Synthesis and evaluation of novel 3-C-alkylated-Neu5Ac2en derivatives as probes of influenza virus sialidase 150-loop flexibility

Novel 3-C-alkylated-Neu5Ac2en derivatives have been designed to target the expanded active site cavity of influenza virus sialidases with an open 150-loop, currently seen in X-ray crystal structures of influenza A virus group-1 (N1, N4, N5, N8), but not group-2 (N2, N9), sialidases. The compounds sh...

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Veröffentlicht in:Organic & biomolecular chemistry 2012-11, Vol.10 (43), p.8628-8639
Hauptverfasser: Rudrawar, Santosh, Kerry, Philip S, Rameix-Welti, Marie-Anne, Maggioni, Andrea, Dyason, Jeffrey C, Rose, Faith J, van der Werf, Sylvie, Thomson, Robin J, Naffakh, Nadia, Russell, Rupert J M, von Itzstein, Mark
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Sprache:eng
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Zusammenfassung:Novel 3-C-alkylated-Neu5Ac2en derivatives have been designed to target the expanded active site cavity of influenza virus sialidases with an open 150-loop, currently seen in X-ray crystal structures of influenza A virus group-1 (N1, N4, N5, N8), but not group-2 (N2, N9), sialidases. The compounds show selectivity for inhibition of H5N1 and pdm09 H1N1 sialidases over an N2 sialidase, providing evidence of the relative 150-loop flexibility of these sialidases. In a complex with N8 sialidase, the C3 substituent of 3-phenylally-Neu5Ac2en occupies the 150-cavity while the central ring and the remaining substituents bind the active site as seen for the unsubstituted template. This new class of inhibitors, which can 'trap' the open 150-loop form of the sialidase, should prove useful as probes of 150-loop flexibility.
ISSN:1477-0520
1477-0539
DOI:10.1039/c2ob25627d