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新型前列腺素F2α前药在眼组织中的体内活性及酶促水解作用

In-vivo activity and enzymatic hydrolysis of novel prostaglandin F2 alpha prodrugs in ocular tissues.

作者信息

Woodward D F, Chan M F, Cheng-Bennett A, Wheeler L A, Chen G, Burke J A, Kharlamb A, Lai R K, Shan T

机构信息

Department of Biological Sciences, Allergan, Inc., Irvine, CA 92715, USA.

出版信息

Exp Eye Res. 1996 Oct;63(4):411-23. doi: 10.1006/exer.1996.0131.

Abstract

Enzymatic hydrolysis and in-vivo ocular studies were performed on a novel series of prostaglandin F2 alpha (PGF2 alpha) pivaloyl ester prodrugs to assess their therapeutic potential. These novel PGF2 prodrugs were esterified at the 9-, 11-, and 15-OH positions. Their enzymatic hydrolysis rates were compared to PGF2 alpha 1-isopropyl ester in dog, monkey, and human ocular tissues. Intraocular pressure (IOP) studies were performed in monkeys and dogs, and ocular surface hyperemia was monitored in dogs. PGF2 alpha 9-monopivaloyl ester was not enzymatically hydrolysed in dog and human ocular tissues. PGF2 alpha 11- and 15-monopivaloyl esters and PGF2 alpha 11,15-dipivaloyl ester were converted to PGF2 alpha by all ocular tissues at a substantially slower rate than PGF2 alpha l-isopropyl ester. Despite their slow enzymatic hydrolysis rates, the ocular hypotensive activity of PGF2 alpha mono and dipivaloyl esters, where positions 11- and 15- were functionalized, closely approached the activity achieved with PGF2 alpha l-isopropyl ester. The degree of ocular surface hyperemia associated with PGF2 alpha 11-pivaloyl ester and PGF2 alpha 11,15-dipivaloyl ester was less than that associated with equivalent doses of PGF2 alpha l-isopropyl ester. It appears that rapid enzymatic hydrolysis rates are not necessary to obtain efficacious ocular hypotensive PGF2 alpha ester prodrugs. Slow enzymatic hydrolysis rates may assist in reducing the degree of ocular surface hyperemia. A further contributory factor in this regard could be the approximately ten-fold favorable difference in enzymatic hydrolysis rates between iris-ciliary body and conjunctival tissue for these novel pivaloyl esters of PGF2 alpha. These factors appear to translate into an improved therapeutic index for separating ocular hypotensive and ocular surface hyperemic effects.

摘要

对一系列新型前列腺素F2α(PGF2α)新戊酰酯前药进行了酶促水解和体内眼部研究,以评估其治疗潜力。这些新型PGF2前药在9-、11-和15-羟基位置进行了酯化。将它们的酶促水解速率与PGF2α 1-异丙酯在狗、猴和人眼组织中的水解速率进行了比较。在猴和狗身上进行了眼内压(IOP)研究,并在狗身上监测了眼表充血情况。PGF2α 9-单新戊酰酯在狗和人眼组织中未被酶促水解。PGF2α 11-和15-单新戊酰酯以及PGF2α 11,15-二新戊酰酯被所有眼组织转化为PGF2α的速率明显低于PGF2α 1-异丙酯。尽管它们的酶促水解速率较慢,但11-和15-位被官能化的PGF2α单新戊酰酯和二新戊酰酯的降眼压活性与PGF2α 1-异丙酯所达到的活性相近。与PGF2α 11-新戊酰酯和PGF2α 11,15-二新戊酰酯相关的眼表充血程度低于同等剂量的PGF2α 1-异丙酯。看来,要获得有效的降眼压PGF2α酯前药,快速的酶促水解速率并非必要。缓慢的酶促水解速率可能有助于降低眼表充血程度。在这方面的另一个促成因素可能是这些新型PGF2α新戊酰酯在虹膜睫状体和结膜组织之间的酶促水解速率存在约10倍的有利差异。这些因素似乎转化为了一个改善的治疗指数,用于区分降眼压和眼表充血效应。

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