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离散弗雷歇距离下的蛋白质局部结构比对。

Protein local structure alignment under the discrete Fréchet distance.

作者信息

Zhu Binhai

机构信息

Department of Computer Science, Montana State University, Bozeman, MT 59717, USA.

出版信息

J Comput Biol. 2007 Dec;14(10):1343-51. doi: 10.1089/cmb.2007.0156.

Abstract

Protein structure alignment is a fundamental problem in computational and structural biology. While there has been lots of experimental/heuristic methods and empirical results, very few results are known regarding the algorithmic/complexity aspects of the problem, especially on protein local structure alignment. A well-known measure to characterize the similarity of two polygonal chains is the famous Fréchet distance, and with the application of protein-related research, a related discrete Fréchet distance has been used recently. In this paper, following the recent work of Jiang et al. we investigate the protein local structural alignment problem using bounded discrete Fréchet distance. Given m proteins (or protein backbones, which are 3D polygonal chains), each of length O(n), our main results are summarized as follows: * If the number of proteins, m, is not part of the input, then the problem is NP-complete; moreover, under bounded discrete Fréchet distance it is NP-hard to approximate the maximum size common local structure within a factor of n(1-epsilon). These results hold both when all the proteins are static and when translation/rotation are allowed. * If the number of proteins, m, is a constant, then there is a polynomial time solution for the problem.

摘要

蛋白质结构比对是计算生物学和结构生物学中的一个基本问题。虽然已经有许多实验性/启发式方法和实证结果,但关于该问题的算法/复杂性方面,尤其是蛋白质局部结构比对方面,所知结果甚少。一种用于表征两条多边形链相似性的著名度量是著名的弗雷歇距离,随着蛋白质相关研究的应用,一种相关的离散弗雷歇距离最近也被使用。在本文中,继Jiang等人最近的工作之后,我们使用有界离散弗雷歇距离研究蛋白质局部结构比对问题。给定m个蛋白质(或蛋白质骨架,它们是三维多边形链),每个长度为O(n),我们的主要结果总结如下:* 如果蛋白质的数量m不是输入的一部分,那么该问题是NP完全问题;此外,在有界离散弗雷歇距离下,将最大尺寸公共局部结构近似到n(1 - ε)的因子内是NP难的。当所有蛋白质都是静态的以及允许平移/旋转时,这些结果都成立。* 如果蛋白质的数量m是一个常数,那么该问题有一个多项式时间解。

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