A [3+3] cyclization strategy for asymmetric synthesis of alkyl substituted piperidine-2-ones using 1,2-cyclic sulfamidates: A formal synthesis of (S)-coniine from l-norvaline

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2012

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Abstract

Regioselective ring-opening reactions of a set of representative 1,2-cyclic sulfamidates with lithium triethylorthopropiolate proceeded efficiently to deliver the corresponding δ-amino-α,β-unsaturated esters after acidic hydrolysis. Hydrogenation of the unsaturated esters and subsequent thermal cyclization afforded the related alkyl substituted piperidine-2-ones. This approach represents a novel [3+3] cyclization strategy for the asymmetric synthesis of alkyl substituted piperidin-2-ones. Efficiency of the cyclization process is illustrated by a formal asymmetric synthesis of (S)-coniine from l-norvaline. © 2012 Elsevier Ltd. All rights reserved.

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1,2 cyclic sulfamidate derivative , alkyl group , amide , amino acid , coniine , ester , lithium derivative , norvaline , piperidone derivative , unclassified drug , alkylation , annulation reaction , article , asymmetric synthesis , cyclization , hydrogenation , hydrolysis , nuclear Overhauser effect , priority journal , proton nuclear magnetic resonance , ring opening , stereochemistry , substitution reaction

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http://akademikarsiv.cbu.edu.tr:4000/handle/123456789/17507

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