Inference of Disease E3s from Integrated Functional Relation Network

Bumki Min, G. Yi
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引用次数: 1

Abstract

Recently, the potential of E3 ligase as a therapeutic target is increasing. The systematic method to derive disease-related E3s can provide significant contribution for this demand. Several disease gene prediction methods have been introduced but it is hard to find E3 ligase-specific information from them. We have developed a unique approach to prioritize the disease relation of E3 by integrating E3-substrate relations and their neighboring network with known disease genes. The potential of our method is demonstrated by showing better performance against the previous methods to predict known disease relations of E3. We could discover 101 E3s and their functional network having 1,285 relations with diseases. Our method will provide new promising chances in drug target discovery field as well as disease mechanism study.
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基于综合功能关系网络的疾病e3推断
近年来,E3连接酶作为治疗靶点的潜力越来越大。系统地推导疾病相关e3的方法可以为这一需求提供重要贡献。目前已有几种疾病基因预测方法,但很难从中找到E3连接酶特异性信息。我们开发了一种独特的方法,通过将E3-底物关系及其邻近网络与已知的疾病基因整合,来优先考虑E3的疾病关系。与之前的方法相比,我们的方法在预测已知E3疾病关系方面表现出更好的性能,证明了我们的方法的潜力。我们可以发现101个E3s及其功能网络与疾病有1285个关系。该方法将为药物靶点发现和疾病机制研究提供新的前景。
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