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来自嗜热嗜酸泉古菌嗜热栖热菌P2的类Lrp DNA结合蛋白Ss-Lrp的高分辨率接触探测。

High resolution contact probing of the Lrp-like DNA-binding protein Ss-Lrp from the hyperthermoacidophilic crenarchaeote Sulfolobus solfataricus P2.

作者信息

Enoru-Eta Julius, Gigot Daniel, Glansdorff Nicolas, Charlier Daniel

机构信息

Erfelijkheidsleer en Microbiologie, Vrije Universiteit Brussels, Belgium.

出版信息

Mol Microbiol. 2002 Sep;45(6):1541-55. doi: 10.1046/j.1365-2958.2002.03136.x.

Abstract

Ss-Lrp, from Sulfolobus solfataricus, is an archaeal homologue of the global bacterial regulator Lrp (Leucine-responsive regulatory protein), which out of all genome-encoded proteins is most similar to Escherichia coli Lrp (E-value of 5.6 e-14). The recombinant protein has been purified as a 68 kDa homotetramer. The specific binding of Ss-Lrp to its own control region is suggestive of negative autoregulation. A high resolution contact map of Ss-Lrp binding was established by DNase I and hydroxyl radical footprinting, small non-intercalating groove-specific ligand-binding interference, and various base-specific premodification and base removal binding interference techniques. We show that Ss-Lrp binds one face of the DNA helix and establishes the most salient contacts with two major groove segments and the intervening minor groove, in a region that overlaps the TATA-box and BRE promoter elements. Therefore, Ss-Lrp most likely exerts autoregulation by preventing promoter recognition by TBP and TFB. Moreover, the results demonstrate profound Ss-Lrp induced structural alterations of sequence stretches flanking the core contact site, and reveal that the deformability of these regions significantly contributes to binding selectivity.

摘要

来自嗜热栖热菌的Ss-Lrp是全球细菌调节因子Lrp(亮氨酸响应调节蛋白)的古菌同源物,在所有基因组编码蛋白中,它与大肠杆菌Lrp最为相似(E值为5.6×10^-14)。重组蛋白已被纯化成为一种68 kDa的同四聚体。Ss-Lrp与其自身调控区域的特异性结合表明存在负向自调控。通过DNase I和羟基自由基足迹法、小的非嵌入型沟槽特异性配体结合干扰以及各种碱基特异性预修饰和碱基去除结合干扰技术,建立了Ss-Lrp结合的高分辨率接触图谱。我们发现Ss-Lrp结合在DNA螺旋的一个面上,并在与TATA盒和BRE启动子元件重叠的区域,与两个大沟段和中间的小沟建立了最显著的接触。因此,Ss-Lrp很可能通过阻止TBP和TFB识别启动子来发挥自调控作用。此外,结果表明Ss-Lrp诱导了核心接触位点侧翼序列片段的深刻结构改变,并揭示这些区域的可变形性对结合选择性有显著贡献。

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