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Literature DB >> 18546205

Hot-spot residues at the E9/Im9 interface help binding via different mechanisms.

Sergio E Wong¹, Riccardo Baron, J Andrew McCammon.

Abstract

Protein-protein association involves many interface interactions, but they do not contribute equally. Ala scanning experiments reveal that only a few mutations significantly lower binding affinity. These key residues, which appear to drive protein-protein association, are called hot-spot residues. Molecular dynamics simulations of the Colicin E9/Im9 complex show Im9 Glu41 and Im9 Ser50, both hot-spots, bind via different mechanisms. The results suggest that Im9 Ser50 restricts Glu41 in a conformation auspicious for salt-bridge formation across the interface. This type of model may be helpful in engineering hot-spot clusters at protein-protein interfaces and, consequently, the design of specificity.

Entities: Chemical

Mesh：

Substances：

Year: 2008 PMID： 18546205 PMCID： PMC2575057 DOI： 10.1002/bip.21035

Source DB: PubMed Journal: Biopolymers ISSN： 0006-3525 Impact factor: 2.505

28 in total

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1 in total

1. E9-Im9 colicin DNase-immunity protein biomolecular association in water: a multiple-copy and accelerated molecular dynamics simulation study.

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1 in total