Discovery of Novel Seven-Membered Prostacyclin Analogues as Potent and Selective Prostaglandin FP and EP3 Dual Agonists

Isamu Sugimoto,Tohru Kambe,Tomotaka Okino,Tetsuo Obitsu,Nobukazu Ohta,Taihei Nishiyama,Akihiro Kinoshita,Taku Fujimoto,Hiromu Egashira,Shinsaku Yamane,Satoshi Shuto,Kousuke Tani,Toru Maruyama

Discovery of Novel Seven-Membered Prostacyclin Analogues as Potent and Selective Prostaglandin FP and EP3 Dual Agonists

2017

Isamu Sugimoto
Tohru Kambe
Tomotaka Okino
Tetsuo Obitsu
Nobukazu Ohta
Taihei Nishiyama
Akihiro Kinoshita
Taku Fujimoto
Hiromu Egashira
Shinsaku Yamane
Satoshi Shuto
Kousuke Tani
Toru Maruyama

A novel series of prostaglandin analogues with a seven-membered ring scaffold was designed, synthesized, and evaluated for the functional activation of prostaglandin receptors to identify potent and subtype-selective FP and EP3 dual agonists. Starting from the prostacyclin derivative 5b, a nonselective agonist for prostaglandin receptors, replacement of the core structure with an octahydro-2H-cyclopenta[b]oxepine scaffold led to the discovery of the potent and selective FP and EP3 dual agonist 11b as a lead compound for the development of an antiglaucoma agent.

Keywords:

Pharmacology
Biology
Lead compound
FP receptor
Biochemistry
Prostacyclin
Agonist
Prostaglandin E receptor 3
Prostaglandin
Stereochemistry
G protein-coupled receptor
Receptor
ep3 receptor

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