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首页> 外文期刊>Journal of Molecular Biology >Hepatocyte Nuclear Factor 1 alpha Controls Renal Expression of the Npt1-Npt4 Anionic Transporter Locus.
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Hepatocyte Nuclear Factor 1 alpha Controls Renal Expression of the Npt1-Npt4 Anionic Transporter Locus.

机译:肝细胞核因子1α控制Npt1-Npt4阴离子转运蛋白基因座的肾脏表达。

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Hepatocyte nuclear factor 1 alpha (HNF1alpha) is a transcription factor that is expressed in liver, pancreas, kidney and intestine. Mice lacking HNF1alpha are born normally but suffer from several defects including hyperphenylalaninemia, defective bile acid and cholesterol metabolism, an insulin secretion defect and renal Fanconi syndrome. The renal phenotype involves a defect in renal proximal tubule reabsorption, leading to polyuria, glucosuria, aminoaciduria and phosphaturia. We investigated the expression of genes encoding members of the sodium/phosphate cotransporter (Na(+)/Pi) family (namely Npt1, Npt2, Npt4 and Ram1). We show that Npt1 and Npt4 genes were expressed at reduced levels in the kidneys of HNF1alpha -/- mice, whereas the expression of Npt2, the major renal phosphate transporter, was not affected. Analysis of the Npt1 genomic sequence revealed the existence of several alternative promoters activated in liver and/or in kidney. All of these were down-regulated in the kidneys of HNF1alpha -/- animals. Several HNF1alpha binding sites (BS) play an important role in the transcriptional control of this locus, including low-affinity HNF1 BSs localised in a DNase I hypersensitivity site (HSS3). Transient transfection experiments confirmed that HNF1alpha directly transactivates the Npt1 promoter and that the HSS3 region contributes to this activation.
机译:肝细胞核因子1α(HNF1alpha)是在肝,胰腺,肾脏和肠中表达的转录因子。缺乏HNF1alpha的小鼠是正常出生的,但患有多种缺陷,包括高苯丙氨酸血症,胆汁酸和胆固醇代谢缺陷,胰岛素分泌缺陷和肾Fanconi综合征。肾表型涉及肾近端小管重吸收的缺陷,导致多尿,糖尿,氨基酸尿和血尿。我们调查了编码钠/磷酸盐共转运蛋白(Na(+)/ Pi)家族成员的基因的表达(即Npt1,Npt2,Npt4和Ram1)。我们显示Npt1和Npt4基因在HNF1alpha-/-小鼠的肾脏中以降低的水平表达,而Npt2,主要的肾磷酸盐转运蛋白,的表达不受影响。 Npt1基因组序列的分析揭示了在肝脏和/或肾脏中激活的几种替代启动子的存在。所有这些在HNF1alpha-/-动物的肾脏中均下调。几个HNF1alpha结合位点(BS)在此基因座的转录控制中发挥重要作用,包括位于DNase I超敏性位点(HSS3)中的低亲和力HNF1 BS。瞬时转染实验证实,HNF1alpha直接激活Npt1启动子,而HSS3区域有助于这种激活。

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