Design, optimization, and in vivo evaluation of a series of pyridine derivatives with dual NK1 antagonism and SERT inhibition for the treatment of depression

Article ID	Journal	Published Year	Pages	File Type
10596014	Bioorganic & Medicinal Chemistry Letters	2013	5 Pages	PDF

Abstract

A series of substituted pyridines, ether linked to a phenylpiperidine core were optimized for dual NK1/SERT affinity. Optimization based on NK1/SERT binding affinities, and minimization of off-target ion channel activity lead to the discovery of compound 44. In vivo evaluation of 44 in the gerbil forced swim test (a depression model), and ex-vivo NK1/SERT receptor occupancy data support the potential of a dual acting compound for the treatment of depression.

Keywords

Receptor occupancy Depression

Related Topics

Physical Sciences and Engineering Chemistry Organic Chemistry

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Design, optimization, and in vivo evaluation of a series of pyridine derivatives with dual NK1 antagonism and SERT inhibition for the treatment of depression

Authors

Kevin W. Gillman, Michael F. Parker, Mark Silva, Andrew P. Degnan, George O. Tora, Nicholas J. Lodge, Yu-Wen Li, Snjezana Lelas, Matthew Taber, Rudolf G. Krause, Robert L. Bertekap, Amy E. Newton, Rick L. Pieschl, Kelly D. Lengyel, Kim A. Johnson,