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局灶性异质性疾病基因编码的蛋白质在人类蛋白质相互作用网络中具有高度的互联性。

Locus heterogeneity disease genes encode proteins with high interconnectivity in the human protein interaction network.

机构信息

Faculty of Life Sciences, University of Manchester Manchester, UK.

出版信息

Front Genet. 2014 Dec 9;5:434. doi: 10.3389/fgene.2014.00434. eCollection 2014.

Abstract

Mutations in genes potentially lead to a number of genetic diseases with differing severity. These disease genes have been the focus of research in recent years showing that the disease gene population as a whole is not homogeneous, and can be categorized according to their interactions. Locus heterogeneity describes a single disorder caused by mutations in different genes each acting individually to cause the same disease. Using datasets of experimentally derived human disease genes and protein interactions, we created a protein interaction network to investigate the relationships between the products of genes associated with a disease displaying locus heterogeneity, and use network parameters to suggest properties that distinguish these disease genes from the overall disease gene population. Through the manual curation of known causative genes of 100 diseases displaying locus heterogeneity and 397 single-gene Mendelian disorders, we use network parameters to show that our locus heterogeneity network displays distinct properties from the global disease network and a Mendelian network. Using the global human proteome, through random simulation of the network we show that heterogeneous genes display significant interconnectivity. Further topological analysis of this network revealed clustering of locus heterogeneity genes that cause identical disorders, indicating that these disease genes are involved in similar biological processes. We then use this information to suggest additional genes that may contribute to diseases with locus heterogeneity.

摘要

基因突变可能导致多种严重程度不同的遗传疾病。近年来的研究重点是这些疾病基因,表明疾病基因群体并非同质的,可以根据它们的相互作用进行分类。基因座异质性描述了一种由单个基因的突变引起的单一疾病,这些突变各自独立地导致相同的疾病。我们使用实验衍生的人类疾病基因和蛋白质相互作用数据集创建了一个蛋白质相互作用网络,以研究与表现出基因座异质性的疾病相关的基因产物之间的关系,并使用网络参数来提示区分这些疾病基因与整体疾病基因群体的特性。通过对 100 种表现出基因座异质性的疾病和 397 种单基因孟德尔疾病的已知致病基因的手动注释,我们使用网络参数表明,我们的基因座异质性网络与全球疾病网络和孟德尔网络具有不同的特性。通过对全球人类蛋白质组的随机模拟,我们通过网络显示出不均匀基因具有显著的相互连接性。对该网络的进一步拓扑分析揭示了导致相同疾病的基因座异质性基因的聚类,表明这些疾病基因参与了相似的生物过程。然后,我们利用这些信息来推测可能导致基因座异质性疾病的其他基因。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/497d/4260505/556fb55454cf/fgene-05-00434-g001.jpg

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