DGDRP: drug-specific gene selection for drug response prediction via re-ranking through propagating and learning biological network.

Drug response prediction, especially in terms of cell viability prediction, is a well-studied research problem with significant implications for personalized medicine. It enables the identification of the most effective drugs based on individual genetic profiles, aids in selecting potential drug candidates, and helps identify biomarkers that predict drug efficacy and toxicity.A deeper investigation on drug response prediction reveals that drugs exert their effects by targeting specific proteins, which in turn perturb related genes in cascading ways. This perturbation affects cellular pathways and regulatory networks, ultimately influencing the cellular response to the drug. Identifying which genes are perturbed and how they interact can provide critical insights into the mechanisms of drug action. Hence, the problem of predicting drug response can be framed as a dual problem involving both the prediction of drug efficacy and the selection of drug-specific genes. Identifying these drug-specific genes (biomarkers) is crucial because they serve as indicators of how the drug will affect the biological system, thereby facilitating both drug response prediction and biomarker discovery. In this study, we propose DGDRP (Drug-specific Gene selection for Drug Response Prediction), a graph neural network (GNN)-based model that uses a novel rank-and-re-rank process for drug-specific gene selection. DGDRP first ranks genes using a pathway knowledge-enhanced network propagation algorithm based on drug target information, ensuring biological relevance. It then re-ranks genes based on the similarity between gene and drug target embeddings learned from the GNN, incorporating semantic relationships. Thus, our model adaptively learns to select drug mechanism-associated genes that contribute to drug response prediction. This integrated approach not only improves drug response predictions compared to other gene selection methods but also allows for effective biomarker discovery. As a result, our approach demonstrates improved drug response predictions compared to other gene selection methods and demonstrates comparability with state-of-the-art deep learning models. Case studies further support our method by showing alignment of selected gene sets with the mechanisms of action of input drugs. Overall, DGDRP represents a deep learning based re-ranking strategy, offering a robust gene selection framework for more accurate drug response prediction. The source code for DGDRP can be found at: https://github.com/minwoopak/heteronet.