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. 2014 Jan 20;53(4):1076-80.
doi: 10.1002/anie.201308142. Epub 2013 Dec 11.

Serendipitous discovery of a potent influenza virus a neuraminidase inhibitor

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Serendipitous discovery of a potent influenza virus a neuraminidase inhibitor

Sankar Mohan et al. Angew Chem Int Ed Engl. .

Abstract

We have previously reported a potent neuraminidase inhibitor that comprises a carbocyclic analogue of zanamivir in which the hydrophilic glycerol side chain is replaced by the hydrophobic 3-pentyloxy group of oseltamivir. This hybrid inhibitor showed excellent inhibitory properties in the neuraminidase inhibition assay (Ki =0.46 nM; Ki (zanamivir) =0.16 nM) and in the viral replication inhibition assay in cell culture at 10(-8) M. As part of this lead optimization, we now report a novel spirolactam that shows comparable inhibitory activity in the cell culture assay to that of our lead compound at 10(-7) M. The compound was discovered serendipitously during the attempted synthesis of the isothiourea derivative of the original candidate. The X-ray crystal structure of the spirolactam in complex with the N8 subtype neuraminidase offers insight into the mode of inhibition.

Keywords: antiviral agents; drug discovery; influenza A; neuraminidase inhibitors; spiro compounds.

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