A regularized discriminative model for the prediction of protein–peptide interactions

摘要

Motivation: Short well-defined domains known as peptide recognition modules (PRMs) regulate many important protein–protein interactions involved in the formation of macromolecular complexes and biochemical pathways. Since high-throughput experiments like yeast two-hybrid and phage display are expensive and intrinsically noisy, it would be desirable to more specifically target or partially bypass them with complementary in silico approaches. In the present paper, we present a probabilistic discriminative approach to predicting PRM-mediated protein–protein interactions from sequence data. The model is motivated by the discriminative model of Segal and Sharan as an alternative to the generative approach of Reiss and Schwikowski. In our evaluation, we focus on predicting the interaction network. As proposed by Williams, we overcome the problem of susceptibility to over-fitting by adopting a Bayesian a posteriori approach based on a Laplacian prior in parameter space.