Improved Drug-target Interaction Prediction with Intermolecular Graph Transformer
- Siyuan Liu ,
- Yusong Wang ,
- Yifan Deng ,
- Liang He ,
- Bin Shao ,
- Jian Yin ,
- Nanning Zheng ,
- Tie-Yan Liu ,
- Tong Wang
Briefings in Bioinformatics |
The identification of active binding drugs for target proteins (termed as drug-target interaction prediction) is the key challenge in virtual screening, which plays an essential role in drug discovery. Although recent deep learning-based approaches achieved better performance than molecular docking, existing models often neglect certain aspects of the intermolecular information, hindering the performance of prediction. We recognize this problem and propose a novel approach named Intermolecular Graph Transformer (IGT) that employs a dedicated attention mechanism to model intermolecular information with a three-way Transformer-based architecture. IGT outperforms state-of-the-art approaches by 9.1% and 20.5% over the second best for binding activity and binding pose prediction respectively,and shows superior generalization ability to unseen receptor proteins. Furthermore, IGT exhibits promising drug screening ability against SARS-CoV-2 by identifying 83.1% active drugs that have been validated by wet-lab experiments with near-native predicted binding poses.