Publication | Closed Access
Ring-Closing Metathesis on Commercial Scale: Synthesis of HCV Protease Inhibitor Simeprevir
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Citations
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References
2019
Year
Key Macrocyclization StepEngineeringSynthetic VirologyMacrocyclization EfficiencyOrganic ChemistryChemistryAntiviral DrugAntiviral Drug DevelopmentCommercial ScaleBiochemistryVirologyCatalysisAntiviral CompoundBiomolecular EngineeringAlkene MetathesisRing-closing MetathesisAntiviral TherapyMedicineDrug DiscoveryClosing Metathesis
The key macrocyclization step in the synthesis of simeprevir, a hepatitis C virus (HCV) antiviral drug, was studied. N-Boc substitution on the diene precursor changes the site of insertion of the metathesis catalyst and, consequently, the kinetic model of the ring closing metathesis (RCM), enabling a further increase in the macrocyclization efficiency under simulated high dilution (SHD) conditions. NMR of the inserted species of both first and second generation RCM catalysts are reported and discussed.
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