TransformerCPI: improving compound–protein interaction prediction by sequence-based deep learning with self-attention mechanism and label reversal experiments

Motivation Identifying compound–protein interaction (CPI) is a crucial task in drug discovery and chemogenomics studies, and proteins without three-dimensional structure account for a large part of potential biological targets, which requires developing methods using only protein sequence information to predict CPI. However, sequence-based CPI models may face some specific pitfalls, including using inappropriate datasets, hidden ligand bias and splitting datasets inappropriately, resulting in overestimation of their prediction performance. Results To address these issues, we here constructed new datasets specific for CPI prediction, proposed a novel transformer neural network named TransformerCPI, and introduced a more rigorous label reversal experiment to test whether a model learns true interaction features. TransformerCPI achieved much improved performance on the new experiments, and it can be deconvolved to highlight important interacting regions of protein sequences and compound atoms, which may contribute chemical biology studies with useful guidance for further ligand structural optimization.

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Results from the Paper


Task Dataset Model Metric Name Metric Value Global Rank Benchmark
Drug Discovery BindingDB TransformerCPI AUC 0.937 # 3
Drug Discovery LIT-PCBA(ALDH1) TransformerCPI AUC 0.694 # 3
Drug Discovery LIT-PCBA(ESR1_ant) TransformerCPI AUC 0.616 # 2
Drug Discovery LIT-PCBA(KAT2A) TransformerCPI AUC 0.650 # 3
Drug Discovery LIT-PCBA(MAPK1) TransformerCPI AUC 0.683 # 3

Methods


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