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Microvesicles Derived From Human Mesenchymal Stem Cells Restore Alveolar Fluid Clearance in Human Lungs Rejected for Transplantation

机译:源自人间充质干细胞的微泡可恢复被拒绝移植的人肺中的肺泡液间隙。

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摘要

The need to increase the donor pool for lung transplantation is a major public health issue. We previously found that administration of mesenchymal stem cells “rehabilitated” marginal donor lungs rejected for transplantation using ex vivo lung perfusion. However, the use of stem cells has some inherent limitation such as the potential for tumor formation. In the current study, we hypothesized that microvesicles, small anuclear membrane fragments constitutively released from mesenchymal stem cells, may be a good alternative to using stem cells. Using our well established ex vivo lung perfusion model, microvesicles derived from human mesenchymal stem cells increased alveolar fluid clearance (i.e. ability to absorb pulmonary edema fluid) in a dose-dependent manner, decreased lung weight gain following perfusion and ventilation, and improved airway and hemodynamic parameters compared to perfusion alone. Microvesicles derived from normal human lung fibroblasts as a control had no effect. Co-administration of microvesicles with anti-CD44 antibody attenuated these effects, suggesting a key role of the CD44 receptor in the internalization of the microvesicles into the injured host cell and its effect. In summary, microvesicles derived from human mesenchymal stem cells were as effective as the parent mesenchymal stem cells in rehabilitating marginal donor human lungs.
机译:需要增加用于肺移植的供体库是主要的公共卫生问题。我们以前发现间充质干细胞的施用“恢复了”边缘供体肺,但拒绝使用离体肺灌注进行移植。但是,干细胞的使用有一些固有的局限性,例如潜在的肿瘤形成。在当前的研究中,我们假设微细胞,即从间充质干细胞组成性释放的小的环形核膜碎片,可能是使用干细胞的一种很好的选择。使用我们完善的离体肺灌注模型,源自人间充质干细胞的微泡以剂量依赖性方式增加了肺泡液清除率(即吸收肺水肿液的能力),减少了灌注和通气后肺增重,并改善了气道和血液动力学参数相比,单独灌注。以正常人肺成纤维细胞为对照的微泡没有作用。微囊泡与抗CD44抗体的共同给药减弱了这些作用,表明CD44受体在微囊泡内化到受损宿主细胞中及其作用中起关键作用。总之,在修复边缘供体人肺中,源自人间充质干细胞的微泡与亲代间充质干细胞一样有效。

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