The knowledge of protein-protein interaction (PPI) helps us to understand proteins' functions, the causes and growth of several diseases, and can aid in designing new drugs. The majority of existing PPI research has relied mainly on sequence-based approaches. With the availability of multi-omics datasets (sequence, 3D structure) and advancements in deep learning techniques, it is feasible to develop a deep multi-modal framework that fuses the features learned from different sources of information to predict PPI. In this work, we propose a multi-modal approach utilizing protein sequence and 3D structure. To extract features from the 3D structure of proteins, we use a pre-trained vision transformer model that has been fine-tuned on the structural representation of proteins. The protein sequence is encoded into a feature vector using a pre-trained language model. The feature vectors extracted from the two modalities are fused and then fed to the neural network classifier to predict the protein interactions. To showcase the effectiveness of the proposed methodology, we conduct experiments on two popular PPI datasets, namely, the human dataset and the S. cerevisiae dataset. Our approach outperforms the existing methodologies to predict PPI, including multi-modal approaches. We also evaluate the contributions of each modality by designing uni-modal baselines. We perform experiments with three modalities as well, having gene ontology as the third modality.

• PMID: 37027644
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Journal Article | Research Support, Non-U.S. Gov't

Authors

Jha K, Saha S, Karmakar S

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