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与酪氨酸转氨酶基因发育调控相关的远端增强子与肝脏特异性因子和普遍存在的因子结合。

The distal enhancer implicated in the developmental regulation of the tyrosine aminotransferase gene is bound by liver-specific and ubiquitous factors.

作者信息

Nitsch D, Schütz G

机构信息

Division Molecular Biology of the Cell I, German Cancer Research Center, Heidelberg.

出版信息

Mol Cell Biol. 1993 Aug;13(8):4494-504. doi: 10.1128/mcb.13.8.4494-4504.1993.

Abstract

Tyrosine aminotransferase gene expression is confined to parenchymal cells of the liver, is inducible by glucocorticoids and glucagon, and is repressed by insulin. Three enhancers control this tissue-specific and hormone-dependent activity, one of which, located at -11 kb, is implicated in establishing an active expression domain. We have studied in detail this important regulatory element and have identified a 221-bp fragment containing critical enhancer sequences which stimulated the heterologous thymidine kinase promoter more than 100-fold in hepatoma cells. Within this region, we have characterized two essential liver-specific enhancer domains, one of which was bound by proteins of the hepatocyte nuclear factor 3 (HNF3) family. Analyses with the dedifferentiated hepatoma cell line HTC suggested that HNF3 alpha and/or -gamma, but not HNF3 beta, are involved in activating the tyrosine aminotransferase gene via the -11-kb enhancer. Genomic footprinting and in vitro protein-DNA binding studies documented cell-type-specific binding of ubiquitous factors to the second essential enhancer domain, which by itself stimulated the thymidine kinase promoter preferentially in hepatoma cells. These results will allow further characterization of the role of these enhancer sequences in developmental activation of the tyrosine aminotransferase gene.

摘要

酪氨酸转氨酶基因的表达仅限于肝脏实质细胞,可被糖皮质激素和胰高血糖素诱导,并被胰岛素抑制。有三个增强子控制这种组织特异性和激素依赖性活性,其中一个位于-11 kb处,与建立一个活跃的表达结构域有关。我们已经详细研究了这个重要的调控元件,并鉴定出一个含有关键增强子序列的221 bp片段,该片段在肝癌细胞中能将异源胸苷激酶启动子刺激100倍以上。在这个区域内,我们鉴定了两个必需的肝脏特异性增强子结构域,其中一个与肝细胞核因子3(HNF3)家族的蛋白质结合。对去分化的肝癌细胞系HTC的分析表明,HNF3α和/或-γ,而非HNF3β,通过-11 kb增强子参与激活酪氨酸转氨酶基因。基因组足迹分析和体外蛋白质-DNA结合研究证明,普遍存在的因子与第二个必需增强子结构域存在细胞类型特异性结合,该结构域本身在肝癌细胞中优先刺激胸苷激酶启动子。这些结果将有助于进一步阐明这些增强子序列在酪氨酸转氨酶基因发育激活中的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9d8f/360060/41c21e5aaaa9/molcellb00020-0054-a.jpg

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