Sulfonamides as Selective NaV1.7 Inhibitors: Optimizing Potency and Pharmacokinetics to Enable in Vivo Target Engagement

Isaac E. Marx,Thomas Dineen,Jessica Able,Christiane Bode,Howard Bregman,Margaret Y. Chu-Moyer,Erin F. DiMauro,Bingfan Du,Robert S. Foti,Robert T. Fremeau,Hua Gao,Hakan Gunaydin,Brian E. Hall,Liyue Huang,Thomas Kornecook,Charles Kreiman,Daniel S. La,Joseph Ligutti,Min-Hwa Jasmine Lin,Dong Liu,Jeff S. McDermott,Bryan D. Moyer,Emily A. Peterson,Jonathan Roberts,Paul Rose,Jean Wang,Beth D. Youngblood,Violeta Yu,Matthew Weiss

Sulfonamides as Selective NaV1.7 Inhibitors: Optimizing Potency and Pharmacokinetics to Enable in Vivo Target Engagement

2016

Human genetic evidence has identified the voltage-gated sodium channel NaV1.7 as an attractive target for the treatment of pain. We initially identified naphthalene sulfonamide 3 as a potent and selective inhibitor of NaV1.7. Optimization to reduce biliary clearance by balancing hydrophilicity and hydrophobicity (Log D) while maintaining NaV1.7 potency led to the identification of quinazoline 16 (AM-2099). Compound 16 demonstrated a favorable pharmacokinetic profile in rat and dog and demonstrated dose-dependent reduction of histamine-induced scratching bouts in a mouse behavioral model following oral dosing.

Keywords:

Pharmacology
Biology
In vivo
Potency
Quinazoline
Pharmacokinetics
Nav1.5
NAV1
Chemistry
Dosing
Sodium channel

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