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Site-Specific Structural Constraints on Protein Sequence Evolutionary Divergence: Local Packing Density versus Solvent Exposure

机译:蛋白质序列进化差异的位点特异性结构限制:局部堆积密度与溶剂暴露

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摘要

Protein sequences evolve under selection pressures imposed by functional and biophysical requirements, resulting in site-dependent rates of amino acid substitution. Relative solvent accessibility (RSA) and local packing density (LPD) have emerged as the best candidates to quantify structural constraint. Recent research assumes that RSA is the main determinant of sequence divergence. However, it is not yet clear which is the best predictor of substitution rates. To address this issue, we compared RSA and LPD with site-specific rates of evolution for a diverse data set of enzymes. In contrast with recent studies, we found that LPD measures correlate better than RSA with evolutionary rate. Moreover, the independent contribution of RSA is minor. Taking into account that LPD is related to backbone flexibility, we put forward the possibility that the rate of evolution of a site is determined by the ease with which the backbone deforms to accommodate mutations.
机译:蛋白质序列在功能和生物物理要求施加的选择压力下进化,导致氨基酸取代的位点依赖性速率。相对溶剂可及性 (RSA) 和局部堆积密度 (LPD) 已成为量化结构约束的最佳候选者。最近的研究假设RSA是序列分歧的主要决定因素。然而,目前尚不清楚哪个是替代率的最佳预测指标。为了解决这个问题,我们将RSA和LPD与不同酶数据集的位点特异性进化速率进行了比较。与最近的研究相比,我们发现LPD测量比RSA与进化率的相关性更好。此外,RSA的独立贡献很小。考虑到LPD与骨架灵活性有关,我们提出了一种可能性,即一个位点的进化速度取决于骨架变形以适应突变的难易程度。

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