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Directed Hungary Greedy Algorithm for Biomolecular Networks Alignment

机译:用于生物分子网络对齐的指导匈牙利贪婪算法

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There are many algorithms for conducting alignments between undirected biomolecular networks (UBNs), including protein-protein interaction networks (PINs). However, none of them are specialized for directed biomolecular networks (DBNs), such as gene regulatory networks (GRNs) and metabolic networks (MNs). It is challenging and meaningful to achieve optimal mapping in DBN alignment. In this article, we propose a new algorithm, referred to as Directed Hungary Greedy Algorithm (DHGA), for the alignment of DBNs. DHGA focuses on a directed graph and catches information on the direction of edges. Furthermore, both the homology of biomolecules and the similarities of the network topologies are taken into consideration. In DHGA, expert knowledge can be brought in to pre-match biomolecules. We verified the effectiveness and robustness of DHGA using simulation datasets. Our experiments demonstrate that the performance of DHGA is clearly improved when expert knowledge is introduced. Moreover, we conducted DHGA on two metabolic pathway maps from KEGG and identified 21 pairs of similar cell cycle regulatory relationships between human and yeast, 12 of which were supported by references indicating that the paired relationships have the same function.
机译:有许多用于在无向生物分子网络(UBNS)之间进行对准的算法,包括蛋白质 - 蛋白质相互作用网络(销)。然而,它们都不是专门用于指向的生物分子网络(DBN),例如基因调节网络(GRNS)和代谢网络(MNS)。在DBN对齐中实现最佳映射是具有挑战性和有意义的。在本文中,我们提出了一种新的算法,称为指示匈牙利贪婪算法(DHGA),用于对准DBN。 DHGA专注于定向图,并捕获有关边缘方向的信息。此外,考虑了生物分子的同源性和网络拓扑的相似性。在DHGA中,专业知识可以进入前匹配的生物分子。我们使用模拟数据集验证了DHGA的有效性和鲁棒性。我们的实验表明,当介绍专家知识时,DHGA的性能明显改善。此外,我们对来自Kegg的两种代谢途径图进行了DHGA,并确定了人和酵母之间的21对类似的细胞周期调节关系,其中12对指示配对关系具有相同功能的参考。

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