A Visible‐Light‐Mediated Radical Smiles Rearrangement and its Application to the Synthesis of a Difluoro‐Substituted Spirocyclic ORL‐1 Antagonist | Zendy

Douglas James J. | Zendy; Albright Haley | Zendy; Sevrin Martin J. | Zendy; Cole Kevin P. | Zendy; Stephenson Corey R. J. | Zendy

Premium

A Visible‐Light‐Mediated Radical Smiles Rearrangement and its Application to the Synthesis of a Difluoro‐Substituted Spirocyclic ORL‐1 Antagonist

Author(s) -

Douglas James J.,

Albright Haley,

Sevrin Martin J.,

Cole Kevin P.,

Stephenson Corey R. J.

Publication year - 2015

Publication title -

angewandte chemie international edition

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 5.831

H-Index - 550

eISSN - 1521-3773

pISSN - 1433-7851

DOI - 10.1002/anie.201507369

Subject(s) - moiety , chemistry , antagonist , combinatorial chemistry , aryl , catalysis , stereochemistry , functional group , photochemistry , receptor , organic chemistry , biochemistry , alkyl , polymer

A visible‐light‐mediated radical Smiles rearrangement has been developed to address the challenging synthesis of the gem ‐difluoro group present in an opioid receptor‐like 1 (ORL‐1) antagonist that is currently in development for the treatment of depression and/or obesity. This method enables the direct and efficient introduction of the difluoroethanol motif into a range of aryl and heteroaryl systems, representing a new disconnection for the synthesis of this versatile moiety. When applied to the target compound, the photochemical step could be conducted on 15 g scale using industrially relevant [Ru(bpy) 3 Cl 2 ] catalyst loadings of 0.01 mol %. This transformation is part of an overall five‐step route to the antagonist that compares favorably to the current synthetic sequence and demonstrates, in this specific case, a clear strategic benefit of photocatalysis.

This content is not available in your region!

Continue researching here.

Having issues? You can contact us here

Accelerating Research