Imidazopyridazine Hepatitis C Virus Polymerase Inhibitors. Structure–Activity Relationship Studies and the Discovery of a Novel, Traceless Prodrug Mechanism

By reducing the basicity of the core heterocycle in a series of HCV NS5B inhibitors, the hERG liability was reduced. The SAR was then systematically explored in order to increase solubility and enable dose escalation while retaining potency. During this exploration, a facile decarboxylation was note...

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Veröffentlicht in:	Journal of medicinal chemistry 2014-03, Vol.57 (5), p.1964-1975
Hauptverfasser:	Leivers, Martin, Miller, John F., Chan, Stephanie A., Lauchli, Ryan, Liehr, Sebastian, Mo, Wenyan, Ton, Tony, Turner, Elizabeth M., Youngman, Michael, Falls, J. Greg, Long, Susan, Mathis, Amanda, Walker, Jill
Format:	Artikel
Sprache:	eng
Schlagworte:	Animals Antiviral Agents - chemistry Antiviral Agents - pharmacokinetics Antiviral Agents - pharmacology Dogs Enzyme Inhibitors - chemistry Enzyme Inhibitors - pharmacokinetics Enzyme Inhibitors - pharmacology Hepacivirus - drug effects Hepacivirus - enzymology Magnetic Resonance Spectroscopy Mass Spectrometry Pyridazines - chemistry Pyridazines - pharmacokinetics Pyridazines - pharmacology Rats Structure-Activity Relationship Viral Nonstructural Proteins - antagonists & inhibitors
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Zusammenfassung:	By reducing the basicity of the core heterocycle in a series of HCV NS5B inhibitors, the hERG liability was reduced. The SAR was then systematically explored in order to increase solubility and enable dose escalation while retaining potency. During this exploration, a facile decarboxylation was noted and was exploited as a novel prodrug mechanism. The synthesis and characterization of these prodrugs and their utilization in chronic toxicity studies are presented.
ISSN:	0022-2623 1520-4804
DOI:	10.1021/jm401337x