Background: The potential of graph neural networks (GNNs) to revolutionize the analysis of non-Euclidean data has gained attention recently, making them attractive models for deep machine learning. However, insufficient compound or moleculargraphs and feature representations might significantly impair and jeopardize their full potential. Despite the devastating impacts of ongoing COVID-19 across the globe, for which there is no drug with proven efficacy that has been shown tobe effective. As various stages of drug discovery and repositioning require the accurate prediction of drugtarget interactions(DTI), here, we propose a relational graph convolution network using multi-features based on the developed drug chemicalcompound-coronavirus target graph representation and combination of features. During the implementation of the model, we further introduced the use of not only the feature module to understand the topological structure of drugs but also the structure of the proven drug target (i.e., 3CLpro) for SARS-Cov-2 that shares a genome sequence similar to that of other members of the beta-coronavirus group such as SARS-Cov, MERS-CoV, bat coronavirus. Our feature comprises topologicalinformation in molecular SMILES and local chemical context in the SMILES sequence for the drug chemical compound and drug target. Our proposed method prevailed with high and compelling performance accuracy of 97.30% which could beprioritized as the potential and promising prediction route for the development of novel oral antiviral medicine for COVID-19 drugs. Objective: Forecasting DTI stands as a pivotal aspect of drug discovery. The focus on computational methods in DTI prediction has intensified due to the considerable expense and time investment associated with conducting extensive in vitro and in vivo experiments. Machine learning techniques, particularly deep learning, have found broad applications in DTI prediction. We are convinced that this study could be prioritized and utilized as the promising predictive route for the development of novel oral antiviral treatments for COVID-19 and other variants of coronaviruses. Methods: This study addressed the problem of COVID-19 drugs using proposed RGCN with multifeatures as an attractive and potential route. This study focused mainly on the prediction of novel antiviral drugs against coronaviruses using graph-based methodology, namely RGCN. This research further utilized the features of both drugs and common potential drug targets found in betacoronaviruses group to deepen understanding of their underlying relation. Results: Our suggested approach prevailed with a high and convincing performance accuracy of 97.30%, which may be utilizedas a top priority to support and advance this field in the prediction and development of novel antiviral treatments against coronaviruses and their variants. Conclusion: We recursively performed experiments using the proposed method on our constructed DCCCvT graph dataset from our collected dataset with various single and multiple combinations of features and found that our model had achieved comparable best-averaged accuracy performance on T7 features followed by a combination of T7, R6, and L8. The proposed model implemented in this investigation turns out to outperform the previous related works.
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