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单细胞高通量分析细胞与血管壁的对接。

Single-cell, high-throughput analysis of cell docking to vessel wall.

机构信息

NeuroRepair Department, Mossakowski Medical Research Centre, Polish Academy of Sciences, Warsaw, Poland.

Laboratory of Advanced Microscopy Techniques, Mossakowski Medical Research Centre, Polish Academy of Sciences, Warsaw, Poland.

出版信息

J Cereb Blood Flow Metab. 2019 Nov;39(11):2308-2320. doi: 10.1177/0271678X18805238. Epub 2018 Oct 26.

Abstract

Therapeutic potential of mesenchymal stem cells (MSCs) has been reported consistently in animal models of stroke, with mechanism mainly through immunomodulation and paracrine activity. Intravenous injection has been a prevailing route for MSCs administration, but cell quantities needed when scaling-up from mouse to human are extremely high putting into question feasibility of that approach. Intra-arterial delivery directly routes the cells to the brain thus lowering the required dose. Cell engineering may additionally improve cell homing, further potentiating the value of intra-arterial route. Therefore, our goal was to create microfluidic platform for screening and fast selection of molecules that enhance the docking of stem cells to vessel wall. We hypothesized that our software will be capable of detecting distinct docking properties of naïve and ITGA4-engineered MSCs. Indeed, the cell flow tracker analysis revealed positive effect of cell engineering on docking frequency of MSCs (42% vs. 9%, engineered vs. control cells,  < 0.001). These observations were then confirmed in an animal model of focal brain injury where cell engineering resulted in improved homing to the brain. To conclude, we developed a platform to study the docking of cells to the vessel wall which is highly relevant for intraarterial cell targeting or studies on neuroinflammation.

摘要

间充质干细胞 (MSCs) 的治疗潜力在中风动物模型中得到了一致的报道,其机制主要通过免疫调节和旁分泌活性。静脉注射一直是 MSC 给药的主要途径,但从小鼠到人类的放大规模所需的细胞数量极高,这使得该方法的可行性受到质疑。动脉内给药可直接将细胞输送到大脑,从而降低所需剂量。细胞工程还可以增加细胞归巢,进一步增强动脉内途径的价值。因此,我们的目标是创建一个微流控平台,用于筛选和快速选择可增强干细胞与血管壁结合的分子。我们假设我们的软件将能够检测到原始和 ITGA4 工程 MSC 的不同结合特性。事实上,细胞流动追踪分析显示细胞工程对 MSC 结合频率有积极影响(42%对 9%,工程细胞对对照细胞,<0.001)。这些观察结果随后在局灶性脑损伤的动物模型中得到了证实,细胞工程导致细胞向大脑的归巢得到改善。总之,我们开发了一个研究细胞与血管壁结合的平台,这对于动脉内细胞靶向或神经炎症研究非常重要。

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