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将Z310细胞用作体外血脑脊髓液屏障模型:紧密连接蛋白与转运特性

Use of Z310 cells as an in vitro blood-cerebrospinal fluid barrier model: tight junction proteins and transport properties.

作者信息

Shi Lewis Zhichang, Li G Jane, Wang Shunzhen, Zheng Wei

机构信息

School of Health Sciences, Purdue University, 550 Stadium Mall Drive, Room 1163D, West Lafayette, IN 47907-2051, United States.

出版信息

Toxicol In Vitro. 2008 Feb;22(1):190-9. doi: 10.1016/j.tiv.2007.07.007. Epub 2007 Jul 28.

Abstract

Immortalized rat choroidal epithelial Z310 cells have the potential to become an in vitro model for studying transport of materials at blood-cerebrospinal fluid barrier (BCB) (Shi and Zheng, 2005) [Shi, L.Z., Zheng, W., 2005. Establishment of an in vitro brain barrier epithelial transport system for pharmacological and toxicological study. Brain Research 1057, 37-48]. This study was designed to demonstrate the presence of tight junction properties in Z310 cells and the functionality of Z310 monolayer in transport of selected model compounds. Western blot analyses revealed the presence of claudin-1, ZO-1, and occludin in Z310 cells. Transmission electron microscopy showed a "tight junction" type of structure in the sub-apical lateral membranes between adjacent Z310 cells. Real-time RT-PCR revealed that Z310 cells expressed representative transporters such as DMT1, MTP1, TfR, p-glycoprotein, ATP7A, ZnT1, ABCC1, Oat3, OCT1 and OB-Ra. Moreover, Z310 cells cultured in a two-chamber Transwell device possessed the ability to transport zidovudine (anionic drug), thyroxine (hormone), thymidine (nucleoside), and leptin (large polypeptide) with kinetic properties similar to those obtained from the in vitro model based on primary culture of choroidal epithelial cells. Taken together, these data indicate that the Z310 BCB model expresses major tight junction proteins and forms a tight barrier in vitro. The model also exhibits the ability to transport substances of various categories across the barrier.

摘要

永生化大鼠脉络膜上皮Z310细胞有潜力成为研究血脑屏障(BCB)物质转运的体外模型(Shi和Zheng,2005年)[Shi,L.Z.,Zheng,W.,2005年。建立用于药理学和毒理学研究的体外脑屏障上皮转运系统。《脑研究》1057,37 - 48]。本研究旨在证明Z310细胞中紧密连接特性的存在以及Z310单层在所选模型化合物转运中的功能。蛋白质免疫印迹分析显示Z310细胞中存在闭合蛋白 - 1、紧密连接蛋白 - 1和闭合蛋白。透射电子显微镜显示相邻Z310细胞之间顶端下外侧膜存在“紧密连接”类型的结构。实时逆转录 - 聚合酶链反应显示Z310细胞表达代表性转运蛋白,如二价金属离子转运体1、微粒体甘油三酯转运蛋白1、转铁蛋白受体、P - 糖蛋白、ATP7A、锌转运体1、ABCC1、有机阴离子转运体3、有机阳离子转运体1和瘦素受体a。此外,在双室Transwell装置中培养的Z310细胞具有转运齐多夫定(阴离子药物)、甲状腺素(激素)、胸苷(核苷)和瘦素(大的多肽)的能力,其动力学特性与基于脉络膜上皮细胞原代培养的体外模型相似。综上所述,这些数据表明Z310 BCB模型表达主要的紧密连接蛋白并在体外形成紧密屏障。该模型还表现出跨屏障转运各类物质的能力。

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