RLFDDA: a meta-path based graph representation learning model for drug-disease association prediction

Meng-Long Zhang; Bo-Wei Zhao; Xiao-Rui Su; Yi-Zhou He; Yue Yang; Lun Hu

doi:10.1186/s12859-022-05069-z

RLFDDA: a meta-path based graph representation learning model for drug-disease association prediction

BMC Bioinformatics. 2022 Dec 1;23(1):516. doi: 10.1186/s12859-022-05069-z.

Authors

Meng-Long Zhang^{1

2

3}, Bo-Wei Zhao^{1

2

3}, Xiao-Rui Su^{1

2

3}, Yi-Zhou He⁴, Yue Yang⁴, Lun Hu^{5

6

7}

Affiliations

¹ The Xinjiang Technical Institute of Physics and Chemistry, Chinese Academy of Sciences, Urumqi, China.
² University of Chinese Academy of Sciences, Beijing, China.
³ Xinjiang Laboratory of Minority Speech and Language Information Processing, Urumqi, China.
⁴ School of Computer Science and Technology, Wuhan University of Technology, Wuhan, China.
⁵ The Xinjiang Technical Institute of Physics and Chemistry, Chinese Academy of Sciences, Urumqi, China. hulun@ms.xjb.ac.cn.
⁶ University of Chinese Academy of Sciences, Beijing, China. hulun@ms.xjb.ac.cn.
⁷ Xinjiang Laboratory of Minority Speech and Language Information Processing, Urumqi, China. hulun@ms.xjb.ac.cn.

Abstract

Background: Drug repositioning is a very important task that provides critical information for exploring the potential efficacy of drugs. Yet developing computational models that can effectively predict drug-disease associations (DDAs) is still a challenging task. Previous studies suggest that the accuracy of DDA prediction can be improved by integrating different types of biological features. But how to conduct an effective integration remains a challenging problem for accurately discovering new indications for approved drugs.

Methods: In this paper, we propose a novel meta-path based graph representation learning model, namely RLFDDA, to predict potential DDAs on heterogeneous biological networks. RLFDDA first calculates drug-drug similarities and disease-disease similarities as the intrinsic biological features of drugs and diseases. A heterogeneous network is then constructed by integrating DDAs, disease-protein associations and drug-protein associations. With such a network, RLFDDA adopts a meta-path random walk model to learn the latent representations of drugs and diseases, which are concatenated to construct joint representations of drug-disease associations. As the last step, we employ the random forest classifier to predict potential DDAs with their joint representations.

Results: To demonstrate the effectiveness of RLFDDA, we have conducted a series of experiments on two benchmark datasets by following a ten-fold cross-validation scheme. The results show that RLFDDA yields the best performance in terms of AUC and F1-score when compared with several state-of-the-art DDAs prediction models. We have also conducted a case study on two common diseases, i.e., paclitaxel and lung tumors, and found that 7 out of top-10 diseases and 8 out of top-10 drugs have already been validated for paclitaxel and lung tumors respectively with literature evidence. Hence, the promising performance of RLFDDA may provide a new perspective for novel DDAs discovery over heterogeneous networks.

Keywords: Drug–disease association prediction; Graph representation learning; Heterogeneous network; Meta-path based random walk.

MeSH terms

Benchmarking
Drug Discovery
Humans
Learning*
Lung Neoplasms*
Paclitaxel

Substances

Paclitaxel

Abstract

MeSH terms

Substances

Grants and funding