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Structural Insights into the Role of Architectural Proteins in DNA Looping Deduced from Computer Simulations

机译:从计算机模拟推断结构蛋白在DNA循环中的作用的结构见解

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摘要

Bacterial gene expression is regulated by DNA elements that often lie far apart along the genomic sequence but come close together during genetic processing. The intervening residues form loops, which are organized by the binding of various proteins. For example, the Escherichia coli Lac repressor protein binds DNA operators, separated by 92 or 401 base pairs, and suppresses the formation of gene products involved in the metabolism of lactose. The system also includes several highly abundant architectural proteins, such as the histone-like (heat unstable) HU protein, which severely deform the double helix upon binding. In order to gain a better understanding of how the naturally stiff DNA double helix forms the short loops detected in vivo, we have developed new computational methods to study the effects of various non-specifically binding proteins on the three-dimensional configurational properties of DNA sequences. This article surveys the approach that we use to generate ensembles of spatially constrained protein-decorated DNA structures (minicircles and Lac repressor-mediated loops) and presents some of the insights gained from the correspondence between computation and experiment about the potential contributions of architectural and regulatory proteins to DNA looping and gene expression.
机译:细菌基因的表达受到DNA元件的调节,这些DNA元件通常沿着基因组序列距离很远,但在基因加工过程中却彼此靠近。中间残基形成环,其通过各种蛋白质的结合而组织。例如,大肠杆菌Lac阻遏蛋白结合被92或401个碱基对分隔的DNA操纵子,并抑制涉及乳糖代谢的基因产物的形成。该系统还包括几种高度丰富的建筑蛋白,例如组蛋白样(热不稳定)HU蛋白,它们在结合后会严重变形双螺旋。为了更好地了解天然刚性DNA双螺旋如何形成体内检测到的短环,我们开发了新的计算方法来研究各种非特异性结合蛋白对DNA序列三维构型特性的影响。本文调查了我们用于生成空间受限的蛋白质修饰的DNA结构(微型圆和Lac阻遏物介导的环)集合的方法,并提供了从计算和实验之间的对应关系中获得的一些见解,涉及建筑和调控的潜在贡献蛋白质使DNA循环和基因表达。

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