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Wnt 激活永生化脑内皮细胞作为体外血脑屏障标准化模型的工具。

Wnt activation of immortalized brain endothelial cells as a tool for generating a standardized model of the blood brain barrier in vitro.

机构信息

IFOM-FIRC Institute of Molecular Oncology Foundation, Milan, Italy.

出版信息

PLoS One. 2013 Aug 5;8(8):e70233. doi: 10.1371/journal.pone.0070233. Print 2013.

Abstract

Reproducing the characteristics and the functional responses of the blood-brain barrier (BBB) in vitro represents an important task for the research community, and would be a critical biotechnological breakthrough. Pharmaceutical and biotechnology industries provide strong demand for inexpensive and easy-to-handle in vitro BBB models to screen novel drug candidates. Recently, it was shown that canonical Wnt signaling is responsible for the induction of the BBB properties in the neonatal brain microvasculature in vivo. In the present study, following on from earlier observations, we have developed a novel model of the BBB in vitro that may be suitable for large scale screening assays. This model is based on immortalized endothelial cell lines derived from murine and human brain, with no need for co-culture with astrocytes. To maintain the BBB endothelial cell properties, the cell lines are cultured in the presence of Wnt3a or drugs that stabilize β-catenin, or they are infected with a transcriptionally active form of β-catenin. Upon these treatments, the cell lines maintain expression of BBB-specific markers, which results in elevated transendothelial electrical resistance and reduced cell permeability. Importantly, these properties are retained for several passages in culture, and they can be reproduced and maintained in different laboratories over time. We conclude that the brain-derived endothelial cell lines that we have investigated gain their specialized characteristics upon activation of the canonical Wnt pathway. This model may be thus suitable to test the BBB permeability to chemicals or large molecular weight proteins, transmigration of inflammatory cells, treatments with cytokines, and genetic manipulation.

摘要

在体外重现血脑屏障(BBB)的特征和功能反应是研究界的一项重要任务,这将是生物技术的一个重大突破。制药和生物技术行业强烈需要廉价且易于处理的体外 BBB 模型来筛选新的候选药物。最近,研究表明,经典 Wnt 信号通路负责诱导体内新生大脑微血管 BBB 特性。在本研究中,基于早期的观察结果,我们开发了一种新的体外 BBB 模型,该模型可能适合大规模筛选测定。该模型基于源自鼠和人脑的永生化内皮细胞系,无需与星形胶质细胞共培养。为了保持 BBB 内皮细胞特性,在存在 Wnt3a 或稳定 β-连环蛋白的药物的情况下培养细胞系,或者用转录激活形式的 β-连环蛋白感染细胞系。经过这些处理,细胞系维持 BBB 特异性标志物的表达,导致跨内皮电阻增加和细胞通透性降低。重要的是,这些特性在培养物中保持几个传代,并且可以在不同的实验室中随着时间的推移再现和维持。我们得出结论,我们研究的源自大脑的内皮细胞系在经典 Wnt 通路被激活时获得其特化特征。因此,该模型可能适用于测试化学物质或大分子量蛋白质对 BBB 的通透性、炎症细胞的迁移、细胞因子处理和基因操作。

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