3D brain angiogenesis model to reconstitute functional human blood–brain barrier in vitro

血脑屏障 血管生成 流出 中枢神经系统 新生血管 生物 体外 细胞生物学 周细胞 运输机 内皮 神经科学 内皮干细胞 癌症研究 生物化学 内分泌学 基因
作者
Somin Lee,Minhwan Chung,Byungjun Lee,Noo Li Jeon
出处
期刊:Biotechnology and Bioengineering [Wiley]
卷期号:117 (3): 748-762 被引量:109
标识
DOI:10.1002/bit.27224
摘要

Abstract The human central nervous system (CNS) vasculature expresses a distinctive barrier phenotype, the blood–brain barrier (BBB). As the BBB contributes to low efficiency in CNS pharmacotherapy by restricting drug transport, the development of an in vitro human BBB model has been in demand. Here, we present a microfluidic model of CNS angiogenesis having three‐dimensional (3D) lumenized vasculature in concert with perivascular cells. We confirmed the necessity of the angiogenic tri‐culture system (brain endothelium in direct interaction with pericytes and astrocytes) to attain essential phenotypes of BBB vasculature, such as minimized vessel diameter and maximized junction expression. In addition, lower vascular permeability is achieved in the tri‐culture condition compared to the monoculture condition. Notably, we focussed on reconstituting the functional efflux transporter system, including p‐glycoprotein (p‐gp), which is highly responsible for restrictive drug transport. By conducting the calcein‐AM efflux assay on our 3D perfusable vasculature after treatment of efflux transporter inhibitors, we confirmed the higher efflux property and prominent effect of inhibitors in the tri‐culture model. Taken together, we designed a 3D human BBB model with functional barrier properties based on a developmentally inspired CNS angiogenesis protocol. We expect the model to contribute to a deeper understanding of pathological CNS angiogenesis and the development of effective CNS medications.
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