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基于RNA测序数据鉴定人类缺血性心肌病的潜在基因

Identification of potential genes for human ischemic cardiomyopathy based on RNA-Seq data.

作者信息

Li Wan, Li Liansheng, Zhang Shiying, Zhang Ce, Huang Hao, Li Yiran, Hu Erqiang, Deng Gui, Guo Shanshan, Wang Yahui, Li Weimin, Chen Lina

机构信息

College of Bioinformatics Science and Technology, Harbin Medical University, Harbin, Heilongjiang, China.

Department of internal medicine, Heilongjiang Commercial Hospital, Harbin, Heilongjiang, China.

出版信息

Oncotarget. 2016 Dec 13;7(50):82063-82073. doi: 10.18632/oncotarget.13331.

Abstract

Ischemic cardiomyopathy (ICM) is an important cause of heart failure, yet no ICM disease genes were stored in any public databases. Mutations of genes provided by RNA-Seq data could set a foundation for a variety of biological processes. This also made it possible to elucidate the mechanism and identify potential genes for ICM. In this paper, an integrated co-expression network was constructed using univariate and bivariate canonical correlation analysis for RNA-Seq data of human ICM samples. Three ICM-related modules were recognized after comparing between Pearson correlation coefficients of ICM samples and normal controls. Furthermore, 32 ICM potential genes were identified from ICM-related modules considering protein-protein interactions. Most of these genes were verified to be involved in ICM and diseases caused it by OMIM and literature. Our study could provide a novel perspective for potential gene identification and the pathogenesis for ICM and other complex diseases.

摘要

缺血性心肌病(ICM)是心力衰竭的一个重要原因,但尚无ICM疾病基因存储在任何公共数据库中。由RNA测序数据提供的基因突变可为多种生物学过程奠定基础。这也使得阐明ICM的机制并鉴定其潜在基因成为可能。本文利用单变量和双变量典型相关分析,对人类ICM样本的RNA测序数据构建了一个整合共表达网络。在比较ICM样本和正常对照的皮尔逊相关系数后,识别出了三个与ICM相关的模块。此外,考虑到蛋白质-蛋白质相互作用,从与ICM相关的模块中鉴定出32个ICM潜在基因。通过在线人类孟德尔遗传数据库(OMIM)和文献证实,这些基因中的大多数与ICM及其引发的疾病有关。我们的研究可为ICM及其他复杂疾病的潜在基因鉴定和发病机制提供新的视角。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/66be/5347674/7f7e951c6aa8/oncotarget-07-82063-g001.jpg

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