| Literature DB >> 20527890 |
Christopher McGuigan1, Arnaud Gilles, Karolina Madela, Mohamed Aljarah, Sabrina Holl, Sarah Jones, John Vernachio, Jeff Hutchins, Brenda Ames, K Dawn Bryant, Elena Gorovits, Babita Ganguly, Damound Hunley, Andrea Hall, Alexander Kolykhalov, Yule Liu, Jerry Muhammad, Nicholas Raja, Robin Walters, Jin Wang, Stanley Chamberlain, Geoffrey Henson.
Abstract
Hepatitis C virus infection constitutes a serious health problem in need of more effective therapies. Nucleoside analogues with improved exposure, efficacy, and selectivity are recognized as likely key components of future HCV therapy. 2'-C-Methylguanosine triphosphate has been known as a potent inhibitor of HCV RNA polymerase for some time, but the parent nucleoside is only moderately active due to poor intracellular phosphorylation. We herein report the application of phosphoramidate ProTide technology to bypass the rate-limiting initial phosphorylation of this nucleoside. Over 30 novel ProTides are reported, with variations in the aryl, ester, and amino acid regions. l-Alanine compounds are recognized as potent and selective inhibitors of HCV in replicon assay but lack rodent plasma stability despite considerable ester variation. Amino acid variation retaining the lead benzyl ester moiety gives an increase in rodent stability but at the cost of potency. Finally l-valine esters with ester variation lead to potent, stable compounds. Pharmacokinetic studies on these agents in the mouse reveal liver exposure to the bioactive triphosphate species following single oral dosing. Systemic exposure of the ProTide and parent nucleoside are low, indicating possible low toxicity in vivo, while liver concentrations of the active species may be predictive of efficacy in the clinic. This represents one of the most thorough cross-species studies of ProTides to date.Entities:
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Year: 2010 PMID: 20527890 DOI: 10.1021/jm1003792
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446