Rhodium-catalysed vinyl 1,4-conjugate addition coupled with Sharpless asymmetric dihydroxylation in the synthesis of the CDE ring fragment of pectenotoxin-4

Melodie S W Richardson; Christopher J Tame; Darren L Poole; Timothy J Donohoe

doi:10.1039/c9sc01761e

Rhodium-catalysed vinyl 1,4-conjugate addition coupled with Sharpless asymmetric dihydroxylation in the synthesis of the CDE ring fragment of pectenotoxin-4

Chem Sci. 2019 May 24;10(25):6336-6340. doi: 10.1039/c9sc01761e. eCollection 2019 Jul 7.

Authors

Melodie S W Richardson¹, Christopher J Tame², Darren L Poole², Timothy J Donohoe¹

Affiliations

¹ Department of Chemistry , University of Oxford , Chemistry Research Laboratory , Mansfield Road , Oxford , OX1 3TA , UK . Email: timothy.donohoe@chem.ox.ac.uk.
² GlaxoSmithKline Medicines Research Centre , Gunnels Wood Road , Stevenage , SG1 2NY , UK.

Abstract

Our synthesis of the CDE ring fragment of pectenotoxin-4 utilised two key steps to make the complex bicyclic ketal unit: (i) a rhodium-catalysed vinyl group 1,4-addition as the major C-C bond forming step; (ii) a stereoselective Sharpless Asymmetric Dihydroxylation (SAD) of the resulting 1,1-disubstituted homoallylic alcohol. Subsequent acid-catalysed cyclisation afforded the desired [5,6]-bicyclic ketal of the target molecule. This methodology was shown to be compatible with the desired E ring fragment 35 in order to construct the CDE fragment 37 of pectenotoxin-4.