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首页> 外文期刊>Biochemistry and Cell Biology >In vivo DNA-protein interactions at hypersensitive site 3.5 of the human beta-globin locus control region.
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In vivo DNA-protein interactions at hypersensitive site 3.5 of the human beta-globin locus control region.

机译:人β-珠蛋白基因座控制区超敏位点3.5的体内DNA-蛋白质相互作用。

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摘要

Using ligation-mediated polymerase chain reaction and in vivo footprinting methods to study the status of DNA-protein interactions at hypersensitive site 3.5 (HS3.5) of the locus control region in K562 and HEL cells, we found that there was protein occupancy in vivo at HS3.5 in both cell lines and the status of DNA-protein interaction was different between K562 and HEL. These data provide direct evidence that specific nuclear factor-DNA complexes form in vivo at functionally important sequence motifs of the HS3.5 in erythroid cells. This indicates that HS3.5 may play an important role in the regulation of the beta-globin gene cluster. K562 is a human erythroleukemia cell line in which the embryonic epsilon-globin gene is predominantly expressed, while the HEL cell line expresses predominantly the fetal beta-globin genes. Thus, HS3.5 might also be involved in the regulation of developmental stage-specific expression of beta-globin genes. Our results are also consistent with the model that each hypersensitive site acts as a functional unit and HS3.5 may facilitate the formation of the HS3 functional unit.
机译:使用连接介导的聚合酶链反应和体内足迹方法研究K562和HEL细胞中基因座控制区超敏感位点3.5(HS3.5)的DNA-蛋白质相互作用的状态,我们发现体内存在蛋白质占用在两种细胞系中,HS3.5的表达都不同,并且K562和HEL之间的DNA-蛋白质相互作用状态不同。这些数据提供了直接的证据,表明特定的核因子-DNA复合物在体内在红系细胞中HS3.5的功能重要序列基序上形成。这表明HS3.5可能在调节β-珠蛋白基因簇中起重要作用。 K562是人红白血病细胞株,其中主要表达胚胎ε-珠蛋白基因,而HEL细胞株主要表达胎儿β-珠蛋白基因。因此,HS3.5也可能参与β-珠蛋白基因发育阶段特异性表达的调节。我们的结果也与每个超敏位点充当功能单元并且HS3.5可以促进HS3功能单元形成的模型相一致。

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