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首页> 外文期刊>The Journal of Physiology >Calcineurin involvement in the regulation of high-threshold Ca2+ channels in NG108-15 (rodent neuroblastoma x glioma hybrid) cells.
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Calcineurin involvement in the regulation of high-threshold Ca2+ channels in NG108-15 (rodent neuroblastoma x glioma hybrid) cells.

机译:钙调神经磷酸酶参与调节NG108-15(啮齿类神经母细胞瘤x胶质瘤杂种)细胞中高阈值Ca2 +通道。

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摘要

1. We examined the relationship between calcineurin (protein phosphatase 2B (PP2B) and voltage-operated Ca2+ channels (VOCCs) in NG108-15 cells. PP2B expression in NG108-15 cells was altered by transfection with plasmid constructs containing a full length cDNA of human PP2B beta(3) in sense (CN-15) and antisense (CN-21) orientation. 2. Confocal immunocytochemical localization showed that in wild-type cells, PP2B immunoreactivity is uniformly distributed in undifferentiated cells and located at the inner surface of soma membrane and neurites in differentiated cells. 3. To test the Ca2+ dependence of the VOCC, we used high-frequency stimulation (HFS). The L- and N-type VOCCs decreased by 37 and 52%, respectively, whereas the T-type current was only marginally sensitive to this procedure. FK-506 (2 microM), a specific blocker of PP2B, reduced the inhibition of L- and N-type VOCCs induced by HFS by 30 and 33%, respectively. 4. In CN-15-transfected cells overexpressing PP2B, total high-voltage-activated (HVA) VOCCs were suppressed by about 60% at a test potential of +20 mV. Intracellular addition of EGTA or FK-506 into CN-15-transfected cells induced an up to 5-fold increase of HVA VOCCs. 5. These findings indicate that PP2B activity does not influence the expression of HVA Ca2+ channels, but modulates their function by Ca(2+)-dependent dephosphorylation. Thus HVA VOCCs, in a phosphorylated state under control conditions, are downregulated by PP2B upon stimulation, with the major effect on N-type VOCCs.
机译:1.我们研究了钙调神经磷酸酶(蛋白磷酸酶2B(PP2B))与NG108-15细胞中电压控制的Ca2 +通道(VOCC)之间的关系,通过转染全长cDNA的质粒构建体改变了NG108-15细胞中PP2B的表达。人类PP2B beta(3)处于有义(CN-15)和反义(CN-21)方向; 2.共聚焦免疫细胞化学定位显示,在野生型细胞中,PP2B免疫反应性均匀地分布在未分化的细胞中,并位于细胞的内表面3.为了测试VOCC对Ca2 +的依赖性,我们使用了高频刺激(HFS),其中L型和N型VOCC分别降低了37%和52%,而T型类型电流仅对该程序稍有敏感,PP2B的特异阻滞剂FK-506(2 microM)分别将HFS诱导的L型和N型VOCC的抑制作用分别降低了30%和33%。4.在CN中-15转染的细胞过表达PP2B,总高电压在+20 mV的测试电势下,年龄激活(HVA)VOCC被抑制了约60%。 EGTA或FK-506的细胞内添加到CN-15转染的细胞中导致HVA VOCC最多增加5倍。 5.这些发现表明PP2B活性不会影响HVA Ca2 +通道的表达,但会通过Ca(2+)依赖性去磷酸化来调节其功能。因此,在控制条件下处于磷酸化状态的HVA VOCC受刺激后被PP2B下调,对N型VOCC具有主要作用。

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