YAPP-CD: Yet another protein-peptide complex database

Abstract Protein-peptide interactions are of great interest to the research community not only because they serve as mediators in many protein-protein interactions but also because of the increasing demand for peptide-based pharmaceutical products. Protein-peptide docking is a major tool for studying protein-peptide interactions, and several docking methods are currently available. Among various protein-peptide docking algorithms, template-based approaches, which utilize known protein-peptide complexes or templates to predict a new one, have been shown to yield more reliable results than template-free methods in recent comparative research. To obtain reliable results with a template-based docking method, the template database must be comprehensive enough; that is, there must be similar templates of protein-peptide complexes to the protein and peptide being investigated. Thus, the template database must be updated to leverage recent advances in structural biology. However, the template database distributed with GalaxyPepDock, one of the most widely used peptide docking programs, is outdated, limiting the prediction quality of the method. Here, we present an up-to-date protein-peptide complex database called YAPP-CD, which can be directly plugged into the GalaxyPepDock binary package to improve GalaxyPepDock’s prediction quality by drawing on recent discoveries in structural biology. Experimental results show that YAPP-CD significantly improves GalaxyPepDock’s prediction quality, e.g., the average Ligand/Interface RMSD of a benchmark set is reduced from 7.60 Å/3.62 Å to 3.47 Å/1.71 Å.