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Fragment-based discovery of hepatitis C virus NS5b RNA polymerase inhibitors
Authors:Antonysamy Stephen S  Aubol Brandon  Blaney Jeff  Browner Michelle F  Giannetti Anthony M  Harris Seth F  Hébert Normand  Hendle Jörg  Hopkins Stephanie  Jefferson Elizabeth  Kissinger Charles  Leveque Vincent  Marciano David  McGee Ethel  Nájera Isabel  Nolan Brian  Tomimoto Masaki  Torres Eduardo  Wright Tobi
Affiliation:

aMedicinal Chemistry, SGX Pharmaceuticals, Inc., 10505 Roselle Street, San Diego, CA 92121, USA

bRoche Palo Alto, 3431 Hillview Avenue, Palo Alto, CA 94304, USA

Abstract:Non-nucleoside inhibitors of HCV NS5b RNA polymerase were discovered by a fragment-based lead discovery approach, beginning with crystallographic fragment screening. The NS5b binding affinity and biochemical activity of fragment hits and inhibitors was determined by surface plasmon resonance (Biacore) and an enzyme inhibition assay, respectively. Crystallographic fragment screening hits with 1–10 mM binding affinity (KD) were iteratively optimized to give leads with 200 nM biochemical activity and low μM cellular activity in a Replicon assay.
Keywords:HCV   NS5b   Fragment screening   Protein crystallography
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