Hyeoncheol Cho

Hyeoncheol Cho, Youngrock Oh, Eunjoo Jeon

Explaining the foundations for predictions obtained from graph neural networks (GNNs) is critical for credible use of GNN models for real-world problems. Owing to the rapid growth of GNN applications, recent progress in explaining predictions from GNNs, such as sensitivity analysis, perturbation methods, and attribution methods, showed great opportunities and possibilities for explaining GNN predictions. In this study, we propose a method to improve the explanation quality of node classification tasks that can be applied in a post hoc manner through aggregation of auxiliary explanations from important neighboring nodes, named SEEN. Applying SEEN does not require modification of a graph and can be used with diverse explainability techniques due to its independent mechanism. Experiments on matching motif-participating nodes from a given graph show great improvement in explanation accuracy of up to 12.71% and demonstrate the correlation between the auxiliary explanations and the enhanced explanation accuracy through leveraging their contributions. SEEN provides a simple but effective method to enhance the explanation quality of GNN model outputs, and this method is applicable in combination with most explainability techniques.

Hyeoncheol Cho, Eok Kyun Lee, Insung S. Choi

Expanding the scope of graph-based, deep-learning models to noncovalent protein-ligand interactions has earned increasing attention in structure-based drug design. Modeling the protein-ligand interactions with graph neural networks (GNNs) has experienced difficulties in the conversion of protein-ligand complex structures into the graph representation and left questions regarding whether the trained models properly learn the appropriate noncovalent interactions. Here, we proposed a GNN architecture, denoted as InteractionNet, which learns two separated molecular graphs, being covalent and noncovalent, through distinct convolution layers. We also analyzed the InteractionNet model with an explainability technique, i.e., layer-wise relevance propagation, for examination of the chemical relevance of the model's predictions. Separation of the covalent and noncovalent convolutional steps made it possible to evaluate the contribution of each step independently and analyze the graph-building strategy for noncovalent interactions. We applied InteractionNet to the prediction of protein-ligand binding affinity and showed that our model successfully predicted the noncovalent interactions in both performance and relevance in chemical interpretation.

Hyeoncheol Cho, Insung S. Choi

We present a three-dimensional graph convolutional network (3DGCN), which predicts molecular properties and biochemical activities, based on 3D molecular graph. In the 3DGCN, graph convolution is unified with learning operations on the vector to handle the spatial information from molecular topology. The 3DGCN model exhibits significantly higher performance on various tasks compared with other deep-learning models, and has the ability of generalizing a given conformer to targeted features regardless of its rotations in the 3D space. More significantly, our model also can distinguish the 3D rotations of a molecule and predict the target value, depending upon the rotation degree, in the protein-ligand docking problem, when trained with orientation-dependent datasets. The rotation distinguishability of 3DGCN, along with rotation equivariance, provides a key milestone in the implementation of three-dimensionality to the field of deep-learning chemistry that solves challenging biochemical problems.