Synthesis and Preliminary Biological Evaluation of Potent and Selective 2-(3-alkoxy-1-azetidinyl) Quinolines As Novel PDE10A Inhibitors with Improved Solubility

Overview

Journal Bioorg Med Chem

Specialties Biochemistry
Chemistry

Date 2014 Dec 3

PMID 25456383

Citations 2

Authors

Robert M Rzasa

Michael J Frohn

Kristin L Andrews

Samer Chmait

Ning Chen

Jeffrey G Clarine

Carl Davis

Heather A Eastwood

Daniel B Horne

Essa Hu

Adrie D Jones

Matthew R Kaller

Roxanne K Kunz

Silke Miller

Holger Monenschein

Thomas Nguyen

Alexander J Pickrell

Amy Porter

Andreas Reichelt

Xiaoning Zhao

James J S Treanor

Jennifer R Allen

Affiliations

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Abstract

We report the discovery of a novel series of 2-(3-alkoxy-1-azetidinyl) quinolines as potent and selective PDE10A inhibitors. Structure-activity studies improved the solubility (pH 7.4) and maintained high PDE10A activity compared to initial lead compound 3, with select compounds demonstrating good oral bioavailability. X-ray crystallographic studies revealed two distinct binding modes to the catalytic site of the PDE10A enzyme. An ex vivo receptor occupancy assay in rats demonstrated that this series of compounds covered the target within the striatum.

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