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Lagrangian Relaxation Applied to Sparse Global Network Alignment

机译:拉格朗日放松适用于稀疏的全球网络对齐

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Data on molecular interactions is increasing at a tremendous pace, while the development of solid methods for analyzing this network data is lagging behind. This holds in particular for the field of comparative network analysis, where one wants to identify commonalities between biological networks. Since biological functionality primarily operates at the network level, there is a clear need for topology-aware comparison methods. In this paper we present a method for global network alignment that is fast and robust, and can flexibly deal with various scoring schemes taking both node-to-node correspondences as well as network topologies into account. It is based on an integer linear programming formulation, generalizing the well-studied quadratic assignment problem. We obtain strong upper and lower bounds for the problem by improving a Lagrangian relaxation approach and introduce the software tool NATALIE 2.0, a publicly available implementation of our method. In an extensive computational study on protein interaction networks for six different species, we find that our new method outperforms alternative state-of-the-art methods with respect to quality and running time. An extended version of this paper including proofs and pseudo code is available at http://arxiv.org/pdf/1108.4358v1.
机译:关于分子相互作用的数据以巨大的速度越来越大,而用于分析该网络数据的固体方法的开发是滞后的。这尤其适用于比较网络分析领域,其中人们想要识别生物网络之间的共性。由于生物功能主要在网络级别运行,因此有一种清楚地需要拓扑感知的比较方法。在本文中,我们介绍了一种快速且稳健的全局网络对齐方法,并且可以灵活地处理以节点到节点对应关系的各种评分方案以及对帐户的网络拓扑。它基于整数线性编程配方,概括了研究良好的二次分配问题。通过改善拉格朗日放松方法,介绍了软件工具Natalie 2.0,获得了强大的上下范围,并介绍了我们的方法。在六种不同物种的蛋白质相互作用网络的广泛计算研究中,我们发现我们的新方法始于质量和运行时间的替代现有方法。本文的扩展版本包括证据和伪代码可在http://arxiv.org/pdf/1108.4358v1上获得。

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