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A theoretical investigation of DNA dynamics and desolvation kinetics for zinc finger proteinZif268

机译:锌指蛋白的DNA动力学和去溶剂化动力学的理论研究

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摘要

BackgroundTranscription factors, regulating the expression inventory of a cell, interact with its respective DNA subjugated by a specific recognition pattern, which if well exploited may ensure targeted genome engineering. The mostly widely studied transcription factors are zinc finger proteins that bind to its target DNA via direct and indirect recognition levels at the interaction interface. Exploiting the binding specificity and affinity of the interaction between the zinc fingers and the respective DNA can help in generating engineered zinc fingers for therapeutic applications. Experimental evidences lucidly substantiate the effect of indirect interaction like DNA deformation and desolvation kinetics, in empowering ZFPs to accomplish partial sequence specificity functioning around structural properties of DNA. Exploring the structure-function relationships of the existing zinc finger-DNA complexes at the indirect recognition level can aid in predicting the probable zinc fingers that could bind to any target DNA. Deformation energy, which defines the energy required to bend DNA from its native shape to its shape when bound to the ZFP, is an effect of indirect recognition mechanism. Water is treated as a co-reactant for unfurling the affinity studies in ZFP-DNA binding equilibria that takes into account the unavoidable change in hydration that occurs when these two solvated surfaces come into contact.
机译:背景转录因子调节细胞的表达量,并通过特定的识别模式与各自的DNA相互作用,如果利用得当,可以确保靶向的基因组工程。研究最广泛的转录因子是锌指蛋白,它们通过相互作用界面上的直接和间接识别水平与靶DNA结合。利用锌指和相应DNA之间相互作用的结合特异性和亲和力可以帮助产生工程化的锌指以用于治疗应用。实验证据清楚地证实了间接相互作用(如DNA变形和去溶剂化动力学)的作用,使ZFP能够完成围绕DNA结构特性的部分序列特异性功能。在间接识别水平上探索现有锌指-DNA复合物的结构-功能关系可以帮助预测可能与任何靶DNA结合的锌指。变形能是间接识别机制的作用,它定义了将DNA从其原始形状弯曲到与ZFP结合时所需的能量。将水视为展开ZFP-DNA结合平衡中亲和力研究的共反应剂,考虑到这两个溶剂化表面接触时不可避免的水合变化。

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