Discovery, Optimization, and Characterization of Novel Chlorcyclizine Derivatives for the Treatment of Hepatitis C Virus Infection
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posted on 2016-02-04, 17:55 authored by Shanshan He, Jingbo Xiao, Andrés E. Dulcey, Billy Lin, Adam Rolt, Zongyi Hu, Xin Hu, Amy Q. Wang, Xin Xu, Noel Southall, Marc Ferrer, Wei Zheng, T. Jake Liang, Juan J. MaruganRecently,
we reported that chlorcyclizine (CCZ, Rac-2), an over-the-counter
antihistamine piperazine drug, possesses in vitro and in vivo activity against hepatitis
C virus. Here, we describe structure–activity relationship
(SAR) efforts that resulted in the optimization of novel chlorcyclizine
derivatives as anti-HCV agents. Several compounds exhibited EC50 values below 10 nM against HCV infection, cytotoxicity selectivity
indices above 2000, and showed improved in vivo pharmacokinetic
properties. The optimized molecules can serve as lead preclinical
candidates for the treatment of hepatitis C virus infection and as
probes to study hepatitis C virus pathogenesis and host–virus
interaction.
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hepatitis C virus infectionCCZ10 nMcytotoxicity selectivity indicesantihistamine piperazine drugHCV infectionoptimized moleculeshepatitis C virusnovel chlorcyclizine derivativesSARvivo pharmacokinetic propertiesNovel Chlorcyclizine Derivativesvivo activityEC 50 valuesstudy hepatitis C virus pathogenesisHepatitis C Virus InfectionRecentlySeveral compounds
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