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细菌组蛋白样 HU 蛋白的功能进化。

Functional evolution of bacterial histone-like HU proteins.

机构信息

Department of Biological Sciences, Louisiana State University, Baton Rouge, LA 70803, USA.

出版信息

Curr Issues Mol Biol. 2011;13(1):1-12. Epub 2010 May 20.

PMID:20484776
Abstract

Bacterial histone-like HU proteins are critical to maintenance of the nucleoid structure. In addition, they participate in all DNA-dependent functions, including replication, repair, recombination and gene regulation. In these capacities, their function is typically architectural, inducing a specific DNA topology that promotes assembly of higher-order nucleo-protein structures. Although HU proteins are highly conserved, individual homologs have been shown to exhibit a wide range of different DNA binding specificities and affinities. The existence of such distinct specificities indicates functional evolution and predicts distinct in vivo roles. Emerging evidence suggests that HU proteins discriminate between DNA target sites based on intrinsic flexure, and that two primary features of protein binding contribute to target site selection: The extent to which protein-mediated DNA kinks are stabilized and a network of surface salt-bridges that modulate interaction between DNA flanking the kinks and the body of the protein. These features confer target site selection for a specific HU homolog, they suggest the ability of HU to induce different DNA structural deformations depending on substrate, and they explain the distinct binding properties characteristic of HU homologs. Further divergence is evidenced by the existence of HU homologs with an additional lysine-rich domain also found in eukaryotic histone H1.

摘要

细菌组蛋白样 HU 蛋白对于维持核基质结构至关重要。此外,它们还参与所有依赖 DNA 的功能,包括复制、修复、重组和基因调控。在这些功能中,它们的作用通常是结构的,诱导特定的 DNA 拓扑结构,促进更高阶核蛋白结构的组装。尽管 HU 蛋白高度保守,但已表明单个同源物具有广泛不同的 DNA 结合特异性和亲和力。这种独特特异性的存在表明功能进化,并预测了不同的体内作用。新出现的证据表明,HU 蛋白根据固有弯曲度来区分 DNA 靶位点,并且蛋白质结合的两个主要特征有助于靶位点选择:蛋白介导的 DNA 弯曲稳定的程度,以及调节弯曲侧翼和蛋白质主体之间相互作用的表面盐桥网络。这些特征赋予了特定 HU 同源物的靶位点选择能力,它们表明 HU 能够根据底物诱导不同的 DNA 结构变形,并解释了 HU 同源物特有的独特结合特性。进一步的分歧证据是存在具有额外赖氨酸丰富结构域的 HU 同源物,该结构域也存在于真核组蛋白 H1 中。

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