MCCS, a novel characterization method for protein-ligand complex

Delineating the fingerprint or feature vector of a receptor/protein will facilitate the structural and biological studies, as well as the rational design and development of drugs with high affinities and selectivity. However, protein is complicated by its different functional regions that can bind to some of its protein partner(s), substrate(s), orthosteric ligand(s) or allosteric modulator(s) where cogent methods like molecular fingerprints do not work well. We here elaborate a scoring-functionbased computing protocol Molecular Complex Characterizing System to help characterize the binding feature of protein-ligand complexes. Based on the reported receptor-ligand interactions, we first quantitate the energy contribution of each individual residue which may be an alternative of molecular dynamics (MD)-based energy decomposition. We then construct a vector for the energy contribution to represent the pattern of the ligand recognition at a receptor and qualitatively analyze the matching level with other receptors. Finally, the energy contribution vector is explored for extensive use in similarity and clustering. The present work provides a new approach to cluster proteins, a perspective counterpart for determining the protein characteristics in the binding, and an advanced screening technique where molecular docking is applicable.

Automated summary

This study introduces a scoring-function based computing protocol to characterize the binding feature of protein-ligand complexes. The energy contribution of individual residues is quantitated to construct a vector representing ligand recognition pattern, which is then used for similarity and clustering analysis. This approach offers a new perspective for clustering proteins, determining protein characteristics in binding, and advanced screening using molecular docking.