Met-204 And Tyr-205 Are Together Important For Binding Glp-1 Receptor Agonists But Not Their N-Terminally Truncated Analogues

Rakel   Lopez   de Maturana; Janet      Treece-Birch; Fatima      Abidi; John   B.C.   Findlay; Dan      Donnelly

Protein & Peptide Letters

Author(s): Rakel Lopez de Maturana, Janet Treece-Birch, Fatima Abidi, John B.C. Findlay and Dan Donnelly

DOI: 10.2174/0929866043478491

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Met-204 And Tyr-205 Are Together Important For Binding Glp-1 Receptor Agonists But Not Their N-Terminally Truncated Analogues

Page: [15 - 22] Pages: 8

* (Excluding Mailing and Handling)

Abstract

A mutagenesis study to systematically analyse residues spanning the first extracellular loop of the GLP-1 receptor identified a double mutant, Met-204 / Tyr-205-Ala / Ala, which displayed: markedly reduced affinity for the natural agonist GLP-1; slightly reduced affinity for its analogue exendin-4; and unaltered affinity for several N-terminally truncated analogues of GLP-1 and exendin-4. This suggests that the locus is important for the formation of the binding site for the N-terminal residues of peptide agonists.

Keywords: Met-204 And Tyr-205, N-terminally, Glp-1 Receptor

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