TY - JOUR
T1 - A non-negative matrix factorization based method for predicting disease-Associated miRNAs in miRNA-disease bilayer network
AU - Zhong, Yingli
AU - Xuan, Ping
AU - Wang, Xiao
AU - Zhang, Tiangang
AU - Li, Jianzhong
AU - Liu, Yong
AU - Zhang, Weixiong
N1 - Publisher Copyright:
© The Author 2017. Published by Oxford University Press. All rights reserved. For Permissions, please e-mail: [email protected].
PY - 2018/1/15
Y1 - 2018/1/15
N2 - Motivation Identification of disease-Associated miRNAs (disease miRNAs) is critical for understanding disease etiology and pathogenesis. Since miRNAs exert their functions by regulating the expression of their target mRNAs, several methods based on the target genes were proposed to predict disease miRNA candidates. They achieved only limited success as they all suffered from the high false-positive rate of target prediction results. Alternatively, other prediction methods were based on the observation that miRNAs with similar functions tend to be associated with similar diseases and vice versa. The methods exploited the information about miRNAs and diseases, including the functional similarities between miRNAs, the similarities between diseases, and the associations between miRNAs and diseases. However, how to integrate the multiple kinds of information completely and consider the biological characteristic of disease miRNAs is a challenging problem. Results We constructed a bilayer network to represent the complex relationships among miRNAs, among diseases and between miRNAs and diseases. We proposed a non-negative matrix factorization based method to rank, so as to predict, the disease miRNA candidates. The method integrated the miRNA functional similarity, the disease similarity and the miRNA-disease associations seamlessly, which exploited the complex relationships within the bilayer network and the consensus relationship between multiple kinds of information. Considering the correlation between the candidates related to various diseases, it predicted their respective candidates for all the diseases simultaneously. In addition, the sparseness characteristic of disease miRNAs was introduced to generate more reliable prediction model that excludes those noisy candidates. The results on 15 common diseases showed a superior performance of the new method for not only well-characterized diseases but also new ones. A detailed case study on breast neoplasms, colorectal neoplasms, lung neoplasms and 32 other diseases demonstrated the ability of the method for discovering potential disease miRNAs. Availability and implementation The web service for the new method and the list of predicted candidates for all the diseases are available at http://www.bioinfolab.top. Contact [email protected] or [email protected] or [email protected] Supplementary informationSupplementary dataare available at Bioinformatics online.
AB - Motivation Identification of disease-Associated miRNAs (disease miRNAs) is critical for understanding disease etiology and pathogenesis. Since miRNAs exert their functions by regulating the expression of their target mRNAs, several methods based on the target genes were proposed to predict disease miRNA candidates. They achieved only limited success as they all suffered from the high false-positive rate of target prediction results. Alternatively, other prediction methods were based on the observation that miRNAs with similar functions tend to be associated with similar diseases and vice versa. The methods exploited the information about miRNAs and diseases, including the functional similarities between miRNAs, the similarities between diseases, and the associations between miRNAs and diseases. However, how to integrate the multiple kinds of information completely and consider the biological characteristic of disease miRNAs is a challenging problem. Results We constructed a bilayer network to represent the complex relationships among miRNAs, among diseases and between miRNAs and diseases. We proposed a non-negative matrix factorization based method to rank, so as to predict, the disease miRNA candidates. The method integrated the miRNA functional similarity, the disease similarity and the miRNA-disease associations seamlessly, which exploited the complex relationships within the bilayer network and the consensus relationship between multiple kinds of information. Considering the correlation between the candidates related to various diseases, it predicted their respective candidates for all the diseases simultaneously. In addition, the sparseness characteristic of disease miRNAs was introduced to generate more reliable prediction model that excludes those noisy candidates. The results on 15 common diseases showed a superior performance of the new method for not only well-characterized diseases but also new ones. A detailed case study on breast neoplasms, colorectal neoplasms, lung neoplasms and 32 other diseases demonstrated the ability of the method for discovering potential disease miRNAs. Availability and implementation The web service for the new method and the list of predicted candidates for all the diseases are available at http://www.bioinfolab.top. Contact [email protected] or [email protected] or [email protected] Supplementary informationSupplementary dataare available at Bioinformatics online.
UR - https://www.scopus.com/pages/publications/85040546974
U2 - 10.1093/bioinformatics/btx546
DO - 10.1093/bioinformatics/btx546
M3 - Article
C2 - 28968753
AN - SCOPUS:85040546974
SN - 1367-4803
VL - 34
SP - 267
EP - 277
JO - Bioinformatics
JF - Bioinformatics
IS - 2
ER -