Synthesis of 9(0)-Methano-Δ6(9α)-PGI1: The highly potent carbon analog of prostacyclin

A synthesis of dl-9(O)-methano-A 6(9a)\_pGI 1 (1\_), a more potent prostacyclin analog than carbacyclin, has been accomplished utilizing regiocontrolled transformation of the enone to the olefin via the allylsilane as a key step.

A key intermediate for the synthesis of isocarbacyclin, a promising therapeutic agent for cardiovascular and circulatory disorders, has been synthesized from (&J-(+)-methyl 2-oxo-l-cyclopentaneacetate by employing rhodium(II)-catalyzed intramolecular C-H insertion reaction of a-diazo B-keto ester as

The first total synthesis of the carbon analog of 6,9a-oxido-lla,lSadihydroprosta-6( 7),13E-dienoic acid ( A6-~Il ) is described starting from 1,3-cyclooctadiene.

## (O)-methano-A 6(9a)_pGI has been synthesized by utilizing the regiocontrolled cleavage of the B-propio&one tiith the dialkylaluminum acetylide.

A method for the conversion of aldehydes to acetylenes via I-alkenylstannanes is reported, including its application to the synthesis of 9(O)-thia-A6-PCIl. In connection with studies directed toward the synthesis of prostacyclin analogs, it was required to develop a mild method for the transformati