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Insulin Mimetic Peptide Disrupts the Primary Binding Site of the Insulin Receptor

J Biol Chem. 2016-06-01; 
Callum F Lawrence, Mai B Margetts, John G Menting, Nicholas A Smith, Brian J Smith, Colin W Ward, Michael C Lawrence
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Peptide Synthesis … S519C16 peptide (synthesized by Genscript and prepared at a concentration of 60 μm in TBSA) was titrated against the IR310.T·83-7 Fv complex (prepared at a concentration of 6 μm in TBSA) using a MicroCal iTC200 instrument (Malvern Instruments, UK) … Get A Quote

摘要

Sets of synthetic peptides that interact with the insulin receptor ectodomain have been discovered by phage display and reported in the literature. These peptides were grouped into three classes termed Site 1, Site 2, and Site 3 based on their mutual competition of binding to the receptor. Further refinement has yielded, in particular, a 36-residue Site 2-Site 1 fusion peptide, S519, that binds the insulin receptor with subnanomolar affinity and exhibits agonist activity in both lipogenesis and glucose uptake assays. Here, we report three-dimensional crystallographic detail of the interaction of the C-terminal, 16-residue Site 1 component (S519C16) of S519 with the first leucine-rich repeat domain (L1) of the i... More

关键词

Fv antibody fragment, insulin, insulin receptor, mimetic peptide, molecular modeling, peptides, protein structure, x-ray crystallography