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对红系细胞与其他细胞的细胞杂交体中与珠蛋白基因和非珠蛋白基因表达相关的染色质变化的分析。

Analysis of chromatin changes associated with the expression of globin and non-globin genes in cell hybrids between erythroid and other cells.

作者信息

Affara N, Fleming J, Goldfarb P S, Black E, Thiele B, Harrison P R

出版信息

Nucleic Acids Res. 1985 Aug 12;13(15):5629-44. doi: 10.1093/nar/13.15.5629.

Abstract

Red blood cell differentiation involves the coordinate expression of a set of polypeptides some of which are erythroid-specific (the abundant globins as well as minor species such as glycophorin, carbonic anhydrase I and the RBC lipoxygenase) whereas others are found also in a subset of other cells, e.g. beta spectrin and a 19 kd polypeptide (ep 19) found in adult liver and kidney as well as erythroid cells. To investigate the genetic mechanisms involved in the regulation of these classes of genes, the expression of lipoxygenase, ep 19 and beta globin mRNAs was investigated in cell hybrids between mouse erythroid (Friend) cells and mouse T-lymphoma or neuroblastoma cells. All three mRNAs are expressed or repressed together in cell hybrids between the Friend cell and lymphoma or neuroblastoma cells respectively. Moreover, studies of the chromatin structure surrounding the genes reveal that erythroid cell-specific DNaseI hypersensitive sites within the ep 19 and beta major globin genes are lost in the Friend cell X neuroblastoma hybrids whereas they are retained in the Friend cell X lymphoma cell hybrids. This implies that the trans-acting mechanism responsible for regulating the RBC phenotype in these cell hybrids acts at the level of the early chromatin changes thought to reflect a pre-activation stage in gene expression.

摘要

红细胞分化涉及一组多肽的协同表达,其中一些是红细胞特异性的(丰富的珠蛋白以及诸如血型糖蛋白、碳酸酐酶I和红细胞脂氧合酶等次要成分),而其他一些在其他细胞的亚群中也有发现,例如在成体肝脏、肾脏以及红细胞中都存在的β-血影蛋白和一种19kd多肽(ep19)。为了研究参与这些基因类别调控的遗传机制,我们在小鼠红细胞(Friend)细胞与小鼠T淋巴瘤或神经母细胞瘤细胞之间的细胞杂种中,研究了脂氧合酶、ep19和β-珠蛋白mRNA的表达。在Friend细胞与淋巴瘤或神经母细胞瘤细胞之间的细胞杂种中,这三种mRNA分别共同表达或受到抑制。此外,对这些基因周围染色质结构的研究表明,ep19和β-主要珠蛋白基因内的红细胞特异性DNaseI超敏位点在Friend细胞X神经母细胞瘤杂种中消失,而在Friend细胞X淋巴瘤细胞杂种中则保留。这意味着在这些细胞杂种中负责调节红细胞表型的反式作用机制在早期染色质变化水平起作用,这种变化被认为反映了基因表达的预激活阶段。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6311/321894/44a41008f590/nar00309-0226-a.jpg

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