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3
Development of a high-throughput brain slice method for studying drug distribution in the central nervous system.一种用于研究药物在中枢神经系统中分布的高通量脑片方法的开发。
Drug Metab Dispos. 2009 Jun;37(6):1226-33. doi: 10.1124/dmd.108.026377. Epub 2009 Mar 19.
4
Cassette analysis of eight beta-blockers in bovine eye sclera, choroid-RPE, retina, and vitreous by liquid chromatography-tandem mass spectrometry.通过液相色谱-串联质谱法对牛眼巩膜、脉络膜-视网膜色素上皮、视网膜和玻璃体中的八种β受体阻滞剂进行盒式分析。
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Roles of inner blood-retinal barrier organic anion transporter 3 in the vitreous/retina-to-blood efflux transport of p-aminohippuric acid, benzylpenicillin, and 6-mercaptopurine.视网膜内血屏障有机阴离子转运体3在对氨基马尿酸、苄青霉素和6-巯基嘌呤从玻璃体/视网膜到血液的外流转运中的作用。
J Pharmacol Exp Ther. 2009 Apr;329(1):87-93. doi: 10.1124/jpet.108.146381. Epub 2008 Dec 30.
6
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Gene expression profiles of human trabecular meshwork cells induced by triamcinolone and dexamethasone.曲安奈德和地塞米松诱导的人小梁网细胞的基因表达谱
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Modeling of corneal and retinal pharmacokinetics after periocular drug administration.眼周给药后角膜和视网膜药代动力学的建模
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脂溶性对药物向巩膜、脉络膜-视网膜色素上皮、视网膜、小梁网和视神经分配的影响。

Influence of lipophilicity on drug partitioning into sclera, choroid-retinal pigment epithelium, retina, trabecular meshwork, and optic nerve.

机构信息

Department of Pharmaceutical Sciences, University of Colorado Denver, 12700 E 19th Ave., Aurora, CO 80045, USA.

出版信息

J Pharmacol Exp Ther. 2010 Mar;332(3):1107-20. doi: 10.1124/jpet.109.161570. Epub 2009 Nov 19.

DOI:10.1124/jpet.109.161570
PMID:19926800
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2835449/
Abstract

In vitro bovine eye tissue/phosphate-buffered saline, pH 7.4, partition coefficients (Kt:b), in vitro binding to natural melanin, and in vivo delivery at 1 h after posterior subconjunctival injection in Brown Norway rats were determined for eight beta-blockers. The Kt:b was in the order intact tissue, dry weight method >or= intact tissue, wet weight method corrected for tissue water and drug in tissue water >> intact tissue, wet weight method > homogenized tissue. In intact tissue methods, Kt:b followed the order choroid-retinal pigment epithelium (RPE) > trabecular meshwork > retina > sclera approximately optic nerve; propranolol > betaxolol > pindolol approximately timolol approximately metoprolol > sotalol approximately atenolol approximately nadolol. Intact tissue, wet weight log (Kt:b) correlated positively with log D for all tissues (R(2) of 0.7-0.9). Log (melanin binding capacity) correlated positively with choroid-RPE log (Kt:b) (R(2) of 0.5). With an increase in concentration, Kt:b decreased in trabecular meshwork for all beta-blockers and for some lipophilic beta-blockers in choroid-RPE and sclera. With an increase in drug lipophilicity, in vivo tissue distribution increased in choroid-RPE, iris-ciliary body, sclera, and cornea but exhibited a declining trend in retina, vitreous, and lens. In vitro bovine intact tissue, wet weight Kt:b correlated positively with rat in vivo tissue/vitreous humor distribution for sclera, choroid-RPE, and retina (R(2) of 0.985-0.993). In vitro tissue partition coefficients might be useful in predicting in vivo drug distribution after trans-scleral delivery. Less lipophilic solutes exhibiting limited nonproductive binding in choroid-RPE might exhibit greater trans-scleral delivery to the retina and vitreous.

摘要

在体外牛眼组织/磷酸盐缓冲盐水,pH7.4,分配系数(Kt:b),在体外与天然黑色素结合,并在布朗挪威大鼠后结膜下注射后 1 小时体内给药,对 8 种β受体阻滞剂进行了测定。Kt:b 的顺序为完整组织,干重法≥完整组织,湿重法校正组织水和组织水中的药物>>完整组织,湿重法>匀浆组织。在完整组织方法中,Kt:b 的顺序为脉络膜-视网膜色素上皮(RPE)>小梁网>视网膜>巩膜≈视神经;普萘洛尔>倍他洛尔>吲哚洛尔≈噻吗洛尔≈美托洛尔>索他洛尔≈阿替洛尔≈纳多洛尔。完整组织,湿重对数(Kt:b)与所有组织的 log D 呈正相关(R(2)为 0.7-0.9)。Log(黑色素结合能力)与脉络膜-RPE log(Kt:b)呈正相关(R(2)为 0.5)。随着浓度的增加,所有β受体阻滞剂在小梁网中,以及一些亲脂性β受体阻滞剂在脉络膜-RPE 和巩膜中,Kt:b 降低。随着药物亲脂性的增加,在体内组织分布在脉络膜-RPE、虹膜睫状体、巩膜和角膜中增加,但在视网膜、玻璃体液和晶状体中呈下降趋势。在体外牛完整组织,湿重 Kt:b 与大鼠体内组织/玻璃体液分布呈正相关,用于巩膜、脉络膜-RPE 和视网膜(R(2)为 0.985-0.993)。体外组织分配系数可能有助于预测经巩膜给药后体内药物分布。在脉络膜-RPE 中表现出有限的非生产性结合的亲脂性较小的溶质可能会向视网膜和玻璃体表现出更大的经巩膜传递。