In the context of aprogramme directed at the manufacture of telaprevir, eight possible approaches to its bicyclic alpha-amino acid core, based on organocatalytic enantioselective conjugate additionstocyclopent-1-enecarbaldehyde, were identified and preliminarily explored. Four reactions, delivering advanced intermediates en route to the target amino acid, were selected for athorough optimisation. Three of this reactions involved iminium ion catalysis with a prolinol catalyst(addition of nitromethane, nitroacetate and acetamidomalonate) and one was based on a Cinchona-derived phase-transfer catalyst (addition of glycine imines). A careful choice of additives allowed lowering of the catalyst loading to 0.5 mol % in some cases. The preparation of intermediates that would give access to the core of telaprevir in good yields and enantioselectivities by exploiting readily available substrates and catalysts, highlights the potential of organocatalytic technology for a cost-effective preparation of pharmaceuticals.
Luca Bernardi, Mariafrancesca Fochi, Riccardo Carbone, Ada Martinelli, Martin E. Fox, Christopher J. Cobley, et al. (2015). Organocatalytic asymmetric conjugate additions to cyclopent-1-enecarbaldehyde: a critical assessment of organocatalytic approaches towards the telaprevir bicyclic core. CHEMISTRY, 21, 19208-19222 [10.1002/chem.201503352].
Organocatalytic asymmetric conjugate additions to cyclopent-1-enecarbaldehyde: a critical assessment of organocatalytic approaches towards the telaprevir bicyclic core
BERNARDI, LUCA;FOCHI, MARIAFRANCESCA;Ada Martinelli;
2015
Abstract
In the context of aprogramme directed at the manufacture of telaprevir, eight possible approaches to its bicyclic alpha-amino acid core, based on organocatalytic enantioselective conjugate additionstocyclopent-1-enecarbaldehyde, were identified and preliminarily explored. Four reactions, delivering advanced intermediates en route to the target amino acid, were selected for athorough optimisation. Three of this reactions involved iminium ion catalysis with a prolinol catalyst(addition of nitromethane, nitroacetate and acetamidomalonate) and one was based on a Cinchona-derived phase-transfer catalyst (addition of glycine imines). A careful choice of additives allowed lowering of the catalyst loading to 0.5 mol % in some cases. The preparation of intermediates that would give access to the core of telaprevir in good yields and enantioselectivities by exploiting readily available substrates and catalysts, highlights the potential of organocatalytic technology for a cost-effective preparation of pharmaceuticals.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
