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在缺氧条件下培养的孕晚期羊水干细胞的内皮特性

Endothelial properties of third-trimester amniotic fluid stem cells cultured in hypoxia.

作者信息

Schiavo Andrea Alex, Franzin Chiara, Albiero Mattia, Piccoli Martina, Spiro Giovanna, Bertin Enrica, Urbani Luca, Visentin Silvia, Cosmi Erich, Fadini Gian Paolo, De Coppi Paolo, Pozzobon Michela

机构信息

Stem Cells and Regenerative Medicine Laboratory, Foundation Institute of Pediatric Research Città della Speranza, Corso Stati Uniti 4, 35127, Padova, Italy.

Department of Woman and Children Health, University of Padova, via Giustinani 2, 35100, Padova, Italy.

出版信息

Stem Cell Res Ther. 2015 Oct 31;6:209. doi: 10.1186/s13287-015-0204-0.

Abstract

INTRODUCTION

Endothelial dysfunction is found in different pathologies such as diabetes and renal and heart diseases, representing one of the major health problems. The reduced vasodilation of impaired endothelium starts a prothrombotic state associated with irregular blood flow. We aimed to explore the potential of amniotic fluid stem (AFS) cells as a source for regenerative medicine in this field; for the first time, we focused on third-trimester amniotic fluid AFS cells and compared them with the already-described AFS cells from the second trimester.

METHODS

Cells from the two trimesters were cultured, selected and expanded in normoxia (20 % oxygen) and hypoxia (5 % oxygen). Cells were analysed to compare markers, proliferation rate and differentiation abilities. Endothelial potential was assessed not only in vitro-Matrigel tube formation assay, acetylated human low-density lipoprotein (AcLDL) uptake-but also in vivo (Matrigel plug with cell injection and two animal models). Specifically, for the latter, we used established protocols to assess the involvement of AFS cells in two different mouse models of endothelial dysfunction: (1) a chronic ischemia model with local injection of cells and (2) an electric carotid damage where cells were systemically injected.

RESULTS

We isolated and expanded AFS cells from third-trimester amniotic fluid samples by using CD117 as a selection marker. Hypoxia enhanced the proliferation rate, the surface protein pattern was conserved between the trimesters and comparable differentiation was achieved after culture in both normoxia and hypoxia. Notably, the expression of early endothelial transcription factors and AngiomiRs was detected before and after induction. When in vivo, AFS cells from both trimesters expanded in hypoxia were able to rescue the surface blood flow when locally injected in mice after chronic ischemia damage, and importantly AFS cells at term of gestation possessed enhanced ability to fix carotid artery electric damage compared with AFS cells from the second trimester.

CONCLUSIONS

To the best of our knowledge, this is the first research work that fully characterizes AFS cells from the third trimester for regenerative medicine purposes. The results highlight how AFS cells, in particular at term of gestation and cultured in hypoxia, can be considered a promising source of stem cells possessing significant endothelial regenerative potential.

摘要

引言

内皮功能障碍存在于多种病理状况中,如糖尿病、肾脏疾病和心脏疾病,是主要的健康问题之一。受损内皮的血管舒张功能降低会引发与血流不规则相关的促血栓形成状态。我们旨在探索羊水干细胞(AFS细胞)作为该领域再生医学细胞来源的潜力;我们首次聚焦于孕晚期羊水AFS细胞,并将其与已描述的孕中期AFS细胞进行比较。

方法

将两个孕期的细胞在常氧(20%氧气)和低氧(5%氧气)条件下进行培养、筛选和扩增。对细胞进行分析以比较标志物、增殖率和分化能力。不仅通过体外基质胶管形成试验、乙酰化人低密度脂蛋白(AcLDL)摄取来评估内皮潜能,还通过体内试验(细胞注射的基质胶塞和两种动物模型)进行评估。具体而言,对于后者,我们采用既定方案评估AFS细胞在两种不同的内皮功能障碍小鼠模型中的作用:(1)局部注射细胞的慢性缺血模型;(2)全身注射细胞的颈动脉电损伤模型。

结果

我们使用CD117作为筛选标志物,从孕晚期羊水样本中分离并扩增出AFS细胞。低氧增强了增殖率,两个孕期的细胞表面蛋白模式保持一致,在常氧和低氧培养后均实现了类似的分化。值得注意的是,在诱导前后均检测到早期内皮转录因子和血管生成微RNA的表达。在体内,两个孕期在低氧条件下扩增的AFS细胞在慢性缺血损伤后局部注射到小鼠体内时能够挽救表面血流,重要的是,与孕中期的AFS细胞相比,足月妊娠的AFS细胞修复颈动脉电损伤的能力更强。

结论

据我们所知,这是第一项为再生医学目的全面表征孕晚期AFS细胞的研究工作。结果突出表明,AFS细胞,特别是足月妊娠且在低氧条件下培养的AFS细胞,可被视为具有显著内皮再生潜力的有前景的干细胞来源。

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