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Peg3/PW1 是血管相关内皮祖细胞亚群的标志物。

Peg3/PW1 Is a Marker of a Subset of Vessel Associated Endothelial Progenitors.

机构信息

FIRC Institute of Molecular Oncology (IFOM) Fondazione, Milan, Italy.

Stem Cells and Regenerative Medicine, Institute of Cardiometabolism and Nutrition (ICAN) UMRS 1166 Université de Pierre et Marie Curie-Sorbonne Universités and INSERM, Paris, France.

出版信息

Stem Cells. 2017 May;35(5):1328-1340. doi: 10.1002/stem.2566. Epub 2017 Feb 5.

DOI:10.1002/stem.2566
PMID:28090691
Abstract

Vascular associated endothelial cell (ECs) progenitors are still poorly studied and their role in the newly forming vasculature at embryonic or postnatal stage remains elusive. In the present work, we first defined a set of genes highly expressed during embryo development and strongly downregulated in the adult mouse. In this group, we then concentrated on the progenitor cell marker Peg3/PW1. By in vivo staining of the vasculature we found that only a subset of cells coexpressed endothelial markers and PW1. These cells were quite abundant in the embryo vasculature but declined in number at postnatal and adult stages. Using a reporter mouse for PW1 expression, we have been able to isolate PW1-positive (PW1posECs) and negative endothelial cells (PW1negECs). PW1-positive cells were highly proliferative in comparison to PW1negECs and were able to form colonies when seeded at clonal dilution. Furthermore, by RNAseq analysis, PW1posECs expressed endothelial cell markers together with mesenchymal and stem cell markers. When challenged by endothelial growth factors in vitro, PW1posECs were able to proliferate more than PW1negECs and to efficiently form new vessels in vivo. Taken together these data identify a subset of vessel associated endothelial cells with characteristics of progenitor cells. Considering their high proliferative potential these cells may be of particular importance to design therapies to improve the perfusion of ischemic tissues or to promote vascular repair. Stem Cells 2017;35:1328-1340.

摘要

血管相关的内皮细胞(ECs)祖细胞的研究还很不充分,其在胚胎或出生后阶段新形成的血管中的作用仍然难以捉摸。在本工作中,我们首先定义了一组在胚胎发育过程中高度表达且在成年小鼠中强烈下调的基因。在这一组中,我们集中研究了祖细胞标志物 Peg3/PW1。通过对血管的体内染色,我们发现只有一部分细胞共表达内皮标记物和 PW1。这些细胞在胚胎血管中非常丰富,但在出生后和成年阶段数量减少。使用用于 PW1 表达的报告基因小鼠,我们能够分离出 PW1 阳性(PW1posECs)和阴性内皮细胞(PW1negECs)。与 PW1negECs 相比,PW1 阳性细胞具有更高的增殖能力,并且当以克隆稀释播种时能够形成集落。此外,通过 RNAseq 分析,PW1posECs 表达内皮细胞标记物以及间质和干细胞标记物。当在体外受到内皮生长因子的挑战时,PW1posECs 比 PW1negECs 更能增殖,并能有效地在体内形成新的血管。这些数据共同表明,血管相关的内皮细胞具有祖细胞的特征。考虑到它们的高增殖潜力,这些细胞可能对设计治疗缺血组织灌注或促进血管修复的治疗方法具有特别重要的意义。干细胞 2017;35:1328-1340。

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