Predicting Protein-Ligand Binding Affinity Using Fusion Model of Spatial-Temporal Graph Neural Network and 3D Structure-Based Complex Graph.

Abstract

The investigation of molecular interactions between ligands and their target molecules is becoming more significant as protein structure data continues to develop. In this study, we introduce PLA-STGCNnet, a deep fusion spatial-temporal graph neural network designed to study protein-ligand interactions based on the 3D structural data of protein-ligand complexes. Unlike 1D protein sequences or 2D ligand graphs, the 3D graph representation offers a more precise portrayal of the complex interactions between proteins and ligands. Research studies have shown that our fusion model, PLA-STGCNnet, outperforms individual algorithms in accurately predicting binding affinity. The advantage of a fusion model is the ability to fully combine the advantages of multiple different models and improve overall performance by combining their features and outputs. Our fusion model shows satisfactory performance on different data sets, which proves its generalization ability and stability. The fusion-based model showed good performance in protein-ligand affinity prediction, and we successfully applied the model to drug screening. Our research underscores the promise of fusion spatial-temporal graph neural networks in addressing complex challenges in protein-ligand affinity prediction. The Python scripts for implementing various model components are accessible at https://github.com/ligaili01/PLA-STGCN.