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一种常见的双能祖细胞在胚胎干细胞衍生的原始造血过程中产生红细胞和巨核细胞谱系。

A common bipotent progenitor generates the erythroid and megakaryocyte lineages in embryonic stem cell-derived primitive hematopoiesis.

作者信息

Klimchenko Olena, Mori Marcella, Distefano Antonio, Langlois Thierry, Larbret Frédéric, Lecluse Yann, Feraud Olivier, Vainchenker William, Norol Françoise, Debili Najet

机构信息

Inserm U790, Institut Gustave Roussy, Villejuif, France.

出版信息

Blood. 2009 Aug 20;114(8):1506-17. doi: 10.1182/blood-2008-09-178863. Epub 2009 May 28.

Abstract

The megakaryocytic (MK) and erythroid lineages are tightly associated during differentiation and are generated from a bipotent megakaryocyte-erythroid progenitor (MEP). In the mouse, a primitive MEP has been demonstrated in the yolk sac. In human, it is not known whether the primitive MK and erythroid lineages are generated from a common progenitor or independently. Using hematopoietic differentiation of human embryonic stem cells on the OP9 cell line, we identified a primitive MEP in a subset of cells coexpressing glycophorin A (GPA) and CD41 from day 9 to day 12 of coculturing. This MEP differentiates into primitive erythroid (GPA(+)CD41(-)) and MK (GPA(-)CD41(+)) lineages. In contrast to erythropoietin (EPO)-dependent definitive hematopoiesis, KIT was not detected during erythroid differentiation. A molecular signature for the commitment and differentiation toward both the erythroid and MK lineages was detected by assessing expression of transcription factors, thrombopoietin receptor (MPL) and erythropoietin receptor (EPOR). We showed an inverse correlation between FLI1 and both KLF1 and EPOR during primitive erythroid and MK differentiation, similar to definitive hematopoiesis. This novel MEP differentiation system may allow an in-depth exploration of the molecular bases of erythroid and MK commitment and differentiation.

摘要

巨核细胞(MK)和红系谱系在分化过程中紧密相关,并且由双能巨核细胞-红系祖细胞(MEP)产生。在小鼠中,已在卵黄囊中证实存在原始MEP。在人类中,尚不清楚原始MK和红系谱系是由共同祖细胞产生还是独立产生。利用人胚胎干细胞在OP9细胞系上的造血分化,我们在共培养第9天至第12天共表达血型糖蛋白A(GPA)和CD41的细胞亚群中鉴定出一种原始MEP。这种MEP分化为原始红系(GPA(+)CD41(-))和MK(GPA(-)CD41(+))谱系。与依赖促红细胞生成素(EPO)的确定性造血不同,在红系分化过程中未检测到KIT。通过评估转录因子、血小板生成素受体(MPL)和促红细胞生成素受体(EPOR)的表达,检测到了向红系和MK谱系定向分化的分子特征。我们发现在原始红系和MK分化过程中,FLI1与KLF1和EPOR均呈负相关,这与确定性造血相似。这种新型的MEP分化系统可能有助于深入探索红系和MK定向分化及分化的分子基础。

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