Discovery of Ledipasvir (GS-5885): A Potent, Once-Daily Oral NS5A Inhibitor for the Treatment of Hepatitis C Virus Infection

John O. Link(Gilead Sciences (United States)), James G. Taylor(Gilead Sciences (United States)), Lianhong Xu(Gilead Sciences (United States)), Michael L. Mitchell(Gilead Sciences (United States)), Hongyan Guo(Gilead Sciences (United States)), Hongtao Liu(Gilead Sciences (United States)), Darryl Kato(Gilead Sciences (United States)), Thorsten Kirschberg(Gilead Sciences (United States)), Jianyu Sun(Gilead Sciences (United States)), Neil Squires(Gilead Sciences (United States)), Jay P. Parrish(Gilead Sciences (United States)), Terry Keller(Gilead Sciences (United States)), Zhengyu Yang(Gilead Sciences (United States)), Chris Yang(Gilead Sciences (United States)), Mike Matles(Gilead Sciences (United States)), Yujin Wang(Gilead Sciences (United States)), Kelly Wang(Gilead Sciences (United States)), Guofeng Cheng(Gilead Sciences (United States)), Tian Yang(Gilead Sciences (United States)), Erik Mogalian(Gilead Sciences (United States)), Elsa Mondou(Gilead Sciences (United States)), Melanie Cornpropst(Gilead Sciences (United States)), Jason K. Perry(Gilead Sciences (United States)), Manoj C. Desai(Gilead Sciences (United States))
Journal of Medicinal Chemistry
December 9, 2013
Cited by 292

Abstract

A new class of highly potent NS5A inhibitors with an unsymmetric benzimidazole-difluorofluorene-imidazole core and distal [2.2.1]azabicyclic ring system was discovered. Optimization of antiviral potency and pharmacokinetics led to the identification of 39 (ledipasvir, GS-5885). Compound 39 (GT1a replicon EC50 = 31 pM) has an extended plasma half-life of 37-45 h in healthy volunteers and produces a rapid >3 log viral load reduction in monotherapy at oral doses of 3 mg or greater with once-daily dosing in genotype 1a HCV-infected patients. 39 has been shown to be safe and efficacious, with SVR12 rates up to 100% when used in combination with direct-acting antivirals having complementary mechanisms.


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