Issue 6, 2000

Synthesis and structure–activity studies of 8α- and 9β-analogues of 14,17-ethanoestradiol

Abstract

Synthetic routes to the title compounds are described, commencing with readily available 19-norsteroid precursors. The reaction of 3-methoxy-8α-estra-1,3,5(10),14,16-pentaen-17-yl acetate 3 with phenyl vinyl sulfone at 150 °C proceeded in high yield, but with poor selectivity, to give a mixture of 14α,17-cycloadducts, which underwent convergent functional group modification, to furnish 14α,17α-ethano-8α-estradiol 13. The feasibility of performing similar cycloaddition chemistry on analogous 9β-precursors was demonstrated, but the preferred synthetic route entailed configurational inversion at C-9, of 14α,17α-ethanoestradiol 25, via moderately stereoselective hydrogenation of a 9,11-dehydro intermediate, leading to 14α,17α-ethano-9β-estradiol 32. The estrogen receptor binding affinities of 13 and 32 are reported, and discussed in terms of superimpositional modelling on estradiol.

Article information

Article type
Paper
Submitted
19 Oct 1999
Accepted
23 Dec 1999
First published
07 Mar 2000

J. Chem. Soc., Perkin Trans. 1, 2000, 1003-1013

Synthesis and structure–activity studies of 8α- and 9β-analogues of 14,17-ethanoestradiol

J. R. Bull and P. D. de Koning, J. Chem. Soc., Perkin Trans. 1, 2000, 1003 DOI: 10.1039/A908375H

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