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The endo-lysosomal system of bEnd.3 and hCMEC/D3 brain endothelial cells

机译:bEnd.3和hCMEC / D3脑内皮细胞的溶酶体系统

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Brain endothelial cell-based in vitro models are among the most versatile tools in blood–brain barrier research for testing drug penetration to the central nervous system. Transcytosis of large pharmaceuticals across the brain capillary endothelium involves the complex endo-lysosomal system. This system consists of several types of vesicle, such as early, late and recycling endosomes, retromer-positive structures, and lysosomes. Since the endo-lysosomal system in endothelial cell lines of in vitro blood–brain barrier models has not been investigated in detail, our aim was to characterize this system in different models. For the investigation, we have chosen two widely-used models for in vitro drug transport studies: the bEnd.3 mouse and the hCMEC/D3 human brain endothelial cell line. We compared the structures and attributes of their endo-lysosomal system to that of primary porcine brain endothelial cells. We detected significant differences in the vesicular network regarding number, morphology, subcellular distribution and lysosomal activity. The retromer-positive vesicles of the primary cells were distinct in many ways from those of the cell lines. However, the cell lines showed higher lysosomal degradation activity than the primary cells. Additionally, the hCMEC/D3 possessed a strikingly unique ratio of recycling endosomes to late endosomes. Taken together our data identify differences in the trafficking network of brain endothelial cells, essentially mapping the endo-lysosomal system of in vitro blood–brain barrier models. This knowledge is valuable for planning the optimal route across the blood–brain barrier and advancing drug delivery to the brain.
机译:基于脑内皮细胞的体外模型是血脑屏障研究中最通用的工具,用于测试药物对中枢神经系统的渗透。大型药物跨脑毛细血管内皮细胞的胞吞作用涉及复杂的溶酶体系统。该系统由几种类型的囊泡组成,例如早期,晚期和回收内体,逆转录酶阳性结构和溶酶体。由于尚未详细研究体外血脑屏障模型的内皮细胞系中的溶酶体系统,因此我们的目的是在不同模型中表征该系统。为了进行调查,我们选择了两种广泛用于体外药物转运研究的模型:bEnd.3小鼠和hCMEC / D3人脑内皮细胞系。我们比较了它们的内溶酶体系统与原代猪脑内皮细胞的结构和属性。我们发现水泡网络在数量,形态,亚细胞分布和溶酶体活性方面存在显着差异。原代细胞的逆转录阳性细胞囊泡在许多方面与细胞系截然不同。然而,细胞系显示出比原代细胞更高的溶酶体降解活性。另外,hCMEC / D3具有回收内体与晚期内体的惊人的独特比例。综上所述,我们的数据确定了脑内皮细胞运输网络中的差异,从本质上绘制了体外血脑屏障模型的溶酶体系统。这些知识对于规划跨血脑屏障的最佳途径以及促进向大脑的药物输送非常有价值。

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