Proteome-Wide Inference of Src Homology 3 Domain-Binding Peptides

Src homology 3 (SH3) domain is a versatile protein structure module that participates in mediating various protein–protein binding events by specifically recognizing proline-rich region of diverse plasmatic proteins. Reliable and fast inference of SH3-binding partners over the human proteome are fundamentally important for our understanding of the molecular functions and biological implications underlying SH3-mediated signaling network. Herein, we employ an atom-realistic protocol to perform proteome-wide inference of SH3-binding peptides using the information gained from both the primary sequence of affinity-known peptides and the interaction properties deriving from SH3–peptide complex structures. It is revealed that the binding affinity and specificity of peptides to SH3 domain are co-contributed from electrostatic, steric and hydrophobic effects, and the hydrophobicity and electrostatic property at P2, P0 and/or P−3 play an essential role in determining the binding. In addition, SH3 domain exhibits a broad specificity of recognizing its ligands and thus a large number of protein candidates that might be the potential interacting partners of SH3 domain are extracted from the human proteome, from which several samples are suggested to be the highly promising SH3 binders.