AVP-Pro: An Adaptive Multi-Modal Fusion and Contrastive Learning Approach for Comprehensive Two-Stage Antiviral Peptide Identification

The accurate identification of antiviral peptides (AVPs) is crucial for novel drug development. However, existing methods still have limitations in capturing complex sequence dependencies and distinguishing confusing samples with high similarity. To address these challenges, we propose AVP-Pro, a novel two-stage predictive framework that integrates adaptive feature fusion and contrastive learning. To comprehensively capture the physicochemical properties and deep-seated patterns of peptide sequences, we constructed a panoramic feature space encompassing 10 distinct descriptors and designed a hierarchical fusion architecture. This architecture integrates self-attention and adaptive gating mechanisms to dynamically modulate the weights of local motifs extracted by CNNs and global dependencies captured by BiLSTMs based on sequence context. Targeting the blurred decision boundary caused by the high similarity between positive and negative sample sequences, we adopted an Online Hard Example Mining (OHEM)-driven contrastive learning strategy enhanced by BLOSUM62. This approach significantly sharpened the model's discriminative power. Model evaluation results show that in the first stage of general AVP identification, the model achieved an accuracy of 0.9531 and an MCC of 0.9064, outperforming existing state-of-the-art (SOTA) methods. In the second stage of functional subtype prediction, combined with a transfer learning strategy, the model realized accurate classification of 6 viral families and 8 specific viruses under small-sample conditions. AVP-Pro provides a powerful and interpretable new tool for the high-throughput screening of antiviral drugs. To further enhance accessibility for users, we have developed a user-friendly web interface, which is available at https://wwwy1031-avp-pro.hf.space.

AVP-Fusion: Adaptive Multi-Modal Fusion and Contrastive Learning for Two-Stage Antiviral Peptide Identification

Accurate identification of antiviral peptides (AVPs) is critical for accelerating novel drug development. However, current computational methods struggle to capture intricate sequence dependencies and effectively handle ambiguous, hard-to-classify samples. To address these challenges, we propose AVP-Fusion, a novel two-stage deep learning framework integrating adaptive feature fusion and contrastive learning. Unlike traditional static feature concatenation, we construct a panoramic feature space using 10 distinct descriptors and introduce an Adaptive Gating Mechanism.This mechanism dynamically regulates the weights of local motifs extracted by CNNs and global dependencies captured by BiLSTMs based on sequence context. Furthermore, to address data distribution challenges, we employ a contrastive learning strategy driven by Online Hard Example Mining (OHEM) and BLOSUM62-based data augmentation, which significantly sharpens the model's decision boundaries. Experimental results on the benchmark Set 1 dataset demonstrate that AVP-Fusion achieves an accuracy of 0.9531 and an MCC of 0.9064, significantly outperforming state-of-the-art methods. In the second stage, leveraging transfer learning, the model enables precise subclass prediction for six viral families and eight specific viruses, even under limited sample sizes. In summary, AVP-Fusion serves as a robust and interpretable tool for high-throughput antiviral drug screening.