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Ss-LrpB是嗜热栖热菌P2中一种新型的类似Lrp的调控因子,它与其自身调控区域内的三个保守靶点协同结合。

Ss-LrpB, a novel Lrp-like regulator of Sulfolobus solfataricus P2, binds cooperatively to three conserved targets in its own control region.

作者信息

Peeters Eveline, Thia-Toong Thia-Lin, Gigot Daniel, Maes Dominique, Charlier Daniel

机构信息

Erfelijkheidsleer en Microbiologie, Vrije Universiteit Brussel, Pleinlaan 2, B-1050 Brussels, Belgium.

出版信息

Mol Microbiol. 2004 Oct;54(2):321-36. doi: 10.1111/j.1365-2958.2004.04274.x.

DOI:10.1111/j.1365-2958.2004.04274.x
PMID:15469506
Abstract

Ss-LrpB, a novel Lrp-like DNA-binding protein from the hyperthermophilic crenarchaeon Sulfolobus solfataricus, was shown to bind cooperatively to three regularly spaced targets in its own control region, with as consensus the 15 bp palindrome 5'-TTGYAW WWWWTRCAA-3'. Binding to the border sites occurred with high affinity; the target in the middle proved to be a low affinity site which is stably bound only when both flanking sites are occupied. Ss-LrpB contacts two major groove segments and the intervening minor groove of each site, all aligned on one face of the helix. The operator shows intrinsic bending and is increasingly deformed upon binding of Ss-LrpB to one, two and three targets. Complex formation relies therefore on DNA conformability, protein-DNA and protein-protein contacts. Mobility-shift assays and in gel footprinting indicate that Ss-LrpB and the transcription factors TATA-box binding protein (TBP) and transcription factor B (TFB) can bind simultaneously to the control region. Based on these findings we present a model for the construction of the higher order nucleoprotein complexes and a hypothesis for the autoregulatory process. The latter is based on the concentration-dependent formation of distinct complexes exhibiting different stoichiometries and conformations, which could positively and negatively affect promoter activity.

摘要

Ss-LrpB是一种来自嗜热泉古菌硫磺硫化叶菌的新型类Lrp DNA结合蛋白,已证明它能与其自身调控区域内三个规则间隔的靶标协同结合,共有序列为15bp的回文序列5'-TTGYAW WWWWTRCAA-3'。与边界位点的结合具有高亲和力;中间的靶标被证明是一个低亲和力位点,只有当两侧的位点都被占据时才会稳定结合。Ss-LrpB与每个位点的两个大沟片段及中间的小沟接触,所有这些都排列在螺旋的同一面上。操纵子具有内在的弯曲,并且在Ss-LrpB与一个、两个和三个靶标结合时会越来越变形。因此,复合物的形成依赖于DNA的适应性、蛋白质-DNA和蛋白质-蛋白质接触。迁移率变动分析和凝胶足迹法表明,Ss-LrpB与转录因子TATA框结合蛋白(TBP)和转录因子B(TFB)可以同时结合到调控区域。基于这些发现,我们提出了一个高阶核蛋白复合物构建模型和一个自动调节过程的假说。后者基于浓度依赖性形成具有不同化学计量和构象的不同复合物,这可能对启动子活性产生正向和负向影响。

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