Ti(II) and Rh(I) Complexes as Reagents toward a Thapsigargin Core
- PMID: 30964681
- DOI: 10.1021/acs.joc.8b03249
Ti(II) and Rh(I) Complexes as Reagents toward a Thapsigargin Core
Abstract
A novel approach toward the [5-7]fused bicyclic core of thapsigargin, a subnanomolar inhibitor of the endo/sarcoplasmic calcium ATPase (SERCA), is presented. The synthetic route includes an original Ti(II)-mediated hydroxy-directed reductive coupling of an enantiomerically enriched propargylic alcohol and an intramolecular Rh(I)-catalyzed cyclocarbonylation reaction as key steps. Interestingly, through the first experiments of titanocene-mediated reductive cyclization of a 1,8-enyne, a seven-membered cycle was isolated as a unique product with a total diastereoselectivity.
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