朝着更好地测量蛋白质3D模型质量的方向发展

A. Poleksic
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引用次数: 0

摘要

蛋白质三维结构预测的进展很大程度上依赖于测量蛋白质模型质量的能力。模型质量的最佳单一度量之一是所谓的“GDT函数”图下的面积,该函数将模型结构中可在距离≤θ处与实验结构中相应残数叠加的残数百分比分配给每个距离截止点θ。代替一种方法能够计算这一措施,研究人员往往诉诸其近似GDTTS。在这篇短文中,我们提出了第一个理论框架,用于开发一种算法,该算法能够在多项式时间内计算蛋白质模型GDT曲线下面积的近最优估计。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Towards a better measure of protein 3D model quality
Advances in protein three-dimensional structure prediction depend strongly on the ability to measure the quality of a protein model. One of the best single measures of the model quality is the area under the graph of the so-called “GDT function” that assigns to each distance cutoff θ the percentage of residues in the model structure that can be superimposed at distance ≤ θ from the corresponding residues in the experimental structure. In lieu of a method capable of computing this measure, researchers often resort to its approximation GDTTS. In this short paper we present the first theoretical framework for the development of an algorithm capable of computing near-optimal estimates of the area under the GDT curve of a protein model in polynomial time.
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