY-dependent regulation. By analyzing affinities of wild-type and mutant CodY-binding sites for CodY and their regulation by wild-type CodY and forms of CodY with various levels of activation by branched-chain amino acids, we concluded that unliganded CodY cannot repress transcription in vivo and that the level of endogenously produced effectors is sufficient for CodY-mediated regulation of promoters with stronger sites. Because the sites with higher affinity apparently respond to lower concentrations of CodY effectors and saturate faster as the concentrations of effectors increase, having two sites of binding with different affinities for CodY permits a promoter to respond to a wider range of intracellular concentrations of effectors.

摘要

CodY 是一种支链氨基酸反应性转录调节因子,它直接或间接地控制枯草芽孢杆菌中超过 100 个基因和操纵子的表达。通过使用 DNase I 足迹实验和凝胶迁移实验,我们在枯草芽孢杆菌基因(bcaP,以前称为 yhdG)的上游鉴定了两个 CodY 结合区域,该基因编码支链氨基酸的转运蛋白。突变分析表明,两个 CodY 结合区域都有助于体内的抑制作用,并且彼此独立地起作用。因此,单个 CodY 结合位点显然足以进行大量的 CodY 依赖性调节。通过分析野生型和突变型 CodY 结合位点与 CodY 的亲和力及其受野生型 CodY 和各种支链氨基酸激活水平的 CodY 形式的调节,我们得出结论,未结合的 CodY 不能在体内抑制转录,并且内源性产生的效应物的水平足以对具有更强结合位点的启动子进行 CodY 介导的调节。由于具有更高亲和力的结合位点显然可以响应更低浓度的 CodY 效应物,并且随着效应物浓度的增加更快地达到饱和,因此具有两个具有不同 CodY 亲和力的结合位点可以使启动子响应更广泛的细胞内效应物浓度范围。

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