首页> 外文OA文献 >Differential expression of lacZ in the liver and kidney of transgenic mice carrying chimeric lacZ-erythropoietin gene constructs with or without its 1.2 kb 3'-flanking sequence.
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Differential expression of lacZ in the liver and kidney of transgenic mice carrying chimeric lacZ-erythropoietin gene constructs with or without its 1.2 kb 3'-flanking sequence.

机译:带有嵌合lacZ-促红细胞生成素基因构建体的转基因小鼠的lacZ在肝脏和肾脏中的差异表达,带有或不带有其1.2 kb 3'侧翼序列。

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摘要

Erythropoietin (EPO) plays a key role in erythropoiesis and is expressed predominantly in the fetal liver and in the adult kidney. The EPO gene is up-regulated at the transcriptional level under hypoxic/anemic conditions. We studied the role of the 5'- and 3'-flanking sequences of the mouse EPO gene in its tissue-specific and hypoxia-induced expression by developing transgenic mouse lines carrying chimeric EPO-lacZ gene constructs. Transgenic mice carrying a 6.5 kb segment of the 5'-sequence and most of the EPO gene in which lacZ was substituted for exon 1 (5'-lacZ-EPO) demonstrated induction of lacZ expression following hypoxia/ anemia induction in both the liver and kidney of adult mice. However, transgenic mice carrying the above construct along with the 1.2 kb 3'-flanking sequence (5'-lacZ-EPO-3') showed a high level of lacZ expression following hypoxia/anemia induction in adult kidney but not in adult liver. With the aim of further understanding the role of the 3'-flanking sequence in tissue-specific expression of the EPO gene, we studied the interactions of protein factors with this 1.2 kb 3' region and demonstrated that multiple sets of protein factors interact tissue specifically with a 10 bp sequence, TCAAAGATGG, located downstream of the previously characterized 3' hypoxia-responsive enhancer element.
机译:促红细胞生成素(EPO)在促红细胞生成中起关键作用,并主要在胎儿肝脏和成年肾脏中表达。在缺氧/贫血条件下,EPO基因在转录水平上调。我们通过开发携带嵌合EPO-lacZ基因构建体的转基因小鼠品系,研究了小鼠EPO基因的5'和3'侧翼序列在其组织特异性和低氧诱导的表达中的作用。携带6.5 kb片段的5'序列和大部分lacZ替代外显子1(5'-lacZ-EPO)的EPO基因的转基因小鼠在肝脏和肝脏缺氧/贫血诱导后均表现出lacZ表达的诱导。成年小鼠的肾脏。然而,携带上述构建体以及1.2kb 3′-侧翼序列(5′-lacZ-EPO-3′)的转基因小鼠在低氧/贫血诱导后在成年肾脏中表现出高水平的lacZ表达,而在成年肝脏中则没有。为了进一步了解3'侧翼序列在EPO基因的组织特异性表达中的作用,我们研究了蛋白质因子与该1.2 kb 3'区域的相互作用,并证明了多组蛋白质因子特异性地与组织相互作用具有10bp序列的TCAAAGATGG,位于先前表征的3'低氧反应性增强子元件的下游。

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