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首页> 外文期刊>Nucleic Acids Research >Indirect readout in drug-DNA recognition: role of sequence-dependent DNA conformation.
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Indirect readout in drug-DNA recognition: role of sequence-dependent DNA conformation.

机译:药物DNA识别中的间接读数:序列依赖性DNA构象的作用。

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DNA-binding drugs have numerous applications in the engineered gene regulation. However, the drug-DNA recognition mechanism is poorly understood. Drugs can recognize specific DNA sequences not only through direct contacts but also indirectly through sequence-dependent conformation, in a similar manner to the indirect readout mechanism in protein-DNA recognition. We used a knowledge-based technique that takes advantage of known DNA structures to evaluate the conformational energies. We built a dataset of non-redundant free B-DNA crystal structures to calculate the distributions of adjacent base-step and base-pair conformations, and estimated the effective harmonic potentials of mean force (PMF). These PMFs were used to calculate the conformational energy of drug-DNA complexes, and the Z-score as a measure of the binding specificity. Comparing the Z-scores for drug-DNA complexes with those for free DNA structures with the same sequence, we observed that in several cases the Z-scores became more negative upon drug binding. Furthermore, the specificity is position-dependent within the drug-bound region of DNA. These results suggest that DNA conformation plays an important role in the drug-DNA recognition. The presented method provides a tool for the analysis of drug-DNA recognition and can facilitate the development of drugs for targeting a specific DNA sequence.
机译:DNA结合药物在基因工程调控中有许多应用。但是,药物-DNA识别机制了解甚少。药物不仅可以通过直接接触来识别特定的DNA序列,而且可以通过序列依赖性构象来间接识别特定的DNA序列,其方式类似于蛋白质-DNA识别中的间接读出机制。我们使用了一种基于知识的技术,该技术利用已知的DNA结构来评估构象能量。我们建立了一个非冗余的自由B-DNA晶体结构数据集,以计算相邻基步和碱基对构象的分布,并估算了平均力(PMF)的有效谐波电位。这些PMF用于计算药物-DNA复合物的构象能,Z分数用于衡量结合特异性。比较具有相同序列的药物-DNA复合物的Z分数与游离DNA结构的Z分数,我们观察到在某些情况下,药物结合后Z分数变得更加阴性。此外,特异性在DNA的药物结合区域内是位置依赖性的。这些结果表明,DNA构象在药物-DNA识别中起重要作用。所提出的方法提供了用于分析药物-DNA识别的工具,并且可以促进针对特定DNA序列的药物的开发。

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