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培养的大鼠星形胶质细胞中受体诱导的细胞间钙信号启动和传播所涉及的机制。

Mechanism involved in initiation and propagation of receptor-induced intercellular calcium signaling in cultured rat astrocytes.

作者信息

Venance L, Stella N, Glowinski J, Giaume C

机构信息

Institut National de la Santé et de la Recherche Médicale, U114, Collège de France, 75231 Paris, Cedex 05, France.

出版信息

J Neurosci. 1997 Mar 15;17(6):1981-92. doi: 10.1523/JNEUROSCI.17-06-01981.1997.

Abstract

The mechanisms involved in the initiation and the propagation of intercellular calcium signaling (calcium waves) were studied in cultured rat astrocytes. The analysis of calcium waves, induced either by mechanical stimulation or by focal application of ionomycin, indicated that initiation was dependent on the presence of external calcium. In addition, pharmacological experiments indicate that intercellular propagation required PLC activation, integrity of IP3-sensitive internal calcium stores, and functional gap junctions. An extracellular action of ATP or glutamate and participation of voltage-dependent Ca2+ channels were tested by using enzymatic degradation, receptor antagonists, and channel blockers, respectively. Because neither the speed of propagation nor the extent of the calcium waves was affected by these treatments, these alternate mechanisms were excluded from playing a role in intercellular calcium signaling. Biochemical assays and focal applications of several agonists (methoxamine, carbachol, glutamate) of membrane receptors to neurotransmitters and peptides (endothelin 1) demonstrated that their ability to trigger regenerative calcium waves depended on phospholipase C activity and inositol phosphate production. Thus, in rat astrocytes, initiation and propagation of calcium waves involve a sequence of intra- and intercellular steps in which phospholipase C, inositol trisphosphate, internal calcium stores, and gap junction channels play a critical role. The identification of these different events allows us to determine several targets at which the level of long-range signaling in astrocytes may be controlled.

摘要

在培养的大鼠星形胶质细胞中研究了细胞间钙信号(钙波)起始和传播所涉及的机制。对机械刺激或离子霉素局部应用诱导的钙波分析表明,起始依赖于细胞外钙的存在。此外,药理学实验表明,细胞间传播需要PLC激活、IP3敏感的细胞内钙库完整性和功能性缝隙连接。分别使用酶降解、受体拮抗剂和通道阻滞剂测试了ATP或谷氨酸的细胞外作用以及电压依赖性Ca2+通道的参与情况。由于这些处理均未影响钙波的传播速度和范围,因此排除了这些替代机制在细胞间钙信号中的作用。对几种神经递质和肽(内皮素1)膜受体激动剂(甲氧明、卡巴胆碱、谷氨酸)的生化分析和局部应用表明,它们触发再生钙波的能力取决于磷脂酶C活性和肌醇磷酸生成。因此,在大鼠星形胶质细胞中,钙波的起始和传播涉及一系列细胞内和细胞间步骤,其中磷脂酶C、肌醇三磷酸、细胞内钙库和缝隙连接通道起关键作用。对这些不同事件的识别使我们能够确定几个可控制星形胶质细胞中远程信号水平的靶点。

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