Issue 10, 2009

Activation of IP3 receptors by synthetic bisphosphate ligands

Abstract

Ca2+ release by D-myo-inositol 1,4,5-trisphosphate receptors (IP3Rs) is widely considered to require the vicinal 4,5-bisphosphate motif of IP3, with P-5 and P-4 engaging the α and β domains of the binding site; using synthesis and mutagenesis we show that the adenine of synthetic glyconucleotides, through an interaction with Arg504, can replace the interaction of either P-1 or P-5 with the α-domain producing, respectively, the most potent bisphosphate agonist yet synthesised and the first agonist of IP3R without a vicinal bisphosphate motif; this will stimulate new approaches to IP3R ligand design.

Graphical abstract: Activation of IP3 receptors by synthetic bisphosphate ligands

Article information

Article type
Communication
Submitted
30 Oct 2008
Accepted
20 Jan 2009
First published
04 Feb 2009
This article is Open Access

Chem. Commun., 2009, 1204-1206

Activation of IP3 receptors by synthetic bisphosphate ligands

K. M. Sureshan, A. M. Riley, A. M. Rossi, S. C. Tovey, S. G. Dedos, C. W. Taylor and B. V. L. Potter, Chem. Commun., 2009, 1204 DOI: 10.1039/B819328B

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