Issue 14, 2004

Synthesis and cholera toxin binding properties of multivalent GM1 mimics

Abstract

Dendrimers based on the 3,5-di-(2-aminoethoxy)-benzoic acid branching unit were used to attach multiple copies of a GM1 mimic for inhibition of cholera toxin binding. Systems up to octavalent were synthesized along with relevant reference compounds that contained in one case the ligand in a monovalent format and in another case the scaffold but not the ligand. Using a surface plasmon resonance inhibition assay the prepared inhibitors showed good inhibition. While the monovalent GM1 mimic showed the expected inhibition in the 200 µM range the multivalent scaffolds led to increased binding. The tetravalent compound was shown to be 440-fold more potent than its monovalent counterpart. The octavalent analog, however, was the most potent compound as determined using an ELISA assay.

Graphical abstract: Synthesis and cholera toxin binding properties of multivalent GM1 mimics

Article information

Article type
Paper
Submitted
13 Apr 2004
Accepted
26 May 2004
First published
30 Jun 2004

Org. Biomol. Chem., 2004,2, 2113-2124

Synthesis and cholera toxin binding properties of multivalent GM1 mimics

D. Arosio, I. Vrasidas, P. Valentini, R. M. J. Liskamp, R. J. Pieters and A. Bernardi, Org. Biomol. Chem., 2004, 2, 2113 DOI: 10.1039/B405344C

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