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Fast Hinge Detection Algorithms for Flexible Protein Structures

机译:灵活的蛋白质结构的快速铰链检测算法

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Analysis of conformational changes is one of the keys to the understanding of protein functions and interactions. For the analysis, we often compare two protein structures, taking flexible regions like hinge regions into consideration. The Root Mean Square Deviation (RMSD) is the most popular measure for comparing two protein structures, but it is only for rigid structures without hinge regions. In this paper, we propose a new measure called RMSD considering hinges (RMSDh) and its variant {rm RMSDh}^{(k)} for comparing two flexible proteins with hinge regions. We also propose novel efficient algorithms for computing them, which can detect the hinge positions at the same time. The RMSDh is suitable for cases where there is one small hinge region in each of the two target structures. The new algorithm for computing the RMSDh runs in linear time, which is the same as the time complexity for computing the RMSD and is faster than any of previous algorithms for hinge detection. The {rm RMSDh}^{(k)} is designed for comparing structures with more than one hinge region. The {rm RMSDh}^{(k)} measure considers at most k small hinge region, i.e., the {rm RMSDh}^{(k)} value should be small if the two structures are similar except for at most k hinge regions. To compute the value, we propose an O(kn^{2})-time and O(n)-space algorithm based on a new dynamic programming technique. With the same computational time and space, we can enumerate the predicted hinge positions. We also test our algorithms against actual flexible protein structures, and show that the hinge positions can be correctly detected by our algorithms.
机译:构象变化的分析是理解蛋白质功能和相互作用的关键之一。为了进行分析,我们经常比较两种蛋白质结构,并考虑诸如铰链区之类的柔性区域。均方根偏差(RMSD)是比较两种蛋白质结构的最受欢迎方法,但仅适用于没有铰链区的刚性结构。在本文中,我们提出了一种新方法,即考虑铰链的RMSD(RMSDh)及其变体{rm RMSDh} ^ {(k)},用于比较具有铰链区的两种柔性蛋白质。我们还提出了用于计算它们的新颖有效算法,该算法可以同时检测铰链位置。 RMSDh适用于两个目标结构中每个都有一个小的铰链区域的情况。计算RMSDh的新算法以线性时间运行,这与计算RMSD的时间复杂度相同,并且比任何以前的铰链检测算法都快。 {rm RMSDh} ^ {(k)}设计用于比较具有多个铰链区域的结构。 {rm RMSDh} ^ {(k)}度量考虑最多k个小铰链区域,即,如果两个结构相似(除了最多k个铰链区域),则{rm RMSDh} ^ {(k)}值应较小。 。为了计算该值,我们提出了一种基于新的动态编程技术的O(kn ^ {2})时间和O(n)空间算法。在相同的计算时间和空间下,我们可以枚举预测的铰链位置。我们还针对实际的柔性蛋白质结构测试了我们的算法,并表明铰链位置可以通过我们的算法正确检测。

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