miRNA plays an important role in many biological processes, and increasing evidence shows that miRNAs are closely related to human diseases. Most existing miRNA-disease association prediction methods were only based on data related to miRNAs and diseases and failed to effectively use other existing biological data. However, experimentally verified miRNA-disease associations are limited, there are complex correlations between biological data. Therefore, we propose a novel Three-layer heterogeneous network Combined with unbalanced Random Walk for MiRNA-Disease Association prediction algorithm (TCRWMDA), which can effectively integrate multi-source association data. TCRWMDA based not only on the known miRNA-disease associations, also add the new priori information (lncRNA-miRNA and lncRNA-disease associations) to build a three-layer heterogeneous network, lncRNA was added as the transition path of the intermediate point to mine more effective information between networks. The AUC value obtained by the TCRWMDA algorithm on 5-fold cross validation is 0.9209, compared with other models based on the same similarity calculation method, TCRWMDA obtained better results. TCRWMDA was applied to the analysis of four types of cancer, the results proved that TCRWMDA is an effective tool to predict the potential miRNA-disease association. The source code and dataset of TCRWMDA are available at: https:// github.com/ylm0505/TCRWMDA.
BackgroundMicrobes have been shown to play a crucial role in various ecosystems. Many human diseases have been proved to be associated with bacteria, so it is essential to extract the interaction between bacteria for medical research and application. At the same time, many bacterial interactions with certain experimental evidences have been reported in biomedical literature. Integrating this knowledge into a database or knowledge graph could accelerate the progress of biomedical research. A crucial and necessary step in interaction extraction (IE) is named entity recognition (NER). However, due to the specificity of bacterial naming, there are still challenges in bacterial named entity recognition.ResultsIn this paper, we propose a novel method for bacterial named entity recognition, which integrates domain features into a deep learning framework combining bidirectional long short-term memory network and convolutional neural network. When domain features are not added, F1-measure of the model achieves 89.14%. After part-of-speech (POS) features and dictionary features are added, F1-measure of the model achieves 89.7%. Hence, our model achieves an advanced performance in bacterial NER with the domain features.ConclusionsWe propose an efficient method for bacterial named entity recognition which combines domain features and deep learning models. Compared with the previous methods, the effect of our model has been improved. At the same time, the process of complex manual extraction and feature design are significantly reduced.
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