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Gap junctional communication and pharmacological heterogeneity in astrocytes cultured from the rat striatum.

机译:从大鼠纹状体培养的星形胶质细胞中间隙连接通讯和药理异质性。

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Indo-1 and fluo-3 imaging techniques were used to investigate the role of gap junctions in the changes in cytosolic calcium concentrations ([Ca2+]i) induced by several receptor agonists. Subpopulations of confluent cultured astrocytes from the rat striatum were superfused with submaximal concentrations of endothelin-1 (Et1) and the alpha 1-adrenergic and muscarinic receptor agonists, methoxamine and carbachol, respectively. 2. Combined binding and autoradiographic studies indicated that all striatal astrocytes possess binding sites for Et1. In contrast, alpha 1-adrenergic and muscarinic binding sites were found to be heterogeneously distributed. In agreement with these findings, Et1 induced fast calcium responses in all cells while only subsets of striatal astrocytes responded to the application of methoxamine or carbachol. 3. Halothane, heptanol and octanol, which are commonly used as gap junction inhibitors, drastically reduced the amplitude of Et1-induced calcium responses. In contrast, 18-alpha-glycyrrhetinic acid (alpha GA) used at a concentration known to block gap junction permeability in astrocytes had no significant effect on the amplitude of these calcium responses. 4. As demonstrated by quantitative and topological analysis, Et1 application similarly increased [Ca2+]i levels in all astrocytes in both the absence and presence of alpha GA. 5. In control conditions, subpopulations of cells responding to methoxamine or carbachol exhibited two main types of calcium responses which differed in their shape and kinetic characteristics. In the presence of alpha GA the number of cells responding to these receptor agonists was significantly reduced. Indeed, responses characterized by their long latency, slow rise time and weak amplitude disappeared in the presence of alpha GA while responses with short latency and fast rise time were preserved. 6. These results indicate that permeable gap junction channels tend to attenuate the pharmacological and functional heterogeneity of populations of astrocytes, while their inhibition restricts calcium responses in astrocytes expressing high densities of transmitter receptors coupled to phospholipase C.
机译:Indo-1和fluo-3成像技术用于研究间隙连接在几种受体激动剂诱导的胞浆钙浓度([Ca2 +] i)变化中的作用。将来自大鼠纹状体的融合培养星形胶质细胞亚群分别与亚最大浓度的内皮素-1(Et1)和α1-肾上腺素和毒蕈碱受体激动剂,甲氧明和卡巴胆碱进行超融合。 2.结合结合和放射自显影研究表明,所有纹状体星形胶质细胞都具有Et1的结合位点。相反,发现α1-肾上腺素和毒蕈碱结合位点是异质分布的。与这些发现一致,Et1在所有细胞中诱导快速的钙反应,而仅纹状体星形胶质细胞的一部分对甲氧明或卡巴胆碱的应用有反应。 3.氟烷,庚醇和辛醇通常用作间隙连接抑制剂,可大大降低Et1诱导的钙反应的幅度。相反,已知浓度的18-α-甘草次酸(αGA)可以阻断星形胶质细胞的间隙连接通透性,但对这些钙反应的幅度没有明显影响。 4.如定量和拓扑分析所证实的,在不存在和存在αGA的情况下,Et1的应用均增加了所有星形胶质细胞中[Ca2 +] i的水平。 5.在对照条件下,对甲氧胺或卡巴胆碱有反应的细胞亚群表现出两种主要的钙反应类型,它们的形状和动力学特性不同。在存在αGA的情况下,响应这些受体激动剂的细胞数量显着减少。实际上,在存在αGA的情况下,以潜伏期长,上升时间缓慢和振幅较弱为特征的响应消失了,而保留了潜伏期短和上升时间短的响应。 6.这些结果表明,可渗透的间隙连接通道倾向于减弱星形胶质细胞群的药理和功能异质性,而它们的抑制作用则限制了表达高密度与磷脂酶C结合的递质受体的星形胶质细胞中的钙反应。

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