Literature DB >> 21376717

Effect of PF-04217329 a prodrug of a selective prostaglandin EP(2) agonist on intraocular pressure in preclinical models of glaucoma.

Ganesh Prasanna1, Samantha Carreiro, Scott Anderson, Hovhannes Gukasyan, Soisurin Sartnurak, Husam Younis, David Gale, Cathie Xiang, Peter Wells, Dac Dinh, Chau Almaden, Jay Fortner, Carol Toris, Michael Niesman, Jennifer Lafontaine, Achim Krauss.   

Abstract

Better control of intraocular pressure (IOP) is the most effective way to preserve visual field function in glaucomatous patients. While prostaglandin FP analogs are leading the therapeutic intervention for glaucoma, new target classes also are being identified with new lead compounds being developed for IOP reduction. One target class currently being investigated includes the prostaglandin EP receptor agonists. Recently PF-04217329 (Taprenepag isopropyl), a prodrug of CP-544326 (active acid metabolite), a potent and selective EP(2) receptor agonist, was successfully evaluated for its ocular hypotensive activity in a clinical study involving patients with primary open angle glaucoma. In the current manuscript, the preclinical attributes of CP-544326 and PF-0421329 have been described. CP-544326 was found to be a potent and selective EP(2) agonist (IC(50) = 10 nM; EC(50) = 2.8 nM) whose corneal permeability and ocular bioavailability were significantly increased when the compound was dosed as the isopropyl ester prodrug, PF-04217329. Topical ocular dosing of PF-04217329 was well tolerated in preclinical species and caused an elevation of cAMP in aqueous humor/iris-ciliary body indicative of in vivo EP(2) target receptor activation. Topical ocular dosing of PF-04217329 resulted in ocular exposure of CP-544326 at levels greater than the EC(50) for the EP(2) receptor. PF-04217329 when dosed once daily caused between 30 and 50% IOP reduction in single day studies in normotensive Dutch-belted rabbits, normotensive dogs, and laser-induced ocular hypertensive cynomolgus monkeys and 20-40% IOP reduction in multiple day studies compared to vehicle-dosed eyes. IOP reduction was sustained from 6 h through 24 h following a single topical dose. In conclusion, preclinical data generated thus far appear to support the clinical development of PF-04217329 as a novel compound for the treatment of glaucoma.
Copyright © 2011 Elsevier Ltd. All rights reserved.

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Year:  2011        PMID: 21376717     DOI: 10.1016/j.exer.2011.02.015

Source DB:  PubMed          Journal:  Exp Eye Res        ISSN: 0014-4835            Impact factor:   3.467


  16 in total

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Review 5.  Prostaglandin analogues and nitric oxide contribution in the treatment of ocular hypertension and glaucoma.

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7.  Evaluation of WO 2012/177618 A1 and US-2014/0179750 A1: novel small molecule antagonists of prostaglandin-E2 receptor EP2.

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8.  The role of EP2 receptors in mediating the ultra-long-lasting intraocular pressure reduction by JV-GL1.

Authors:  Jacques A Bertrand; David F Woodward; Joseph M Sherwood; Jenny W Wang; Darryl R Overby
Journal:  Br J Ophthalmol       Date:  2020-11-25       Impact factor: 4.638

9.  Development of second generation EP2 antagonists with high selectivity.

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Authors:  Thota Ganesh
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