Efficient framework for predicting MiRNA-disease associations based on improved hybrid collaborative filtering

Ru Nie; Zhengwei Li; Zhu-hong You; Wenzheng Bao; Jiashu Li

doi:10.1186/s12911-021-01616-5

BMC Medical Informatics and Decision Making (Aug 2021)

Efficient framework for predicting MiRNA-disease associations based on improved hybrid collaborative filtering

Ru Nie,
Zhengwei Li,
Zhu-hong You,
Wenzheng Bao,
Jiashu Li

Affiliations

Ru Nie: Engineering Research Center of Mine Digitalization of Ministry of Education, China University of Mining and Technology
Zhengwei Li: Engineering Research Center of Mine Digitalization of Ministry of Education, China University of Mining and Technology
Zhu-hong You: School of Computer Science, Northwestern Polytechnical University
Wenzheng Bao: School of Information Engineering, Xuzhou University of Technology
Jiashu Li: Engineering Research Center of Mine Digitalization of Ministry of Education, China University of Mining and Technology

DOI: https://doi.org/10.1186/s12911-021-01616-5
Journal volume & issue: Vol. 21, no. S1
pp. 1 – 14

Abstract

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Abstract Background Accumulating studies indicates that microRNAs (miRNAs) play vital roles in the process of development and progression of many human complex diseases. However, traditional biochemical experimental methods for identifying disease-related miRNAs cost large amount of time, manpower, material and financial resources. Methods In this study, we developed a framework named hybrid collaborative filtering for miRNA-disease association prediction (HCFMDA) by integrating heterogeneous data, e.g., miRNA functional similarity, disease semantic similarity, known miRNA-disease association networks, and Gaussian kernel similarity of miRNAs and diseases. To capture the intrinsic interaction patterns embedded in the sparse association matrix, we prioritized the predictive score by fusing three types of information: similar disease associations, similar miRNA associations, and similar disease-miRNA associations. Meanwhile, singular value decomposition was adopted to reduce the impact of noise and accelerate predictive speed. Results We then validated HCFMDA with leave-one-out cross-validation (LOOCV) and two types of case studies. In the LOOCV, we achieved 0.8379 of AUC (area under the curve). To evaluate the performance of HCFMDA on real diseases, we further implemented the first type of case validation over three important human diseases: Colon Neoplasms, Esophageal Neoplasms and Prostate Neoplasms. As a result, 44, 46 and 44 out of the top 50 predicted disease-related miRNAs were confirmed by experimental evidence. Moreover, the second type of case validation on Breast Neoplasms indicates that HCFMDA could also be applied to predict potential miRNAs towards those diseases without any known associated miRNA. Conclusions The satisfactory prediction performance demonstrates that our model could serve as a reliable tool to guide the following research for identifying candidate miRNAs associated with human diseases.

Published in BMC Medical Informatics and Decision Making

ISSN: 1472-6947 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Medicine (General): Computer applications to medicine. Medical informatics
Website: http://bmcmedinformdecismak.biomedcentral.com

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