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Functional Importance of PMCA Isoforms in Growth and Development of PC12 Cells

机译:PMCA同种型在PC12细胞增长和开发中的功能性重要性

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Intracellular Ca~(2+) in neuronal cells is an essential regulatory ion responsible for excitability, synaptic plasticity, and neurite outgrowth. Plasma membrane calcium ATPase (PMCA) is the most sensitive enzyme in decreasing of the Ca~(2+) concentration. The diverse PMCA isoforms composition in the membranes suggests their specific function in the cell, and whereas PMCA1 and 4 appear to be ubiquitous, PMCA2 and 3 are characteristic isoforms for excitable cells. The aim of our study was to elucidate if and how the elimination of neuron-specific isoforms affects the pattern of cell growth and development. We have obtained stable-transfected PC12 cell lines with a suppressed expression of PMCA2, PMCA3, or both neuron-specific isoforms. The modified profile of PMCA generated considerable changes in morphology of examined PC12 lines, suggesting the activation of a differentiation process to pseudoneuronal phenotype. Experiments with Fura-2/AM-loaded cells revealed an increased cytosolic Ca~(2+) concentration in the cell lines with blocked PMCA2 isoform. The suppression of PMCA2 concomitantly altered expression of sarco/endoplasmic Ca~(2+)-ATPase 2 isoform (SERCA2) at the protein level. Comparative flow cytometry analysis, using Annexin V/PI conjugate, showed the difference in the mean percentage of apoptotic cells in modified PC12 lines. Our data suggest that specific PMCA isoforms presence can regulate the intact cell development; however, it may involve multiple unidentified yet signaling pathways.
机译:神经元细胞的细胞内Ca〜(2+)是对兴奋性,突触塑性和神经突的生长负责的基本调节离子。血浆膜钙ATP酶(PMCA)是最敏感的酶在降低Ca〜(2+)浓度。膜中的多样性PMCA同种型组合物表明它们在细胞中的特定功能,而PMCA1和4似乎是普遍的,PMCA2和3是可激发细胞的特征异构型。我们的研究目的是阐明何处以及如何消除神经元特异性同种型的影响会影响细胞生长和发育的模式。我们已经获得了稳定转染的PC12细胞系,抑制了PMCA2,PMCA3或神经元特异性同种型的表达。 PMCA的修改型材产生了检查的PC12线的形态的显着变化,表明将分化过程激活到伪脉络表型。呋喃-2 / am加载细胞的实验显示细胞系中的细胞溶质Ca〜(2+)浓度增加,具有封闭的PMCA2同种型。 PMCA2的抑制在蛋白质水平上伴随着Sarco /内质Ca〜(2 +) - ATP酶2同种型(Serca2)的表达。使用膜蛋白v / pi缀合物的比较流式细胞术分析显示了改性PC12线中凋亡细胞平均百分比的差异。我们的数据表明,特定的PMCA同种型存在可能会调节完整的细胞开发;但是,它可能涉及多个未识别的尚未发信号通路。

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