![Author ORCID: We display the ORCID iD icon alongside authors names on our website to acknowledge that the ORCiD has been authenticated when entered by the user. To view the users ORCiD record click the icon. [opens in a new tab]](https://www.cambridge.org/engage/assets/public/coe/logo/orcid.png){kind=logo}
Abstract
A reliable methodology for the multigram preparation of diastereomerically enriched 3,6-disubstituted bicyclo[3.2.0]heptane building blocks is proposed. The strategy is based on [2 + 2] cycloaddition of 3-substituted cyclopentene derivatives and dichloroketene followed by a diastereoselective reduction reaction. Despite both steps lacked stereospecificity, the target bicyclic building blocks (including amino acids and amino alcohols) could be obtained as pure (1R*,3R*,5S*,6R*) (exo,exo) or (1R*,3R*,5S*,6R*) (exo,endo) isomers on up to 34.4 g scale. Structural characterization of the title scaffolds using exit vector plot (EVP) formalism showed their potential for cycloalkane/benzene isosteric replacements in medicinal chemistry.
Supplementary materials
Title
Supporting Information
Description
Supporting Information containing experimental details and copies of spectra.
Actions
