Studies on the Ocular Hypotensive Effects of Prostaglandin F2α Ester Prodrugs and Receptor Selective Prostaglandin Analogs

Abstract

The use of natural prostaglandins (PG), such as PGD₂, PGF₂, PGF_2α, and PGI₂, for treating glaucoma is limited by their ocular side effects. One approach to achieve the required separation of ocular hypotensive activity from side effects is to employ ester prodrugs. From a novel series of 11- and 15-mono and 11,15-diacyl esters of PGF_2α we identified prodrugs where PGF_2α formation rates in the iris-ciliary body exceeded those in the conjunctiva, sciera, and corneal endothelium. Compared to PGF_2α-1-isopropyl ester the ocular tissue hydrolysis rates of the 11-monopivaloyl, the 11,15-dipivaloyl ester and the 1,11-lactone were up to 1000 fold less. Despite this large disparity in hydrolysis rates, the pivaloyl esters and the 1,11-lactone were potent ocular hypotensives in our animal models. In studying prostaglandin analogs, we found that a diverse variety of prostanoid receptor selective agonists lowered intraocular pressure in dogs and/or monkeys. These included DP-, EP₁-, EP₂-, EP₃-, and FP-receptor selective compounds. These findings were surprising and prompted us to re-examine the receptor selectivity of these agonists by radioligand binding studies. Using radiolabelled PGE₂,17-phenyl PGF_2α, and sulprostone we were able to confirm the selectivity of the agonists currently used for receptor characterization directly by radioligand binding competition studies. It appears that multiple prostanoid receptor subtypes may be involved in regulating intraocular pressure.