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Red Cells: Globin switches in yolk sac–like primitive and fetal-like definitive red blood cells produced from human embryonic stem cells

机译:红细胞:球蛋白转换成人类胚胎干细胞产生的卵黄囊样原始和胎儿样确定性红细胞

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摘要

We have previously shown that coculture of human embryonic stem cells (hESCs) for 14 days with immortalized fetal hepatocytes yields CD34+ cells that can be expanded in serum-free liquid culture into large numbers of megaloblastic nucleated erythroblasts resembling yolk sac–derived cells. We show here that these primitive erythroblasts undergo a switch in hemoglobin (Hb) composition during late terminal erythroid maturation with the basophilic erythroblasts expressing predominantly Hb Gower I (ζ2ϵ2) and the orthochromatic erythroblasts hemoglobin Gower II (α2ϵ2). This suggests that the switch from Hb Gower I to Hb Gower II, the first hemoglobin switch in humans is a maturation switch not a lineage switch. We also show that extending the coculture of the hESCs with immortalized fetal hepatocytes to 35 days yields CD34+ cells that differentiate into more developmentally mature, fetal liver–like erythroblasts, that are smaller, express mostly fetal hemoglobin, and can enucleate. We conclude that hESC-derived erythropoiesis closely mimics early human development because the first 2 human hemoglobin switches are recapitulated, and because yolk sac–like and fetal liver–like cells are sequentially produced. Development of a method that yields erythroid cells with an adult phenotype remains necessary, because the most mature cells that can be produced with current systems express less than 2% adult β-globin mRNA.
机译:先前我们已经证明,人类胚胎干细胞(hESCs)与永生化的胎儿肝细胞共培养14天会产生CD34 + 细胞,这些细胞可以在无血清的液体培养物中扩增成大量类似于巨核成核的成核细胞卵黄囊来源的细胞。我们在这里显示,这些原始的成红细胞在晚期末期红细胞成熟过程中经历血红蛋白(Hb)组成的转换,嗜碱性成红细胞主要表达Hb Gower I(ζ2ϵ2)和正色成红细胞红细胞血红蛋白Gower II(α2ϵ2)。这表明,人类中第一个血红蛋白开关从Hb Gower I切换到Hb Gower II,是成熟开关,而不是血统开关。我们还表明,将hESCs与永生化的胎儿肝细胞的共培养延长至35天会产生CD34 + 细胞,这些细胞分化为发育更成熟的胎儿肝脏样成血红细胞,较小,主要表达胎儿血红蛋白,并且可以使人迷惑。我们得出的结论是,hESC衍生的促红细胞生成与人类早期发育密切相似,因为前两个人类血红蛋白开关被概括,并且依次产生卵黄囊样和胎儿肝样细胞。产生具有成年表型的类红细胞的方法的开发仍然是必要的,因为可以用当前系统产生的最成熟的细胞表达少于2%的成年β-珠蛋白mRNA。

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