Abstract
T cell immune recognition requires the interactions among antigen peptides, Major Histocompatibility Complex (MHC) molecules, and T cell receptors (TCRs). While research into the interactions between MHC and peptides is well established, the specific preferences of TCRs for peptides remain less understood. This gap largely stems from the requirement that antigen peptides must be bound to MHC and presented on the cell surface prior to recognition by TCRs. Typically, motifs related to TCR recognition are influenced by MHC characteristics, limiting the direct identification of TCR-specific motifs. To address this challenge, this study introduces a Bayesian method designed to decompose hierarchical motifs independently of MHC constraints. This model, rigorously tested through comprehensive simulation experiments and applied to real data, establishes a clear hierarchical structure for motifs related to T cell recognition.