静脉注射人骨髓间充质干细胞可改善小鼠心肌梗死,因为肺中栓塞的细胞被激活后会分泌抗炎蛋白TSG-6。
Intravenous hMSCs improve myocardial infarction in mice because cells embolized in lung are activated to secrete the anti-inflammatory protein TSG-6.
作者信息
Lee Ryang Hwa, Pulin Andrey A, Seo Min Jeong, Kota Daniel J, Ylostalo Joni, Larson Benjamin L, Semprun-Prieto Laura, Delafontaine Patrice, Prockop Darwin J
机构信息
Center for Gene Therapy, Tulane University Health Sciences Center, New Orleans, LA 70112, USA.
出版信息
Cell Stem Cell. 2009 Jul 2;5(1):54-63. doi: 10.1016/j.stem.2009.05.003.
Abstract
Quantitative assays for human DNA and mRNA were used to examine the paradox that intravenously (i.v.) infused human multipotent stromal cells (hMSCs) can enhance tissue repair without significant engraftment. After 2 x 10(6) hMSCs were i.v. infused into mice, most of the cells were trapped as emboli in lung. The cells in lung disappeared with a half-life of about 24 hr, but <1000 cells appeared in six other tissues. The hMSCs in lung upregulated expression of multiple genes, with a large increase in the anti-inflammatory protein TSG-6. After myocardial infarction, i.v. hMSCs, but not hMSCs transduced with TSG-6 siRNA, decreased inflammatory responses, reduced infarct size, and improved cardiac function. I.v. administration of recombinant TSG-6 also reduced inflammatory responses and reduced infarct size. The results suggest that improvements in animal models and patients after i.v. infusions of MSCs are at least in part explained by activation of MSCs to secrete TSG-6.
摘要
采用人DNA和mRNA定量分析方法,研究静脉注射人多能基质细胞(hMSCs)可在无显著植入的情况下促进组织修复这一矛盾现象。将2×10⁶个hMSCs静脉注射到小鼠体内后,大部分细胞作为栓子滞留在肺部。肺部的细胞以约24小时的半衰期消失,但在其他六个组织中出现的细胞少于1000个。肺部的hMSCs上调了多个基因的表达,抗炎蛋白TSG-6大幅增加。心肌梗死后,静脉注射hMSCs(而非用TSG-6 siRNA转导的hMSCs)可减轻炎症反应、缩小梗死面积并改善心脏功能。静脉注射重组TSG-6也可减轻炎症反应并缩小梗死面积。结果表明,静脉输注MSCs后动物模型和患者状况的改善至少部分是由MSCs激活分泌TSG-6所致。
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