间接 DNA 读取由 H-NS 相关蛋白完成:Ler 的 C 末端结构域的 DNA 复合物结构。

Indirect DNA readout by an H-NS related protein: structure of the DNA complex of the C-terminal domain of Ler.

机构信息

Institute for Research in Biomedicine (IRB Barcelona), Parc Científic de Barcelona, Barcelona, Spain.

出版信息

PLoS Pathog. 2011 Nov;7(11):e1002380. doi: 10.1371/journal.ppat.1002380. Epub 2011 Nov 17.

Abstract

Ler, a member of the H-NS protein family, is the master regulator of the LEE pathogenicity island in virulent Escherichia coli strains. Here, we determined the structure of a complex between the DNA-binding domain of Ler (CT-Ler) and a 15-mer DNA duplex. CT-Ler recognizes a preexisting structural pattern in the DNA minor groove formed by two consecutive regions which are narrower and wider, respectively, compared with standard B-DNA. The compressed region, associated with an AT-tract, is sensed by the side chain of Arg90, whose mutation abolishes the capacity of Ler to bind DNA. The expanded groove allows the approach of the loop in which Arg90 is located. This is the first report of an experimental structure of a DNA complex that includes a protein belonging to the H-NS family. The indirect readout mechanism not only explains the capacity of H-NS and other H-NS family members to modulate the expression of a large number of genes but also the origin of the specificity displayed by Ler. Our results point to a general mechanism by which horizontally acquired genes may be specifically recognized by members of the H-NS family.

摘要

Ler 是 H-NS 蛋白家族的一员,是毒力大肠杆菌菌株中 LEE 致病岛的主要调节因子。在这里,我们确定了 Ler 的 DNA 结合域(CT-Ler)与 15 个碱基对 DNA 双链复合物的结构。CT-Ler 识别 DNA 小沟中预先存在的结构模式,该结构由两个连续的区域形成,与标准 B-DNA 相比,这两个区域分别更窄和更宽。与 AT 序列相关的压缩区域由 Arg90 的侧链感知,其突变会使 Ler 失去与 DNA 结合的能力。扩展的沟槽允许 Arg90 所在的环接近。这是第一个报告包括属于 H-NS 家族的蛋白质的 DNA 复合物的实验结构的报告。间接读出机制不仅解释了 H-NS 和其他 H-NS 家族成员能够调节大量基因表达的能力,还解释了 Ler 表现出特异性的原因。我们的研究结果指出了一种普遍的机制,通过该机制,水平获得的基因可能被 H-NS 家族的成员特异性识别。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d006/3219716/5f048a9974e6/ppat.1002380.g001.jpg

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