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一种新型的人诱导多能干细胞血脑屏障模型:适用于研究抗体触发的受体介导的胞吞作用。

A novel human induced pluripotent stem cell blood-brain barrier model: Applicability to study antibody-triggered receptor-mediated transcytosis.

机构信息

Human Health Therapeutics Portfolio, National Research Council of Canada, Ottawa, ON, K1A 0R6, Canada.

出版信息

Sci Rep. 2018 Jan 30;8(1):1873. doi: 10.1038/s41598-018-19522-8.

Abstract

We have developed a renewable, scalable and transgene free human blood-brain barrier model, composed of brain endothelial cells (BECs), generated from human amniotic fluid derived induced pluripotent stem cells (AF-iPSC), which can also give rise to syngeneic neural cells of the neurovascular unit. These AF-iPSC-derived BECs (i-BEC) exhibited high transendothelial electrical resistance (up to 1500 Ω cm) inducible by astrocyte-derived molecular cues and retinoic acid treatment, polarized expression of functional efflux transporters and receptor mediated transcytosis triggered by antibodies against specific receptors. In vitro human BBB models enable pre-clinical screening of central nervous system (CNS)-targeting drugs and are of particular importance for assessing species-specific/selective transport mechanisms. This i-BEC human BBB model discriminates species-selective antibody- mediated transcytosis mechanisms, is predictive of in vivo CNS exposure of rodent cross-reactive antibodies and can be implemented into pre-clinical CNS drug discovery and development processes.

摘要

我们开发了一种可再生、可扩展且不含转基因的人血脑屏障模型,由源自人羊水的诱导多能干细胞(AF-iPSC)生成的脑内皮细胞(BEC)组成,这些细胞还可以产生神经血管单元的同种神经细胞。这些源自 AF-iPSC 的 BEC(i-BEC)在星形胶质细胞衍生的分子信号和视黄酸处理的诱导下表现出高跨内皮电阻(高达 1500Ωcm),具有功能性外排转运蛋白的极化表达和通过针对特定受体的抗体触发的受体介导的转胞吞作用。体外人 BBB 模型可用于中枢神经系统(CNS)靶向药物的临床前筛选,对于评估种特异性/选择性转运机制尤为重要。这种 i-BEC 人 BBB 模型可区分种特异性抗体介导的转胞吞作用机制,可预测啮齿动物交叉反应性抗体在体内 CNS 暴露情况,可应用于临床前 CNS 药物发现和开发过程。

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