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自体肺源性间充质干细胞移植治疗实验性肺气肿。

Autologous lung-derived mesenchymal stem cell transplantation in experimental emphysema.

机构信息

Division of Pulmonary & Critical Care Medicine, Brigham and Women's Hospital, Boston, MA, USA.

出版信息

Cell Transplant. 2012;21(1):175-89. doi: 10.3727/096368910X550233. Epub 2011 Feb 3.

Abstract

Autologous lung-derived mesenchymal stem cells (LMSCs) were transplanted endoscopically into sheep with experimental emphysema to assess their capacity to regenerate functional tissue. LMSC lines were derived from transbronchial biopsies, cloned at passage 2, expanded in culture, and labeled. A delivery scaffold containing 1% fibrinogen, 20 μg/ml of fibronectin, and 20 μg/ml of poly-L-lysine was used to promote cell attachment and spreading. Treatment animals received scaffold containing 5-10 × 10(6) cells/site; control animals received scaffold alone. Phenotypic markers, differentiation capacity, extracellular matrix protein expression, and paracrine function of LMSCs were characterized in vitro. Responses to LMSC transplantation in vivo were assessed in terms of clinical toxicity, lung physiology, change in tissue mass (measured by CT scanning) and perfusion (measured by scintigraphy scanning), and tissue histology. At 4-week follow-up, transplants were well tolerated and associated with increased tissue mass and lung perfusion compared to control treatment. Histology confirmed cell retention, increased cellularity, and increased extracellular matrix content following LMSC treatment. Labeled cells were distributed in the alveolar septum and peribronchiolar interstitium. Some label was also present within phagocytes, indicating that a fraction of autologous LMSCs do not survive transplantation. These results suggest that endobronchial delivery of autologous LMSCs has potential therapeutic utility for regenerating functional lung in emphysema.

摘要

自体肺源性间充质干细胞(LMSCs)经支气管镜移植到实验性肺气肿羊体内,以评估其再生功能性组织的能力。LMSC 系源自经支气管活检,在传代 2 时克隆,在培养中扩增并标记。含有 1%纤维蛋白原、20μg/ml 纤连蛋白和 20μg/ml 聚-L-赖氨酸的递送支架用于促进细胞附着和扩展。治疗动物接受含有 5-10×10^6 个细胞/部位的支架;对照动物仅接受支架。体外研究了 LMSC 的表型标记、分化能力、细胞外基质蛋白表达和旁分泌功能。根据临床毒性、肺生理学、组织质量(通过 CT 扫描测量)和灌注(通过闪烁扫描测量)以及组织病理学变化,评估了 LMSC 移植在体内的反应。在 4 周随访时,与对照治疗相比,移植后耐受性良好,与组织质量和肺灌注增加相关。组织学证实了细胞保留、细胞增多和细胞外基质含量增加,这与 LMSC 治疗有关。标记细胞分布在肺泡隔和小支气管周围间质中。一些标记也存在于吞噬细胞中,表明部分自体 LMSC 不能在移植后存活。这些结果表明,支气管内递送电刺激自体 LMSC 具有再生肺气肿中功能性肺的潜在治疗效用。

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