Issue 17, 2011

Synthesis, biological evaluation and structural characterization of novel glycopeptide analogues of nociceptin N/OFQ

Abstract

To examine if the biological activity of the N/OFQ peptide, which is the native ligand of the pain-related and viable drug target NOP receptor, could be modulated by glycosylation and if such effects could be conformationally related, we have synthesized three N/OFQ glycopeptide analogues, namely: [Thr5-O-α-D-GalNAc-N/OFQ] (glycopeptide 1), [Ser10-O-α-D-GalNAc]-N/OFQ (glycopeptide 2) and [Ser10-O-β-D-GlcNAc]-N/OFQ] (glycopeptide 3). They were tested for biological activity in competition binding assays using the zebrafish animal model in which glycopeptide 2 exhibited a slightly improved binding affinity, whereas glycopeptide 1 showed a remarkably reduced binding affinity compared to the parent compound and glycopeptide 3. The structural analysis of these glycopeptides and the parent N/OFQ peptide by NMR and circular dichroism indicated that their aqueous solutions are mainly populated by random coil conformers. However, in membrane mimic environments a certain proportion of the molecules of all these peptides exist as α-helix structures. Interestingly, under these experimental conditions, glycopeptide 1 (glycosylated at Thr-5) exhibited a population of folded hairpin-like geometries. From these facts it is tempting to speculate that nociceptin analogues showing linear helical structures are more complementary and thus interact more efficiently with the native NOP receptor than folded structures, since glycopeptide 1 showed a significantly reduced binding affinity for the NOP receptor.

Graphical abstract: Synthesis, biological evaluation and structural characterization of novel glycopeptide analogues of nociceptin N/OFQ

Supplementary files

Article information

Article type
Paper
Submitted
04 Feb 2011
Accepted
31 May 2011
First published
02 Jun 2011

Org. Biomol. Chem., 2011,9, 6133-6142

Synthesis, biological evaluation and structural characterization of novel glycopeptide analogues of nociceptin N/OFQ

G. Arsequell, M. Rosa, C. Mayato, R. L. Dorta, V. Gonzalez-Nunez, K. Barreto-Valer, F. Marcelo, L. P. Calle, J. T. Vázquez, R. E. Rodríguez, J. Jiménez-Barbero and G. Valencia, Org. Biomol. Chem., 2011, 9, 6133 DOI: 10.1039/C1OB05197K

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