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首页> 美国卫生研究院文献>Molecular and Cellular Biology >Decreased expression of hepatocyte nuclear factor 3 alpha during the acute-phase response influences transthyretin gene transcription.
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Decreased expression of hepatocyte nuclear factor 3 alpha during the acute-phase response influences transthyretin gene transcription.

机译:急性期反应期间肝细胞核因子3α表达的降低影响运甲状腺素蛋白基因转录。

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Three distinct hepatocyte nuclear factor 3 (HNF-3) proteins (alpha, beta, and gamma) are known to regulate the transcription of numerous liver-specific genes. The HNF-3 proteins bind to DNA as monomers through a winged-helix motif, which is also utilized by a number of developmental regulators, including the Drosophila homeotic fork head (fkh) protein. We have previously characterized a strong-affinity HNF-3S site in the transthyretin (TTR) promoter region which is essential for expression in human hepatoma (HepG2) cells. In the current study, we identify an activating protein 1 (AP-1) site which partially overlaps the HNF-3S sequence in the TTR promoter. We show that in HepG2 cells the AP-1 sequence confers 12-O-tetradecanoylphorbol-13-acetate inducibility to the TTR promoter and contributes to normal TTR transcriptional activity. We also demonstrate that the HNF-3 proteins and AP-1 bind independently to the TTR AP-1-HNF-3 site, and cotransfection experiments suggest that they do not cooperate to activate an AP-1-HNF-3 reporter construct. In addition, 12-O-tetradecanoylphorbol-13-acetate exposure of HepG2 cells results in a reciprocal decrease in HNF-3 alpha and -3 gamma expression which may facilitate interaction of AP-1 with the TTR AP-1-HNF-3 site. In order to explore the role of HNF-3 in the liver, we have examined expression patterns of TTR and HNF-3 during the acute-phase response and liver regeneration. Partial hepatectomy produced minimal fluctuation in HNF-3 and TTR expression, suggesting that HNF-3 expression is not influenced by proliferative signals induced during liver regeneration. In acute-phase livers, we observed a dramatic reduction in HNF-3 alpha expression which correlates with a decrease in the expression of its target gene, the TTR gene. Furthermore, consistent with previous studies, the acute-phase livers are induced for c-jun but not c-fos expression. We propose that the reduction in TTR gene expression during the acute phase is likely due to lower HNF-3 alpha expression levels and that the induction of primarily c-jun homodimers, which are poor transcriptional activators, is insufficient to maintain normal TTR expression levels. We also discuss the role of reduced HNF-3 alpha expression in mediating decreased transcription of HNF-3 target genes which respond negatively to cytokine signalling.
机译:已知三种不同的肝细胞核因子3(HNF-3)蛋白(α,β和γ)调节许多肝脏特异性基因的转录。 HNF-3蛋白通过有翼螺旋基序与DNA结合成单体,这也被包括果蝇顺势叉头(fkh)蛋白在内的许多发育调节剂所利用。我们以前已经在转甲状腺素蛋白(TTR)启动子区域中表征了强亲和力的HNF-3S位点,这对于在人肝癌(HepG2)细胞中表达至关重要。在当前的研究中,我们确定了一个激活蛋白1(AP-1)位点,该位点与TTR启动子中的HNF-3S序列部分重叠。我们显示,在HepG2细胞中,AP-1序列赋予TTR启动子12-O-十四烷酰phorbol-13-乙酸盐诱导性,并有助于正常的TTR转录活性。我们还证明了HNF-3蛋白和AP-1独立地结合到TTR AP-1-HNF-3位点,并且共转染实验表明它们不协同激活AP-1-HNF-3报告基因构建体。此外,HepG2细胞的12-O-十四烷酰phorbol-13-乙酸盐暴露会导致HNF-3α和-3γ表达的倒数减少,这可能促进AP-1与TTR AP-1-HNF-3位点的相互作用。为了探讨HNF-3在肝脏中的作用,我们检查了急性期反应和肝再生过程中TTR和HNF-3的表达模式。肝部分切除术在HNF-3和TTR表达上产生的波动很小,表明HNF-3表达不受肝脏再生过程中诱导的增殖信号的影响。在急性期肝脏中,我们观察到HNF-3α表达急剧下降,这与其靶基因TTR基因的表达下降有关。此外,与先前的研究一致,急性期肝脏被诱导产生c-jun而不是c-fos表达。我们提出,急性期TTR基因表达的降低很可能是由于较低的HNF-3α表达水平引起的,并且主要是c-jun同型二聚体(其是转录激活因子)的诱导不足以维持正常的TTR表达水平。我们还讨论了减少HNF-3 alpha表达在介导对细胞因子信号产生负响应的HNF-3靶基因转录降低中的作用。

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