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  • Optimization of a Novel Quinazolinone-Based Series of Transient Receptor Potential A1 (TRPA1) Antagonists Demonstrating Potent in Vivo Activity.

Optimization of a Novel Quinazolinone-Based Series of Transient Receptor Potential A1 (TRPA1) Antagonists Demonstrating Potent in Vivo Activity.

Journal of medicinal chemistry (2016-03-05)
Laurie B Schenkel, Philip R Olivieri, Alessandro A Boezio, Holly L Deak, Renee Emkey, Russell F Graceffa, Hakan Gunaydin, Angel Guzman-Perez, Josie H Lee, Yohannes Teffera, Weiya Wang, Beth D Youngblood, Violeta L Yu, Maosheng Zhang, Narender R Gavva, Sonya G Lehto, Stephanie Geuns-Meyer
RESUMEN

There has been significant interest in developing a transient receptor potential A1 (TRPA1) antagonist for the treatment of pain due to a wealth of data implicating its role in pain pathways. Despite this, identification of a potent small molecule tool possessing pharmacokinetic properties allowing for robust in vivo target coverage has been challenging. Here we describe the optimization of a potent, selective series of quinazolinone-based TRPA1 antagonists. High-throughput screening identified 4, which possessed promising potency and selectivity. A strategy focused on optimizing potency while increasing polarity in order to improve intrinsic clearance culminated with the discovery of purinone 27 (AM-0902), which is a potent, selective antagonist of TRPA1 with pharmacokinetic properties allowing for >30-fold coverage of the rat TRPA1 IC50 in vivo. Compound 27 demonstrated dose-dependent inhibition of AITC-induced flinching in rats, validating its utility as a tool for interrogating the role of TRPA1 in in vivo pain models.

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Sigma-Aldrich
AM-0902, ≥98% (HPLC)