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Alignment of Flexible Protein Structures

机译:柔性蛋白质结构的对准

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摘要

We present two algorithms which align flexible protein structures. Both apply efficient structural pattern detection and graph theoretic techniques. The FlexProt algorithm simultaneously detects the hinge regions and aligns the rigid subparts of the molecules. It does it by efficiently detecting maximal congruent rigid fragments in both molecules and calculating their optimal arrangement which does not violate the protein sequence order. The FlexMol algorithm is sequence order independent, yet requires as input the hypothesized hinge positions. Due its sequence order independence it can also be applied to protein-protein interface matching and drug molecule alignment. It aligns the rigid parts of the molecule using the Geometric Hashing method and calculates optimal connectivity among these parts by graph-theoretic techniques. Both algorithms are highly efficient even compared with rigid structure alignment algorithms. Typical running times on a standard desktop PC (400MHz) are about 7 seconds for FlexProt and about 1 minute for FlexMol.
机译:我们提出了两种对准柔性蛋白质结构的算法。两者都采用高效的结构模式检测和图形理论技术。 FlexProT算法同时检测铰链区域并对准分子的刚性子部分。通过有效地检测两个分子中的最大一致性刚性片段并计算其最佳布置,并计算不违反蛋白质序列顺序的最佳布置。 FlexMol算法是独立的序列顺序,但需要输入假设的铰链位置。由于其顺序独立性,它也可以应用于蛋白质 - 蛋白质界面匹配和药物分子取向。它使用几何散列方法对准分子的刚性部分,并通过图形理论技术计算这些部件之间的最佳连接。即使与刚性结构对准算法相比,这两种算法也高效。标准台式电脑(400MHz)上的典型运行时间约为FlexProT约为7秒,柔性胶片约为1分钟。

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