Preparation of 3,5-Methanobenzo[ b]azepines: An sp3-Rich Quinolone Isostere

Loïc Herter; Timothé Perrin; Thomas Fessard; Christophe Salomé

doi:10.1021/acs.orglett.3c02250

Preparation of 3,5-Methanobenzo[ b]azepines: An sp³-Rich Quinolone Isostere

Org Lett. 2023 Aug 25;25(33):6161-6166. doi: 10.1021/acs.orglett.3c02250. Epub 2023 Aug 13.

Authors

Loïc Herter^{1

2}, Timothé Perrin¹, Thomas Fessard¹, Christophe Salomé¹

Affiliations

¹ SpiroChem, Rosental area, WRO-1047-3, Mattenstrasse 22, 4058 Basel, Switzerland.
² Bio-Functional Chemistry (UMR 7199), LabEx Medalis, University of Strasbourg, 74 Route du Rhin, Illkirch-Graffenstaden 67400, France.

PMID: 37573582
DOI: 10.1021/acs.orglett.3c02250

Abstract

The replacement of the aromatic ring in bioactive compounds with saturated bioisosteres has become a popular tactic to obtain novel structures with improved physicochemical profiles. In this paper, we describe an efficient synthesis of 3,5-methanobenzo[b]azepine analogues and suggest them as isosteres of quinolones. Quinolones are heteroaromatic, flat rings and considered as privileged scaffolds. An isosteric version of this scaffold with more 3D character would offer new options to expand their use.