Dual-channel graph learning reveals similarity and complementarity in protein-protein interaction networks
Journal:
bioRxiv
Published Date:
Jan 27, 2026
Abstract
Protein-protein interactions (PPIs) are governed by two fundamental interfacial mechanisms: similarity-driven, often involving symmetric structural motifs, and complementarity-driven, arising from geometric and physicochemical matching between binding surfaces. Despite their biological significance, computational models have largely overlooked the coexistence and interplay of these twofold interaction modes. Here, we introduce DMG-PPI, a dual-channel graph neural network framework that jointly models similarity and complementarity in PPI networks, extending prior heterophilous GNN concepts to explicitly disentangle these dual interaction modes. The model consists of two parallel message-passing pathways: Alignment Message Passing (AMP), which aggregates signals from similar neighbors to capture symmetric interfaces, and Divergence Message Passing (DMP), which contrasts node features to extract complementary binding patterns. The signals captured by AMP and DMP are integrated via an adaptive fusion strategy within each block, and the outputs of blocks are aggregated using the MixHop framework to encode higher-order interaction patterns. DMG-PPI substantially outperforms state-of-the-art methods on classical benchmark datasets, achieving a 7.19% improvement in Micro-F1 over the second-best method. Additionally, the dual-channel framework provides interpretable insights into key binding residues by identifying interfacial mechanisms. Overall, DMG-PPI serves as a powerful tool that reveals the mechanisms behind accurate PPI predictions and facilitates downstream biological analysis.
