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首页> 外文期刊>Molecular and Cellular Biochemistry: An International Journal for Chemical Biology >Gene expression pattern in PC12 cells with reduced PMCA2 or PMCA3 isoform: selective up-regulation of calmodulin and neuromodulin.
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Gene expression pattern in PC12 cells with reduced PMCA2 or PMCA3 isoform: selective up-regulation of calmodulin and neuromodulin.

机译:PMCA2或PMCA3亚型减少的PC12细胞中的基因表达模式:钙调蛋白和神经调节蛋白的选择性上调。

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Cellular calcium homeostasis is controlled predominantly by the plasma membrane calcium pump (PMCA). From four PMCA isoforms, PMCA1 and PMCA4 are ubiquitous, while PMCA2 and PMCA3 are found in excitable cells. We have previously shown that suppression of neuron-specific PMCAs in non-differentiated PC12 cells changed the cell morphology and triggered neuritogenesis. Using the microarrays, real-time PCR and immunodetection, we analyzed the effect of PMCA2 or PMCA3 reduction in PC12 cells on gene expression, with emphasis on calmodulin (CaM), neuromodulin (GAP43) and MAP kinases. In PMCA-suppressed lines total CaM increased, and the calm I and calm II genes appeared to be responsible for this effect. mRNA and protein levels of GAP43 were increased, however, the amount of phosphorylated form was lower than in control cells. Localization of CaM/GAP43 and CaM/pGAP43 differed between control and PMCA-reduced cells. In both PMCA-modified lines, amounts of ERK1/2 increased. While pERK1 decreased, the pERK2 level was similar in all examined lines. PMCA suppression did not change the p38 amount, but the p-p38 diminished. JNK2 protein decreased in both PMCA-reduced cells without changes in pJNK level. Microarray analysis revealed distinct expression patterns of certain genes involved in the regulation of cell cycle, proliferation, migration, differentiation, apoptosis and cell signaling. Suppression of neuron-specific PMCA isoforms affected the phenotype of PC12 cells enabling adaptation to the sustained increase in cytosolic Ca(2+) concentration. This is the first report showing function of PMCA2 and PMCA3 isoforms in the regulation of signaling pathways in PC12 cells.
机译:细胞钙稳态主要由质膜钙泵(PMCA)控制。在四种PMCA亚型中,PMCA1和PMCA4普遍存在,而PMCA2和PMCA3在可兴奋细胞中发现。先前我们已经表明,在未分化的PC12细胞中抑制神经元特异性PMCA改变了细胞形态并触发了神经形成。使用微阵列,实时PCR和免疫检测,我们分析了PC12细胞中PMCA2或PMCA3减少对基因表达的影响,重点是钙调蛋白(CaM),神经调节蛋白(GAP43)和MAP激酶。在受PMCA抑制的株系中,总CaM增加,而镇静I和镇静II基因似乎是造成这种效应的原因。 GAP43的mRNA和蛋白质水平增加,但是磷酸化形式的量低于对照细胞。 CaM / GAP43和CaM / pGAP43的定位在对照细胞和PMCA还原细胞之间有所不同。在两个PMCA修饰品系中,ERK1 / 2的量均增加。尽管pERK1降低,但在所有检查的品系中pERK2的水平均相似。 PMCA抑制并没有改变p38的量,但p-p38减少了。在两个PMCA还原的细胞中,JNK2蛋白均下降,而pJNK水平没有变化。微阵列分析揭示了某些基因的不同表达模式,这些基因参与细胞周期,增殖,迁移,分化,凋亡和细胞信号传导的调控。神经元特异性PMCA亚型的抑制影响PC12细胞的表型,使其能够适应细胞溶质Ca(2+)浓度的持续增加。这是第一个报告,显示PMCA2和PMCA3同工型在PC12细胞信号传导途径的调节中的功能。

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