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首页> 外文期刊>Hepatology: Official Journal of the American Association for the Study of Liver Diseases >Selenoprotein P expression is controlled through interaction of the coactivator PGC-1alpha with FoxO1a and hepatocyte nuclear factor 4alpha transcription factors.

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Selenoprotein P expression is controlled through interaction of the coactivator PGC-1alpha with FoxO1a and hepatocyte nuclear factor 4alpha transcription factors.

机译：硒蛋白P的表达是通过辅助激活剂PGC-1alpha与FoxO1a和肝细胞核因子4alpha转录因子的相互作用来控制的。

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Selenoprotein P (SeP), the major selenoprotein in plasma, is produced mainly by the liver, although SeP expression is detected in many organs. Recently, we reported stimulation of SeP promoter activity by the forkhead box transcription factor FoxO1a in hepatoma cells and its attenuation by insulin. Here, we demonstrate that this translates into fine-tuning of SeP production and secretion by insulin. Overexpression of peroxisomal proliferator activated receptor-gamma coactivator 1alpha (PGC-1alpha) enhanced the stimulatory effect of FoxO1a on SeP promoter activity. We identified a novel functional binding site for hepatocyte nuclear factor (HNF)-4alpha, termed hepatocyte nuclear factor binding element 1, in the human SeP promoter directly upstream of the FoxO-responsive element daf16-binding element 2 (DBE2). Point mutations in hepatocyte nuclear factor binding element 1 alone or together with DBE2 decreased basal activity and responsiveness of the SeP promoter to PGC-1alpha. Moreover, the PGC-1alpha-inducing glucocorticoid dexamethasone strongly enhanced SeP messenger RNA levels and protein secretion in cultured rat hepatocytes, whereas insulin suppressed the stimulation of both PGC-1alpha and SeP caused by dexamethasone treatment. In a brain-derived neuroblastoma cell line with low basal SeP expression, SeP transcription was stimulated by PGC-1alpha together with FoxO1a, and overexpression of HNF-4alpha potentiated this effect. Conclusion: High-level expression of SeP in liver is ensured by concerted action of the coactivator PGC-1alpha and the transcription factors FoxO1a and HNF-4alpha. Hence, the production of SeP is regulated similarly to that of the gluconeogenic enzyme glucose-6-phosphatase. As hepatic SeP production is crucial for selenium distribution throughout the body, the present study establishes PGC-1alpha as a key regulator of selenium homeostasis.

机译：硒蛋白P（SeP）是血浆中的主要硒蛋白，主要由肝脏产生，尽管在许多器官中都检测到SeP表达。最近，我们报道了叉头盒转录因子FoxO1a在肝癌细胞中刺激SeP启动子活性，并被胰岛素减弱。在这里，我们证明这转化为SeP产生和胰岛素分泌的微调。过氧化物酶体增殖物激活受体-γ共激活因子1alpha（PGC-1alpha）的过表达增强了FoxO1a对SeP启动子活性的刺激作用。我们在人类SeP启动子中直接在FoxO反应元件daf16结合元件2（DBE2）的上游发现了肝细胞核因子（HNF）-4alpha的新功能结合位点，称为肝细胞核因子结合元件1。单独或与DBE2一起的肝细胞核因子结合元件1中的点突变降低了基础活性和SeP启动子对PGC-1alpha的反应性。此外，PGC-1α诱导的糖皮质激素地塞米松强烈增强了培养的大鼠肝细胞中SeP信使RNA的水平和蛋白质分泌，而胰岛素抑制了地塞米松治疗对PGC-1alpha和SeP的刺激。在具有低基础SeP表达的脑源性神经母细胞瘤细胞系中，PGC-1alpha和FoxO1a共同刺激了SeP转录，HNF-4alpha的过表达增强了这种效果。结论：辅激活物PGC-1alpha与转录因子FoxO1a和HNF-4alpha的协同作用确保了SeP在肝脏中的高水平表达。因此，SeP的产生与糖异生酶葡萄糖-6-磷酸酶的产生类似地受到调节。由于肝SeP的产生对于硒在体内的分布至关重要，因此本研究建立了PGC-1alpha作为硒稳态的关键调节剂。

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来源
《Hepatology: Official Journal of the American Association for the Study of Liver Diseases》 |2008年第6期|共9页
作者
Speckmann B; Walter PL; Alili L; Reinehr R; Sies H; Klotz LO; Steinbrenner H;
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正文语种 eng
中图分类消化系及腹部疾病;
关键词
Transcription Factors; Elements; hepatocyte nuclear factor; binding; 转录因子; 元素;

机译：Transcription Factors;Elements;hepatocyte nuclear factor;binding;转录因子;元素;

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专利

1. Selenoprotein P expression is controlled through interaction of the coactivator PGC-1alpha with FoxO1a and hepatocyte nuclear factor 4alpha transcription factors. [J] . Speckmann B, Walter PL, Alili L, Hepatology: Official Journal of the American Association for the Study of Liver Diseases . 2008,第6期

机译：硒蛋白P的表达是通过辅助激活剂PGC-1alpha与FoxO1a和肝细胞核因子4alpha转录因子的相互作用来控制的。
2. Inhibition of CYP3A4 expression by ketoconazole is mediated by the disruption of pregnane X receptor, steroid receptor coactivator-1, and hepatocyte nuclear factor 4alpha interaction. [J] . Lim YP, Kuo SC, Lai ML, Pharmacogenetics and genomics . 2009,第1期

机译：酮康唑对CYP3A4表达的抑制作用是由孕烷X受体，类固醇受体共激活因子1和肝细胞核因子4α相互作用的破坏介导的。
3. Rifampicin induction of CYP3A4 requires pregnane X receptor cross talk with hepatocyte nuclear factor 4alpha and coactivators, and suppression of small heterodimer partner gene expression. [J] . Li T, Chiang JY Drug Metabolism and Disposition: The Biological Fate of Chemicals . 2006,第5期

机译：利福平对CYP3A4的诱导需要与肝细胞核因子4α和共激活因子进行孕烷X受体交叉干扰，并抑制小的异二聚体伴侣基因表达。
4. Helicomimetic cyclic peptides that inhibit steroid receptor coactivator interactions represent a novel approach for transcriptional regulation [C] . Arno F.Spatola, Amit Galande, Anne-Marie Leduc, European Peptide Symposium . 2002

机译：抑制类固醇受体共膜剂相互作用的直升环状肽代表了一种转录调控的新方法
5. Determinants of cofactor recruitment and transcriptional activity for hepatocyte nuclear factor 4alpha (HNF4alpha). [D] . Ruse, Michael Dean, Jr. 2002

机译：肝细胞核因子4α（HNF4alpha）的辅助因子募集和转录活性的决定因素。
6. Cell-extracellular matrix interactions can regulate the switch between growth and differentiation in rat hepatocytes: reciprocal expression of C/EBP alpha and immediate-early growth response transcription factors. [O] . B Rana, D Mischoulon, Y Xie, 1994

机译：细胞与细胞外基质的相互作用可以调节大鼠肝细胞在生长与分化之间的转换：C / EBPα的相互表达和即刻早期生长反应转录因子。
7. Cell-extracellular matrix interactions can regulate the switch between growth and differentiation in rat hepatocytes: reciprocal expression of C/EBP alpha and immediate-early growth response transcription factors. [O] . Rana, B, Mischoulon, D, Xie, Y, 1994

机译：细胞与细胞外基质的相互作用可以调节大鼠肝细胞在生长与分化之间的转换：C / EBPα的相互表达和即刻早期生长反应转录因子。
8. Maintenance of Glucose Homeostasis through Acetylation of the Metabolic Transcriptional Coactivator PGC-1alpha; Annual rept. 9 Jan 2007-8 Jan 2008 [R] . Puigserver, P. 2008

机译：通过代谢转录共激活因子pGC-1α的乙酰化维持葡萄糖稳态;年度报告。 2007年1月9日至2008年1月8日

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