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The gene for erythropoietin receptor is expressed in multipotential hematopoietic and embryonal stem cells: evidence for differentiation stage-specific regulation.

机译:促红细胞生成素受体的基因在多能造血干细胞和胚胎干细胞中表达:分化阶段特异性调控的证据。

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摘要

The principal regulator of erythropoiesis is the glycoprotein erythropoietin, which interacts with a specific cell surface receptor (EpoR). A study aimed at analyzing EpoR gene regulation has shown that both pluripotent embryonal stem cells and early multipotent hematopoietic cells express EpoR transcripts. Commitment to nonerythroid lineages (e.g., macrophage or lymphocytic) results in the shutdown of EpoR gene expression, whereas commitment to the erythroid lineage is concurrent with or followed by dramatic increases in EpoR transcription. To determine whether gene activity could be correlated with chromatin alterations, DNase-hypersensitive sites (HSS) were mapped. Two major HSS located in the promoter region and within the first intron of the EpoR gene are present in all embryonal stem and hematopoietic cells tested, the intensities of which correlate well with EpoR expression levels. In addition, a third major HSS also located within the first intron of the EpoR gene is uniquely present in erythroid cells that express high levels of EpoR. Transfection assays show that sequences surrounding this major HSS impart erythroid cell-specific enhancer activity to a heterologous promoter and that this activity is at least in part mediated by GATA-1. These data, together with concordant expression levels of GATA-1 and EpoR in both early multipotent hematopoietic and committed erythroid cells, support a regulatory role of the erythroid cell-specific transcription factor GATA-1 in EpoR transcription in these cells. However, the lack of significant levels of GATA-1 expression in embryonal stem cells implies an alternative regulatory mechanism of EpoR transcription in cells not committed to the hematopoietic lineage.
机译:促红细胞生成素的主要调节剂是糖蛋白促红细胞生成素,它与特定的细胞表面受体(EpoR)相互作用。一项旨在分析EpoR基因调控的研究表明,多能胚胎干细胞和早期多能造血细胞均表达EpoR转录本。致力于非红系谱系(例如巨噬细胞或淋巴细胞)导致EpoR基因表达的关闭,而对红系谱系的承诺与EpoR转录同时发生或随之而来。为了确定基因活性是否可能与染色质改变相关,对DNase超敏位点(HSS)进行了定位。位于EpoR基因启动子区域和第一内含子的两个主要HSS存在于所有测试的胚胎干细胞和造血细胞中,其强度与EpoR表达水平密切相关。另外,也位于EpoR基因的第一内含子内的第三主要HSS独特地存在于表达高水平EpoR的红系细胞中。转染分析表明,围绕这一主要HSS的序列将异源启动子赋予类红细胞特异性增强子活性,并且该活性至少部分由GATA-1介导。这些数据,以及早期多能造血和定型红系细胞中GATA-1和EpoR的一致表达水平,支持了类红细胞特异性转录因子GATA-1在这些细胞中EpoR转录中的调节作用。但是,胚胎干细胞中GATA-1表达水平的缺乏暗示着EpoR转录在非造血细胞系中的另一种调控机制。

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