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EpiCoCo: De Novo Epitope Generation via MHC-Context Co-Modeling and Contrastive Affinity Guidance

Haoyang Luan, Gufeng Yu, Letian Chen, Zhenran Xiao, Yueshan Huang, Junkun Guo, Yang Yang

ICML 2026 regular

Tóm tắt (nguồn: OpenReview · © tác giả)

The *de novo* generation of high-affinity epitopes tailored to specific major histocompatibility complex (MHC) proteins is a pivotal challenge in computational immunotherapy. However, current methods struggle to effectively integrate the MHC context into the generation process, and often fail to guarantee high binding affinity due to the neglect of discriminative signals from non-binders. To bridge these gaps, we present **EpiCoCo**, a probabilistic framework for **Epi**tope generation via MHC-context **Co**-modeling and **Co**ntrastive affinity learning. EpiCoCo treats the pMHC complex as a dynamic, co-adaptive system by operating on the joint E(3) graph. In addition, we introduce Contrastive Affinity Guidance (CAG), an inference mechanism that leverages the gradient difference between learned high- and low-affinity distributions. CAG actively drives the generation trajectory towards high-affinity manifolds while utilizing repulsive signals to filter out candidates with poor binding potential. Extensive evaluations demonstrate that EpiCoCo achieves a mean binding free energy of -45.20 REU, a 23% improvement over the state-of-the-art, while maintaining high structural plausibility. The results validate that context co-modeling and negative-informed guidance are essential for generating valid, high-potency immunotherapeutics.

Từ khoá

Immunotherapeutics Peptide Design Structure-Sequence Co-design

Metadata từ BioTender-max/icml2026-ai-bio (CC0-1.0). Phở không lưu trữ bản PDF; link trỏ về nguồn gốc.

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