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通过蛋白质寻找其DNA靶位点:1. DNA构象对蛋白质滑动的影响。

Search by proteins for their DNA target site: 1. The effect of DNA conformation on protein sliding.

作者信息

Bhattacherjee Arnab, Levy Yaakov

机构信息

Department of Structural Biology, Weizmann Institute of Science, Rehovot 76100, Israel.

Department of Structural Biology, Weizmann Institute of Science, Rehovot 76100, Israel

出版信息

Nucleic Acids Res. 2014 Nov 10;42(20):12404-14. doi: 10.1093/nar/gku932. Epub 2014 Oct 16.

Abstract

The recognition of DNA-binding proteins (DBPs) to their specific site often precedes by a search technique in which proteins slide, hop along the DNA contour or perform inter-segment transfer and 3D diffusion to dissociate and re-associate to distant DNA sites. In this study, we demonstrated that the strength and nature of the non-specific electrostatic interactions, which govern the search dynamics of DBPs, are strongly correlated with the conformation of the DNA. We tuned two structural parameters, namely curvature and the extent of helical twisting in circular DNA. These two factors are mutually independent of each other and can modulate the electrostatic potential through changing the geometry of the circular DNA conformation. The search dynamics for DBPs on circular DNA is therefore markedly different compared with linear B-DNA. Our results suggest that, for a given DBP, the rotation-coupled sliding dynamics is precluded in highly curved DNA (as well as for over-twisted DNA) because of the large electrostatic energy barrier between the inside and outside of the DNA molecule. Under such circumstances, proteins prefer to hop in order to explore interior DNA sites. The change in the balance between sliding and hopping propensities as a function of DNA curvature or twisting may result in different search efficiency and speed.

摘要

DNA结合蛋白(DBP)对其特定位点的识别通常先经过一种搜索技术,在该技术中,蛋白质沿着DNA轮廓滑动、跳跃,或进行片段间转移以及三维扩散,以解离并重新结合到远处的DNA位点。在本研究中,我们证明了控制DBP搜索动力学的非特异性静电相互作用的强度和性质与DNA的构象密切相关。我们调整了两个结构参数,即环状DNA的曲率和螺旋扭曲程度。这两个因素相互独立,并且可以通过改变环状DNA构象的几何形状来调节静电势。因此,与线性B-DNA相比,DBP在环状DNA上的搜索动力学明显不同。我们的结果表明,对于给定的DBP,由于DNA分子内外存在较大的静电能垒,在高度弯曲的DNA(以及过度扭曲的DNA)中,旋转耦合滑动动力学受到阻碍。在这种情况下,蛋白质更倾向于跳跃以探索DNA内部位点。滑动和跳跃倾向之间的平衡随DNA曲率或扭曲的变化可能导致不同的搜索效率和速度。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bbec/4227778/88f865f18ac9/gku932fig1.jpg

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