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Optimization of an in vitro bilayer model for studying the functional interplay between human?primary retinal pigment epithelial and choroidal endothelial cells isolated from donor eyes

机译:研究人原代视网膜色素上皮和从供体眼分离的脉络膜内皮细胞之间功能相互作用的体外双层模型的优化

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Abstract ObjectiveThe microenvironment of outer retina is largely regulated by retinal pigment epithelium (RPE) and choroid. Damage to either of these layers lead to the development of age related macular degeneration (AMD). A simplified cell culture model that mimics the RPE/Bruch’s membrane (BM) and choroidal layers of the eye is a prerequisite for elucidating the molecular mechanism of disease progression.ResultsWe have isolated primary retinal pigment epithelial cells (hRPE) and human primary choroidal endothelial cells (hCEC) from donor eyes to construct a bilayer of hCEC/hRPE on transwell inserts. Secretion of VEGF in the insert grown bilayer was significantly higher (22?pg/ml) than hCEC monolayer (3?pg/ml). To mimic the disease condition the model was treated with 100?ng/ml of VEGF, which increased the permeability of bilayer for 20?kDa FITC dextran while addition of bevacizumab, a humanized anti-VEGF drug, reversed the effect. To conclude the transwell insert based human primary hCEC/hRPE bilayer model would be an ideal system for studying the disease mechanisms and the crosstalk between RPE and choroid. This model will also be useful in screening small molecules and performing drug permeability kinetics.
机译:摘要目的外层视网膜的微环境主要受视网膜色素上皮(RPE)和脉络膜的调节。这些层中任一层的损坏都会导致年龄相关性黄斑变性(AMD)的发展。模拟RPE /布鲁赫膜(BM)和眼的脉络膜层的简化细胞培养模型是阐明疾病进展的分子机制的先决条件。结果我们分离了原代视网膜色素上皮细胞(hRPE)和人原代脉络膜内皮细胞(hCEC)来自供体的眼睛,以在transwell插入片段上构建双层hCEC / hRPE。插入生长双层中的VEGF分泌(22?pg / ml)明显高于hCEC单层(3?pg / ml)。为了模拟疾病状况,用100?ng / ml VEGF处理模型,该模型增加了双层对20?kDa FITC葡聚糖的渗透性,而加入人源化抗VEGF药物贝伐单抗则逆转了这种作用。结论是,基于transwell插入片段的人类主要hCEC / hRPE双层模型将是研究疾病机理以及RPE与脉络膜之间串扰的理想系统。该模型还将用于筛选小分子并进行药物渗透动力学。

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