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    The Discovery of GS-9669, a Thumb Site II Non-nucleoside Inhibitor of NS5B for the Treatment of Genotype 1 Chronic Hepatitis C Infection

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    Date
    2013-11-06
    Author
    Lazerwith, SE
    Lew, W
    Zhang, J
    Morganelli, P
    Liu, Q
    Canales, E
    Clarke, MO
    Doerffler, E
    Byun, D
    Mertzman, M
    Ye, H
    Chong, L
    Xu, L
    Appleby, T
    Chen, X
    Fenaux, M
    Hashash, A
    Leavitt, SA
    Mabery, E
    Matles, M
    Mwangi, Julius W.
    Tian, Y
    Lee, YJ
    Zhang, J
    Zhu, C
    Murray, BP
    Watkins, WJ
    Type
    Article
    Language
    en
    Metadata
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    Abstract
    Investigation of thiophene-2-carboxylic acid HCV NS5B site II inhibitors, guided by measurement of cell culture medium binding, revealed the structure-activity relationships for intrinsic cellular potency. The pharmacokinetic profile was enhanced through incorporation of heterocyclic ethers on the N-alkyl substituent. Hydroxyl groups were incorporated to modulate protein binding. Intrinsic potency was further improved through enantiospecific introduction of an olefin in the N-acyl motif, resulting in the discovery of the phase 2 clinical candidate GS-9669. The unexpected activity of this compound against the clinically relevant NS5B M423T mutant, relative to the wild type, was shown to arise from both the N-alkyl substituent and the N-acyl group.
    URI
    http://www.ncbi.nlm.nih.gov/pubmed/24144213
    http://erepository.uonbi.ac.ke:8080/xmlui/handle/123456789/58325
    Citation
    J Med Chem. 2013 Nov 6. [Epub ahead of print]
    Publisher
    University of Nairobi
     
    Department of Pharmacology And Pharmacognosy
     
    Collections
    • College of Health Sciences (CHS) [88]

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