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PC12神经突中的钙离子波:一种双向的、以受体为导向的钙离子信号传导形式。

Ca2+ waves in PC12 neurites: a bidirectional, receptor-oriented form of Ca2+ signaling.

作者信息

Lorenzon P, Zacchetti D, Codazzi F, Fumagalli G, Meldolesi J, Grohovaz F

机构信息

Department of Pharmacology, University of Milano, Italy.

出版信息

J Cell Biol. 1995 May;129(3):797-804. doi: 10.1083/jcb.129.3.797.

Abstract

Spatial and temporal aspects of Ca2+ signaling were investigated in PC12 cells differentiated with nerve growth factor, the well known nerve cell model. Activation of receptors coupled to polyphosphoinositide hydrolysis gave rise in a high proportion of the cells to Ca2+ waves propagating non decrementally and at constant speed (2-4 microns/s at 18 degrees C and approximately 10-fold faster at 37 degrees C) along the neurites. These waves relied entirely on the release of Ca2+ from intracellular stores since they could be generated even when the cells were incubated in Ca(2+)-free medium. In contrast, when the cells were depolarized with high K+ in Ca(2+)-containing medium, increases of cytosolic Ca2+ occurred in the neurites but failed to evolve into waves. Depending on the receptor agonist employed (bradykinin and carbachol versus ATP) the orientation of the waves could be opposite, from the neurite tip to the cell body or vice versa, suggesting different and specific distribution of the responsible surface receptors. Cytosolic Ca2+ imaging results, together with studies of inositol 1,4,5-trisphosphate generation in intact cells and inositol 1,4,5-trisphosphate-induced Ca2+ release from microsomes, revealed the sustaining process of the waves to be discharge of Ca2+ from the inositol 1,4,5-trisphosphate- (and not the ryanodine-) sensitive stores distributed along the neurites. The activation of the cognate receptor appears to result from the coordinate action of the second messenger and Ca2+. Because of their properties and orientation, the waves could participate in the control of not only conventional cell activities, but also excitability and differential processing of inputs, and thus of electrochemical computation in nerve cells.

摘要

在经神经生长因子分化的PC12细胞(一种著名的神经细胞模型)中研究了Ca2+信号的时空特性。与多磷酸肌醇水解偶联的受体激活在很大比例的细胞中引发了Ca2+波,这些波以恒定速度(18℃时为2 - 4微米/秒,37℃时快约10倍)沿神经突非递减地传播。这些波完全依赖于细胞内钙库释放Ca2+,因为即使细胞在无Ca2+的培养基中孵育时也能产生。相反,当细胞在含Ca2+的培养基中用高K+使其去极化时,神经突中胞质Ca2+增加,但未能演变成波。根据所使用的受体激动剂(缓激肽和卡巴胆碱与ATP)不同,波的传播方向可能相反,从神经突尖端到细胞体或反之亦然,这表明负责的表面受体存在不同且特定的分布。胞质Ca2+成像结果,连同对完整细胞中肌醇1,4,5 - 三磷酸生成以及肌醇1,4,5 - 三磷酸诱导的微粒体Ca2+释放的研究,揭示了波的维持过程是Ca2+从沿神经突分布的对肌醇1,4,5 - 三磷酸(而非雷诺丁)敏感的钙库中释放。同源受体的激活似乎是第二信使和Ca2+协同作用的结果。由于其特性和传播方向,这些波不仅可以参与传统细胞活动的控制,还可以参与兴奋性和输入的差异处理,进而参与神经细胞中的电化学计算。

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