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Novel regulatory function for NHERF-1 in Npt2a transcription

机译:NHERF-1在Npt2a转录中的新型调控功能

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摘要

Several lines of evidence show that sodium/hydrogen exchanger regulatory factor 1 (NHERF-1) regulates the expression and activity of the type IIa sodium-dependent phosphate transporter (Npt2a) in renal proximal tubules. We have previously demonstrated that expression of a COOH-terminal ezrin binding domain-deficient NHERF-1 in opossum kidney (OK) cells decreased expression of Npt2a in apical membranes but did not affect responses to parathyroid hormone. We hypothesized that NHERF-1 regulates apical membrane expression of Npt2a in renal proximal tubule cells. To address this hypothesis, we compared regulation of Npt2a expression and function in NHERF-deficient OK cells (OK-H) and wild-type cells (OK-WT). In OK-H cells, phosphate uptake and expression of Npt2a protein in apical membranes were significantly lower than in OK-WT cells. Transient transfection of green fluorescent protein-tagged Npt2a cDNA into OK-H cells resulted in aberrant localization of an Npt2a fragment to the cytosol but not to the apical membrane. OK-H cells also exhibited a marked decrease in Npt2a mRNA expression. As demonstrated by luciferase assay, Npt2a promoter activity was significantly decreased in OK-H cells compared with that shown in OK-WT cells. Transfection of OK-H cells with human NHERF-1 restored Npt2a expression at both the protein and mRNA levels and regulation by parathyroid hormone. Expression of NHERF-1 constructs with mutations in the PDZ domains or the ezrin binding domain in OK-H cells suggested that the PDZ2 domain is critical for apical translocation of Npt2a and for expression at the mRNA level. Our data demonstrate for the first time that NHERF-1 regulates Npt2a transcription and membrane insertion.
机译:几条证据表明,钠/氢交换调节因子1(NHERF-1)调节肾近端小管中IIa型钠依赖性磷酸转运蛋白(Npt2a)的表达和活性。我们以前已经证明,在负鼠肾(OK)细胞中COOH末端ezrin结合域缺陷NHERF-1的表达降低了顶膜Npt2a的表达,但不影响对甲状旁腺激素的反应。我们假设NHERF-1调节肾近端小管细胞中Npt2a的顶膜表达。为了解决这个假设,我们比较了NptF缺失的OK细胞(OK-H)和野生型细胞(OK-WT)中Npt2a表达和功能的调节。在OK-H细胞中,其根尖膜的磷酸盐吸收和Npt2a蛋白的表达显着低于OK-WT细胞。将绿色荧光蛋白标记的Npt2a cDNA瞬时转染到OK-H细胞中会导致Npt2a片段异常定位在细胞质内,而不是在心尖膜上。 OK-H细胞还表现出Npt2a mRNA表达的明显下降。如荧光素酶测定所证实,与OK-WT细胞中显示的相比,OK-H细胞中Npt2a启动子活性显着降低。用人NHERF-1转染OK-H细胞可恢复Npt2a在蛋白质和mRNA水平上的表达以及甲状旁腺激素的调控。在OK-H细胞中PDZ结构域或ezrin结合结构域中突变的NHERF-1构建体的表达表明,PDZ2结构域对于Npt2a的根尖转运和在mRNA水平的表达至关重要。我们的数据首次证明NHERF-1调节Npt2a转录和膜插入。

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