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视网膜色素上皮细胞中溴莫尼定转运的特性研究

Characterization of brimonidine transport in retinal pigment epithelium.

作者信息

Zhang Ning, Kannan Ram, Okamoto Curtis T, Ryan Stephen J, Lee Vincent H L, Hinton David R

机构信息

Department of Pharmaceutical Sciences, School of Pharmacy, University of Southern California, Los Angeles, CA, USA.

出版信息

Invest Ophthalmol Vis Sci. 2006 Jan;47(1):287-94. doi: 10.1167/iovs.05-0189.

Abstract

PURPOSE

To investigate the involvement of carrier-mediated transport mechanisms in brimonidine transport in retinal pigment epithelium (RPE).

METHODS

The transport of [3H]-brimonidine in bovine RPE-choroid explants was evaluated in a modified Ussing chamber. The uptake of [3H]brimonidine was evaluated in differentiated ARPE-19 cells cultured on permeable transwell filters.

RESULTS

The transport of brimonidine into (choroid-to-retina transport [inward]) and out of (retina-to-choroid transport [outward]) the eye in bovine RPE-choroid explants was temperature dependent. Both inward and outward brimonidine transport decreased at 5 microM compared with 10 nM. The melanin pigmentation of RPE did not significantly affect tissue permeability at either brimonidine dose. A saturable component was identified for the inward transport with the apparent Michaelis-Menten constant and a maximum transport rate of 51 microM and 148 pmol/(cm2 x h), respectively. Both apical (representing retina-to-choroid transport) and basolateral (representing choroid-to-retina transport) brimonidine uptake in ARPE-19 cells showed temperature dependence. Apical uptake was higher than basolateral uptake at 37 degrees C and was decreased to 70% in the presence of NaN3 or in the absence of extracellular Na+. Besides alpha2-agonists, apical uptake was inhibited by verapamil, desipramine, and quinidine, but not by MPP+ (1-methyl-4-phenylpyridinium), TEA (tetraethylammonium), decynium-22, carnitine, PHA (p-aminohippurate), alanine, or inosine. Basolateral brimonidine uptake increased by 35% at extracellular pH of 6 and decreased by 50% under cell-depolarized conditions of high medium K+ and 1 microM valinomycin. Temperature-dependent components of basolateral uptake were not saturated at doses up to 2 mM.

CONCLUSIONS

A carrier-mediated transport process for brimonidine in RPE was demonstrated in bovine RPE-choroid explants and polarized ARPE-19 cells. This transport system may play a significant role in modulating the movement of brimonidine into and out of the eye.

摘要

目的

研究载体介导的转运机制在视网膜色素上皮(RPE)中溴莫尼定转运过程中的作用。

方法

在改良的Ussing室中评估[3H] - 溴莫尼定在牛RPE - 脉络膜外植体中的转运。在可渗透的Transwell滤器上培养的分化ARPE - 19细胞中评估[3H]溴莫尼定的摄取。

结果

在牛RPE - 脉络膜外植体中,溴莫尼定进入眼内(脉络膜到视网膜的转运[内向])和流出眼外(视网膜到脉络膜的转运[外向])的过程均依赖于温度。与10 nM相比,在5 μM时内向和外向的溴莫尼定转运均降低。在两种溴莫尼定剂量下,RPE的黑色素沉着均未显著影响组织通透性。确定内向转运存在一个可饱和成分,其表观米氏常数和最大转运速率分别为51 μM和148 pmol/(cm2·h)。ARPE - 19细胞中顶端(代表视网膜到脉络膜的转运)和基底外侧(代表脉络膜到视网膜的转运)的溴莫尼定摄取均显示出温度依赖性。在37℃时,顶端摄取高于基底外侧摄取,在存在NaN3或无细胞外Na+时降低至70%。除α2 - 激动剂外,顶端摄取还受到维拉帕米、地昔帕明和奎尼丁的抑制,但不受1 - 甲基 - 4 - 苯基吡啶鎓(MPP+)、四乙铵(TEA)、癸甲氯铵 - 22、肉碱、对氨基马尿酸(PHA)、丙氨酸或肌苷的抑制。在细胞外pH为6时,基底外侧溴莫尼定摄取增加35%,在高钾培养基和1 μM缬氨霉素的细胞去极化条件下降低50%。在高达2 mM的剂量下,基底外侧摄取的温度依赖性成分未达到饱和。

结论

在牛RPE - 脉络膜外植体和极化的ARPE - 19细胞中证实了RPE中存在载体介导的溴莫尼定转运过程。该转运系统可能在调节溴莫尼定进出眼内的运动中起重要作用。

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