Discovery of SAR184841, a potent and long-lasting inhibitor of 11β-hydroxysteroid dehydrogenase type 1, active in a physiopathological animal model of T2D

Olivier Venier,Cecile Pascal,Alain Braun,Claudie Namane,Patrick Mougenot,Olivier Crespin,François Pacquet,Cécile Mougenot,Catherine Monseau,Bénédicte Onofri,Rommel Dadji-Faïhun,Céline Leger,Majdi Ben-Hassine,Thao Van-Pham,Jean-Luc Ragot,Christophe Philippo,Geraldine Farjot,Lionel Noah,Karima Maniani,Asma Boutarfa,Eric Nicolai,Etienne Guillot,Marie-Pierre Pruniaux,Stefan Güssregen,Christian Engel,Anne-Laure Coutant,Beatriz de Miguel,Antonio Castro

Discovery of SAR184841, a potent and long-lasting inhibitor of 11β-hydroxysteroid dehydrogenase type 1, active in a physiopathological animal model of T2D

2013

Starting from 11β-HSD1 inhibitors that were active ex vivo but with Cyp 3A4 liability, we obtained a new series of adamantane ureas displaying potent inhibition of both human and rodent 11β-HSD1 enzymes, devoid of Cyp 3A4 interactions, and rationally designed to provide long-lasting inhibition in target tissues. Final optimizations lead to SAR184841 with good oral pharmacokinetic properties showing in vivo activity and improvement of metabolic parameters in a physiopathological model of type 2 diabetes.

Keywords:

Enzyme
Animal model
11β-hydroxysteroid dehydrogenase type 1
In vivo
Ex vivo
Biochemistry
Biology
Chemistry
Pharmacology
Adamantane
Pharmacokinetics
long lasting

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