A double ring closing metathesis reaction in the rapid, enantioselective synthesis of NK-1 receptor antagonists.

Debra J. Wallace,Jonathan M. Goodman,Derek J. Kennedy,Antony J. Davies,Cameron J. Cowden,Michael S. Ashwood,Ian F. Cottrell,Ulf H. Dolling,Paul J. Reider

A double ring closing metathesis reaction in the rapid, enantioselective synthesis of NK-1 receptor antagonists.

2001

Debra J. Wallace
Jonathan M. Goodman
Derek J. Kennedy
Antony J. Davies
Cameron J. Cowden
Michael S. Ashwood
Ian F. Cottrell
Ulf H. Dolling
Paul J. Reider

The NK-1 receptor antagonist 1 has been prepared in seven steps from phenylglycine methyl ester. The key steps are a double ring closing metathesis reaction of tetraene 7 to prepare spirocycle 6 and a reductive Heck reaction to introduce the aryl moiety. This latter reaction discriminates the olefins of compound 6 and proceeds in a highly regio- and stereoselective manner.

Keywords:

Moiety
Enantioselective synthesis
Stereochemistry
Receptor antagonist
Heck reaction
NK 1 Receptor Antagonists
Aryl
Ring-closing metathesis
Stereoselectivity
Chemistry
Organic chemistry
Salt metathesis reaction
double ring

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