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微血管中培养扩增的间充质干细胞的命运:细胞动力学的体内观察

Fate of culture-expanded mesenchymal stem cells in the microvasculature: in vivo observations of cell kinetics.

作者信息

Toma Catalin, Wagner William R, Bowry Shivani, Schwartz Abigail, Villanueva Flordeliza

机构信息

Cardiovascular Institute, University of Pittsburgh School of Medicine, Pittsburgh, PA, USA.

出版信息

Circ Res. 2009 Feb 13;104(3):398-402. doi: 10.1161/CIRCRESAHA.108.187724. Epub 2008 Dec 18.

Abstract

Vascular delivery of mesenchymal stem cells (MSCs) following myocardial infarction is under clinical investigation. Little is known about the microvascular fate of MSCs. We used intravital microscopy of rat cremaster muscle microcirculation to track intraarterially delivered MSCs. Rat MSCs (average diameter, 23 microm) were bolused into the ipsilateral common iliac artery. Interrogation of an arteriole-venule pair revealed that 92+/-7% (n=6) of MSCs arrest and interrupt flow during first pass at the precapillary level, resulting in decreased flow in the feeding arteriole (velocity decreased from 6.3+/-1.0 to 4.6+/-1.3 mm/sec; P<0.001). MSC deformability evaluated using filtration through polycarbonate membranes revealed that the cortical tension of MSCs (0.49+/-0.07 dyne/cm, n=9) was not different from that of circulating mononuclear cells (0.50+/-0.05 dyne/cm, n=7). When intravital microscopy was performed 3 days following injection, the number of MSCs in the cremaster further decreased to 14% of the initial number, because of cell death in situ. In vivo labeling of the basement membrane revealed that at 1 day, the surviving cells were spread out on the luminal side of the microvessel, whereas at 3 days, they integrated in the microvascular wall. Despite their deformability, intraarterially delivered MSCs entrap at the precapillary level because of their large size, with a small proportion of surviving MSCs integrating in a perivascular niche.

摘要

心肌梗死后间充质干细胞(MSCs)的血管内递送正在进行临床研究。关于MSCs的微血管命运知之甚少。我们利用大鼠提睾肌微循环的活体显微镜来追踪经动脉递送的MSCs。将大鼠MSCs(平均直径23微米)注入同侧髂总动脉。对一对小动脉-小静脉进行观察发现,92±7%(n = 6)的MSCs在首次通过毛细血管前水平时滞留并阻断血流,导致供血小动脉血流减少(速度从6.3±1.0降至4.6±1.3毫米/秒;P<0.001)。通过聚碳酸酯膜过滤评估的MSCs可变形性显示,MSCs的皮质张力(0.49±0.07达因/厘米,n = 9)与循环单核细胞的皮质张力(0.50±0.05达因/厘米,n = 7)无差异。注射后3天进行活体显微镜观察时,提睾肌中的MSCs数量进一步减少至初始数量的14%,原因是细胞原位死亡。对基底膜进行体内标记显示,在第1天,存活细胞散布在微血管的管腔侧,而在第3天,它们整合到微血管壁中。尽管具有可变形性,但经动脉递送的MSCs因其体积较大而在毛细血管前水平滞留,只有一小部分存活的MSCs整合到血管周围微环境中。

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