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用于药物转运筛选试验的具有开放毛细血管结构的三维血脑屏障网络的构建。

Development of a three-dimensional blood-brain barrier network with opening capillary structures for drug transport screening assays.

作者信息

Piantino Marie, Kang Dong-Hee, Furihata Tomomi, Nakatani Noriyuki, Kitamura Kimiko, Shigemoto-Mogami Yukari, Sato Kaoru, Matsusaki Michiya

机构信息

Department of Applied Chemistry, Graduate School of Engineering, Osaka University, Suita, Osaka, Japan.

School of Pharmacy, Tokyo University of Pharmacy and Life Sciences, Hachioji, Tokyo, Japan.

出版信息

Mater Today Bio. 2022 Jun 15;15:100324. doi: 10.1016/j.mtbio.2022.100324. eCollection 2022 Jun.

Abstract

The blood-brain barrier (BBB), a selective barrier regulating the active and passive transport of solutes in the extracellular fluid of the central nervous system, prevents the delivery of therapeutics for brain disorders. The BBB is composed of brain microvascular endothelial cells (BMEC), pericytes and astrocytes. Current BBB models cannot reproduce the human structural complexity of the brain microvasculature, and thus their functions are not enough for drug assessments. In this study, we developed a 3D self-assembled microvascular network formed by BMEC covered by pericytes and astrocyte end feet. It exhibited perfusable microvasculature due to the presence of capillary opening ends on the bottom of the hydrogel. It also demonstrated size-selective permeation of different molecular weights of fluorescent-labeled dextran, as similarly reported for rodent brain, suggesting the same permeability with actual brain. The activity of -glycoprotein efflux pump was confirmed using the substrate Rhodamine 123. Finally, the functionality of the receptor-mediated transcytosis, one of the main routes for drug delivery of large molecules into the brain, could be validated using transferrin receptor (TfR) with confocal imaging, competition assays and permeability assays. Efficient permeability coefficient (P) value of transportable anti-TfR antibody (MEM-189) was seven-fold higher than those of isotype antibody (IgG1) and low transportable anti-TfR antibody (13E4), suggesting a higher TfR transport function than previous reports. The BBB model with capillary openings could thus be a valuable tool for the screening of therapeutics that can be transported across the BBB, including those using TfR-mediated transport.

摘要

血脑屏障(BBB)是一种选择性屏障,可调节中枢神经系统细胞外液中溶质的主动和被动转运,它阻碍了治疗脑部疾病药物的递送。血脑屏障由脑微血管内皮细胞(BMEC)、周细胞和星形胶质细胞组成。目前的血脑屏障模型无法重现人类脑微血管的结构复杂性,因此其功能不足以用于药物评估。在本研究中,我们构建了一种由周细胞和星形胶质细胞终足覆盖的BMEC形成的三维自组装微血管网络。由于水凝胶底部存在毛细血管开口端,该网络呈现出可灌注的微血管系统。它还表现出对不同分子量荧光标记葡聚糖的大小选择性渗透,这与啮齿动物脑的情况类似,表明其与实际脑具有相同的通透性。使用底物罗丹明123证实了P-糖蛋白外排泵的活性。最后,利用转铁蛋白受体(TfR)通过共聚焦成像、竞争试验和通透性试验,可以验证受体介导的转胞吞作用(将大分子药物递送至脑内的主要途径之一)的功能。可转运抗TfR抗体(MEM-189)的有效渗透系数(P)值比同型抗体(IgG1)和低转运抗TfR抗体(13E4)高7倍,表明其TfR转运功能比先前报道的更高。因此,具有毛细血管开口的血脑屏障模型可能是筛选能够穿过血脑屏障的治疗药物(包括那些利用TfR介导转运的药物)的有价值工具。

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