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原始幼稚红细胞中的“成熟型”珠蛋白转换

"Maturational" globin switching in primary primitive erythroid cells.

作者信息

Kingsley Paul D, Malik Jeffrey, Emerson Rachel L, Bushnell Timothy P, McGrath Kathleen E, Bloedorn Laura A, Bulger Michael, Palis James

机构信息

Department of Pediatrics, University of Rochester Medical Center, Center for Pediatric Biomedical Research, Box 703, 601 Elmwood Ave, Rochester, NY 14642, USA.

出版信息

Blood. 2006 Feb 15;107(4):1665-72. doi: 10.1182/blood-2005-08-3097. Epub 2005 Nov 1.

DOI:10.1182/blood-2005-08-3097
PMID:16263786
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1895399/
Abstract

Mammals have 2 distinct erythroid lineages. The primitive erythroid lineage originates in the yolk sac and generates a cohort of large erythroblasts that terminally differentiate in the bloodstream. The definitive erythroid lineage generates smaller enucleated erythrocytes that become the predominant cell in fetal and postnatal circulation. These lineages also have distinct globin expression patterns. Our studies in primary murine primitive erythroid cells indicate that betaH1 is the predominant beta-globin transcript in the early yolk sac. Thus, unlike the human, murine beta-globin genes are not up-regulated in the order of their chromosomal arrangement. As primitive erythroblasts mature from proerythroblasts to reticulocytes, they undergo a betaH1- to epsilony-globin switch, up-regulate adult beta1- and beta2-globins, and down-regulate zeta-globin. These changes in transcript levels correlate with changes in RNA polymerase II density at their promoters and transcribed regions. Furthermore, the epsilony- and betaH1-globin genes in primitive erythroblasts reside within a single large hyperacetylated domain. These data suggest that this "maturational" betaH1- to epsilony-globin switch is dynamically regulated at the transcriptional level. Globin switching during ontogeny is due not only to the sequential appearance of primitive and definitive lineages but also to changes in globin expression as primitive erythroblasts mature in the bloodstream.

摘要

哺乳动物有两种不同的红系谱系。原始红系谱系起源于卵黄囊,产生一群大的成红细胞,这些细胞在血液中终末分化。定型红系谱系产生较小的无核红细胞,这些红细胞成为胎儿和出生后循环中的主要细胞。这些谱系也有不同的珠蛋白表达模式。我们对原代小鼠原始红系细胞的研究表明,βH1是早期卵黄囊中主要的β-珠蛋白转录本。因此,与人类不同,小鼠β-珠蛋白基因的上调顺序与其染色体排列顺序不一致。随着原始成红细胞从早幼红细胞成熟为网织红细胞,它们经历从βH1到εy-珠蛋白的转换,上调成人β1-和β2-珠蛋白,并下调ζ-珠蛋白。转录水平的这些变化与其启动子和转录区域的RNA聚合酶II密度的变化相关。此外,原始成红细胞中的εy-和βH1-珠蛋白基因位于单个大的高乙酰化结构域内。这些数据表明,这种从βH1到εy-珠蛋白的“成熟”转换在转录水平上受到动态调控。个体发育过程中的珠蛋白转换不仅是由于原始和定型谱系的顺序出现,还由于原始成红细胞在血液中成熟时珠蛋白表达的变化。

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本文引用的文献

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KLF2 is essential for primitive erythropoiesis and regulates the human and murine embryonic beta-like globin genes in vivo.KLF2对原始红细胞生成至关重要,并在体内调节人类和小鼠胚胎β样珠蛋白基因。
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