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CRP在复杂acs启动子处的多种作用取决于激活区域2和整合宿主因子(IHF)。

The multiple roles of CRP at the complex acs promoter depend on activation region 2 and IHF.

作者信息

Sclavi Bianca, Beatty Christine M, Thach David S, Fredericks Christine E, Buckle Malcolm, Wolfe Alan J

机构信息

LBPA, UMR8113, CNRS/Ecole Normale Supérieure de Cachan, 94230 Cachan, France.

出版信息

Mol Microbiol. 2007 Jul;65(2):425-40. doi: 10.1111/j.1365-2958.2007.05797.x.

DOI:10.1111/j.1365-2958.2007.05797.x
PMID:17630973
Abstract

acs encodes a high-affinity enzyme that permits survival during carbon starvation. As befits a survival gene, its transcription is subject to complex regulation. Previously, we reported that cAMP receptor protein (CRP) activates acs transcription by binding tandem DNA sites located upstream of the major acsP2 promoter and that the nucleoid protein IHF (integration host factor) binds three specific sites located just upstream. In vivo, the sequence that includes these IHF sites exerts a positive effect on CRP-dependent transcription, while a construct containing only the most proximal site exhibits reduced transcription compared with the full-length promoter or with a construct lacking all three IHF sites. Here, we defined the minimal system required for this IHF-dependent inhibition, showing it requires the promoter-distal CRP site and an amino acid residue located within activation region 2 (AR2), a surface determinant of CRP that interacts with RNA polymerase (RNAP). Surprisingly, for a Class III promoter, disruption of AR2 caused significant changes in the activity and structure of both the full-length promoter and the construct with the single proximal IHF site. We propose that AR2, together with IHF, mediates formation of a multi-protein complex, in which RNAP is stabilized in an open complex that remains poised on the promoter ready to respond rapidly to environmental changes.

摘要

acs编码一种高亲和力酶,使细胞在碳饥饿期间得以存活。作为一个生存基因,其转录受到复杂的调控。此前,我们报道过,环腺苷酸受体蛋白(CRP)通过结合位于主要acsP2启动子上游的串联DNA位点来激活acs转录,并且类核蛋白整合宿主因子(IHF)结合位于其上游的三个特定位点。在体内,包含这些IHF位点的序列对CRP依赖的转录产生正向影响,而与全长启动子或缺乏所有三个IHF位点的构建体相比,仅包含最近端位点的构建体转录水平降低。在此,我们确定了这种依赖于IHF的抑制作用所需的最小系统,表明它需要启动子远端的CRP位点以及位于激活区域2(AR2)内的一个氨基酸残基,AR2是CRP的一个表面决定簇,可与RNA聚合酶(RNAP)相互作用。令人惊讶的是,对于III类启动子,AR2的破坏会导致全长启动子和具有单个近端IHF位点的构建体的活性和结构发生显著变化。我们提出,AR2与IHF一起介导了一种多蛋白复合物的形成,其中RNAP在开放复合物中得到稳定,该复合物在启动子上保持就绪状态,随时准备对环境变化做出快速反应。

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