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醛固酮和血管升压素影响α-和γ-上皮钠通道(ENaC)的信使核糖核酸(mRNA)翻译。

Aldosterone and vasopressin affect {alpha}- and {gamma}-ENaC mRNA translation.

作者信息

Perlewitz Andrea, Nafz Benno, Skalweit Angela, Fähling Michael, Persson Pontus B, Thiele Bernd-Joachim

机构信息

Institut für Vegetative Physiologie, Universitätsmedizin Berlin (Charité), D-10117 Berlin, Germany.

出版信息

Nucleic Acids Res. 2010 Sep;38(17):5746-60. doi: 10.1093/nar/gkq267. Epub 2010 May 7.

Abstract

Vasopressin and aldosterone play key roles in the fine adjustment of sodium and water re-absorption in the nephron. The molecular target of this regulation is the epithelial sodium channel (ENaC) consisting of α-, β- and γ-subunits. We investigated mRNA-specific post-transcriptional mechanisms in hormone-dependent expression of ENaC subunits in mouse kidney cortical collecting duct cells. Transcription experiments and polysome gradient analysis demonstrate that both hormones act on transcription and translation. RNA-binding proteins (RBPs) and mRNA sequence motifs involved in translational control of γ-ENaC synthesis were studied. γ-ENaC-mRNA 3'-UTR contains an AU-rich element (ARE), which was shown by RNA affinity chromatography to interact with AU-rich element binding proteins (ARE-BP) like HuR, AUF1 and TTP. Some RBPs co-localized with γ-ENaC mRNA in polysomes in a hormone-dependent manner. Reporter gene co-expression experiments with luciferase γ-ENaC 3'-UTR constructs and ARE-BP expression plasmids demonstrate the importance of RNA-protein interaction for the up-regulation of γ-ENaC synthesis. We document that aldosterone and the V(2) receptor agonist dDAVP act on synthesis of α- and γ-ENaC subunits mediated by RBPs as effectors of translation but not by mRNA stabilization. Immunoprecipitation and UV-crosslinking analysis of γ-ENaC-mRNA/HuR complexes document the significance of γ-ENaC-mRNA-3'-UTR/HuR interaction for hormonal control of ENaC synthesis.

摘要

血管加压素和醛固酮在肾单位钠和水重吸收的精细调节中发挥关键作用。这种调节的分子靶点是由α、β和γ亚基组成的上皮钠通道(ENaC)。我们研究了小鼠肾皮质集合管细胞中ENaC亚基激素依赖性表达的mRNA特异性转录后机制。转录实验和多核糖体梯度分析表明,这两种激素均作用于转录和翻译过程。我们研究了参与γ-ENaC合成翻译控制的RNA结合蛋白(RBP)和mRNA序列基序。γ-ENaC-mRNA的3'-非翻译区(UTR)包含一个富含AU的元件(ARE),RNA亲和色谱显示该元件可与HuR、AUF1和TTP等富含AU元件结合蛋白(ARE-BP)相互作用。一些RBP以激素依赖性方式与多核糖体中的γ-ENaC mRNA共定位。荧光素酶γ-ENaC 3'-UTR构建体与ARE-BP表达质粒的报告基因共表达实验证明了RNA-蛋白质相互作用对γ-ENaC合成上调的重要性。我们证明,醛固酮和V(2)受体激动剂dDAVP作用于由RBP介导的α-和γ-ENaC亚基的合成,RBP作为翻译效应因子,而非通过mRNA稳定化发挥作用。γ-ENaC-mRNA/HuR复合物的免疫沉淀和紫外线交联分析证明了γ-ENaC-mRNA-3'-UTR/HuR相互作用对ENaC合成激素控制的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5bda/2943617/1baae542daea/gkq267f1.jpg

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