Atomic Contact Vectors in Protein-protein Recognition

Overview

Journal Proteins

Date 2003 Oct 28

PMID 14579354

Citations 41

Authors

Julian Mintseris

Zhiping Weng

Affiliations

Soon will be listed here.

Abstract

The ability to analyze and compare protein-protein interactions on the structural level is critical to our understanding of various aspects of molecular recognition and the functional interplay of components of biochemical networks. In this study, we introduce atomic contact vectors (ACVs) as an intuitive way to represent the physico-chemical characteristics of a protein-protein interface as well as a way to compare interfaces to each other. We test the utility of ACVs in classification by using them to distinguish between homodimers and crystal contacts. Our results compare favorably with those reported by other authors. We then apply ACVs to mine the PDB for all known protein-protein complexes and separate transient recognition complexes from permanent oligomeric ones. Getting at the basis of this difference is important for our understanding of recognition and we achieved a success rate of 91% for distinguishing these two classes of complexes. Although accessible surface area of the interface is a major discriminating feature, we also show that there are distinct differences in the contact preferences between the two kinds of complexes. Illustrating the superiority of ACVs as a basic comparison measure over a sequence-based approach, we derive a general rule of thumb to determine whether two protein-protein interfaces are redundant. With this method, we arrive at a nonredundant set of 209 recognition complexes--the largest set reported so far.

Citing Articles

Statistical analysis of sequential motifs at biologically relevant protein-protein interfaces.

Frank Y, Unger R, Senderowitz H Comput Struct Biotechnol J. 2024; 23:1244-1259.

PMID: 38550974 PMC: 10973581. DOI: 10.1016/j.csbj.2024.03.004.

Protein Complex Organization Imposes Constraints on Proteome Dysregulation in Cancer.

Senger G, Schaefer M Front Bioinform. 2022; 1:723482.

PMID: 36303728 PMC: 9580999. DOI: 10.3389/fbinf.2021.723482.

Are transient protein-protein interactions more dispensable?.

Ghadie M, Xia Y PLoS Comput Biol. 2022; 18(4):e1010013.

PMID: 35404956 PMC: 9000134. DOI: 10.1371/journal.pcbi.1010013.

Distance-based reconstruction of protein quaternary structures from inter-chain contacts.

Soltanikazemi E, Quadir F, Roy R, Guo Z, Cheng J Proteins. 2021; 90(3):720-731.

PMID: 34716620 PMC: 8816881. DOI: 10.1002/prot.26269.

Co-evolutionary landscape at the interface and non-interface regions of protein-protein interaction complexes.

Mukherjee I, Chakrabarti S Comput Struct Biotechnol J. 2021; 19:3779-3795.

PMID: 34285778 PMC: 8271121. DOI: 10.1016/j.csbj.2021.06.039.