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Hypoxia-enhanced Blood-Brain Barrier Chip recapitulates human barrier function and shuttling of drugs and antibodies

机译:缺氧增强的血脑屏障芯片重现了人类的屏障功能以及药物和抗体的穿梭

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摘要

The high selectivity of the human blood-brain barrier (BBB) restricts delivery of many pharmaceuticals and therapeutic antibodies to the central nervous system. Here, we describe an in vitro microfluidic organ-on-a-chip BBB model lined by induced pluripotent stem cell-derived human brain microvascular endothelium interfaced with primary human brain astrocytes and pericytes that recapitulates the high level of barrier function of the in vivo human BBB for at least one week in culture. The endothelium expresses high levels of tight junction proteins and functional efflux pumps, and it displays selective transcytosis of peptides and antibodies previously observed in vivo. Increased barrier functionality was accomplished using a developmentally-inspired induction protocol that includes a period of differentiation under hypoxic conditions. This enhanced BBB Chip may therefore represent a new in vitro tool for development and validation of delivery systems that transport drugs and therapeutic antibodies across the human BBB.
机译:人血脑屏障(BBB)的高选择性限制了许多药物和治疗性抗体向中枢神经系统的输送。在这里,我们描述了体外微流控芯片上BBB模型,该模型由诱导性多能干细胞衍生的人脑微血管内皮细胞与原代人脑星形胶质细胞和周细胞交界,概括了体内人的高水平屏障功能BBB培养至少一周。内皮表达高水平的紧密连接蛋白和功能性外排泵,并且它表现出先前在体内观察到的肽和抗体的选择性转胞吞作用。使用受发展启发的诱导方案(包括在低氧条件下的分化期)可以完成增加的屏障功能。因此,这种增强的BBB芯片可能代表了一种新的体外工具,用于开发和验证跨人类BBB转运药物和治疗性抗体的输送系统。

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