| Literature DB >> 30471255 |
Moshe Ben-David1, Haiming Huang1, Mark G F Sun2, Carles Corbi-Verge2, Evangelia Petsalaki3, Ke Liu4, David Gfeller1, Pankaj Garg1, Wolfram Tempel4, Irina Sochirca1, Julia M Shifman5, Alan Davidson6, Jinrong Min4, Philip M Kim7, Sachdev S Sidhu8.
Abstract
Hydrophobic cores are often viewed as tightly packed and rigid, but they do show some plasticity and could thus be attractive targets for protein design. Here we explored the role of different functional pressures on the core packing and ligand recognition of the SH3 domain from human Fyn tyrosine kinase. We randomized the hydrophobic core and used phage display to select variants that bound to each of three distinct ligands. The three evolved groups showed remarkable differences in core composition, illustrating the effect of different selective pressures on the core. Changes in the core did not significantly alter protein stability, but were linked closely to changes in binding affinity and specificity. Structural analysis and molecular dynamics simulations revealed the structural basis for altered specificity. The evolved domains had significantly reduced core volumes, which in turn induced increased backbone flexibility. These motions were propagated from the core to the binding surface and induced significant conformational changes. These results show that alternative core packing and consequent allosteric modulation of binding interfaces could be used to engineer proteins with novel functions. CrownEntities:
Keywords: SH3 domain; binding specificity; conformational flexibility; hydrophobic core; phage display
Mesh:
Substances:
Year: 2018 PMID: 30471255 DOI: 10.1016/j.jmb.2018.11.018
Source DB: PubMed Journal: J Mol Biol ISSN: 0022-2836 Impact factor: 5.469