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古菌中的新蛋白质-DNA 复合物:一种小单体蛋白质诱导形成尖锐 V 形转折 DNA 结构。

New protein-DNA complexes in archaea: a small monomeric protein induces a sharp V-turn DNA structure.

机构信息

Centre de Biophysique Moléculaire, Centre National de la Recherche Scientifique UPR 4301, rue Charles Sadron, F-45071, Orléans, Cedex 2, France.

UFR Collegium Sciences et Techniques, Université d'Orléans, rue de Chartres, 45100, Orléans, France.

出版信息

Sci Rep. 2019 Oct 3;9(1):14253. doi: 10.1038/s41598-019-50211-2.

Abstract

MC1, a monomeric nucleoid-associated protein (NAP), is structurally unrelated to other DNA-binding proteins. The protein participates in the genome organization of several Euryarchaea species through an atypical compaction mechanism. It is also involved in DNA transcription and cellular division through unknown mechanisms. We determined the 3D solution structure of a new DNA-protein complex formed by MC1 and a strongly distorted 15 base pairs DNA. While the protein just needs to adapt its conformation slightly, the DNA undergoes a dramatic curvature (the first two bend angles of 55° and 70°, respectively) and an impressive torsional stress (dihedral angle of 106°) due to several kinks upon binding of MC1 to its concave side. Thus, it adopts a V-turn structure. For longer DNAs, MC1 stabilizes multiple V-turn conformations in a flexible and dynamic manner. The existence of such V-turn conformations of the MC1-DNA complexes leads us to propose two binding modes of the protein, as a bender (primary binding mode) and as a wrapper (secondary binding mode). Moreover, it opens up new opportunities for studying and understanding the repair, replication and transcription molecular machineries of Archaea.

摘要

MC1 是一种单体核小体相关蛋白(NAP),与其他 DNA 结合蛋白在结构上没有关系。该蛋白通过一种非典型的压缩机制参与了几种古菌物种的基因组组织。它还通过未知的机制参与了 DNA 转录和细胞分裂。我们确定了由 MC1 和一个强烈扭曲的 15 个碱基对 DNA 形成的新的 DNA-蛋白质复合物的三维溶液结构。虽然该蛋白只需稍微改变其构象,但由于 MC1 与其凹面结合时发生了几个扭曲,DNA 会发生剧烈的弯曲(前两个弯曲角度分别为 55°和 70°)和令人印象深刻的扭转应力(二面角为 106°)。因此,它采用 V 型转弯结构。对于较长的 DNA,MC1 以灵活和动态的方式稳定多个 V 型转弯构象。MC1-DNA 复合物中存在这种 V 型转弯构象,使我们提出了该蛋白的两种结合模式,即弯曲(主要结合模式)和包裹(次要结合模式)。此外,它为研究和理解古菌的修复、复制和转录分子机制开辟了新的机会。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/aa36/6776556/d38c7b39cf18/41598_2019_50211_Fig1_HTML.jpg

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