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利用网络拓扑结构从高通量实验数据中发现可靠的蛋白质相互作用。

Discovering reliable protein interactions from high-throughput experimental data using network topology.

作者信息

Chen Jin, Hsu Wynne, Lee Mong Li, Ng See-Kiong

机构信息

School of Computing, National University of Singapore, Singapore 119260, Singapore.

出版信息

Artif Intell Med. 2005 Sep-Oct;35(1-2):37-47. doi: 10.1016/j.artmed.2005.02.004.

Abstract

OBJECTIVE

Current protein-protein interaction (PPI) detection via high-throughput experimental methods, such as yeast-two-hybrid has been reported to be highly erroneous, leading to potentially costly spurious discoveries. This work introduces a novel measure called IRAP, i.e. "interaction reliability by alternative path", for assessing the reliability of protein interactions based on the underlying topology of the PPI network.

METHODS AND MATERIALS

A candidate PPI is considered to be reliable if it is involved in a closed loop in which the alternative path of interactions between the two interacting proteins is strong. We devise an algorithm called AlternativePathFinder to compute the IRAP value for each interaction in a complex PPI network. Validation of the IRAP as a measure for assessing the reliability of PPIs is performed with extensive experiments on yeast PPI data. All the data used in our experiments can be downloaded from our supplementary data web site at .

RESULTS

Results show consistently that IRAP measure is an effective way for discovering reliable PPIs in large datasets of error-prone experimentally-derived PPIs. Results also indicate that IRAP is better than IG2, and markedly better than the more simplistic IG1 measure.

CONCLUSION

Experimental results demonstrate that a global, system-wide approach-such as IRAP that considers the entire interaction network instead of merely local neighbors-is a much more promising approach for assessing the reliability of PPIs.

摘要

目的

据报道,目前通过高通量实验方法(如酵母双杂交)进行的蛋白质 - 蛋白质相互作用(PPI)检测存在高度错误,可能导致代价高昂的虚假发现。这项工作引入了一种名为IRAP的新方法,即“通过替代路径的相互作用可靠性”,用于基于PPI网络的潜在拓扑结构评估蛋白质相互作用的可靠性。

方法和材料

如果候选PPI参与一个闭环,且两个相互作用蛋白质之间的替代相互作用路径很强,则认为该候选PPI是可靠的。我们设计了一种名为AlternativePathFinder的算法,用于计算复杂PPI网络中每个相互作用的IRAP值。通过对酵母PPI数据进行广泛实验,对IRAP作为评估PPI可靠性的一种方法进行了验证。我们实验中使用的所有数据都可以从我们的补充数据网站(.)下载。

结果

结果一致表明,IRAP方法是在容易出错的实验衍生PPI的大型数据集中发现可靠PPI的有效方法。结果还表明,IRAP优于IG2,并且明显优于更简单的IG1方法。

结论

实验结果表明,一种全局的、全系统的方法——如IRAP,它考虑整个相互作用网络而不仅仅是局部邻居——是评估PPI可靠性更有前景的方法。

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