TY - JOUR AU - Wang, Huiqing AU - Wang, Jingjing AU - Dong, Chunlin AU - Lian, Yuanyuan AU - Liu, Dan AU - Yan, Zhiliang PY - 2020 M3 - Methods TI - A Novel Approach for Drug-Target Interactions Prediction Based on Multimodal Deep Autoencoder JO - Frontiers in Pharmacology UR - https://www.frontiersin.org/articles/10.3389/fphar.2019.01592 VL - 10 SN - 1663-9812 N2 - Drug targets are biomacromolecules or biomolecular structures that bind to specific drugs and produce therapeutic effects. Therefore, the prediction of drug-target interactions (DTIs) is important for disease therapy. Incorporating multiple similarity measures for drugs and targets is of essence for improving the accuracy of prediction of DTIs. However, existing studies with multiple similarity measures ignored the global structure information of similarity measures, and required manual extraction features of drug-target pairs, ignoring the non-linear relationship among features. In this paper, we proposed a novel approach MDADTI for DTIs prediction based on MDA. MDADTI applied random walk with restart method and positive pointwise mutual information to calculate the topological similarity matrices of drugs and targets, capturing the global structure information of similarity measures. Then, MDADTI applied multimodal deep autoencoder to fuse multiple topological similarity matrices of drugs and targets, automatically learned the low-dimensional features of drugs and targets, and applied deep neural network to predict DTIs. The results of 5-repeats of 10-fold cross-validation under three different cross-validation settings indicated that MDADTI is superior to the other four baseline methods. In addition, we validated the predictions of the MDADTI in six drug-target interactions reference databases, and the results showed that MDADTI can effectively identify unknown DTIs. ER -