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首页> 外文期刊>Cell Calcium: The International Interdisciplinary Forum for Research on Calcium >Local and global calcium signals associated with the opening of neuronal alpha7 nicotinic acetylcholine receptors.
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Local and global calcium signals associated with the opening of neuronal alpha7 nicotinic acetylcholine receptors.

机译:与神经元α7烟碱乙酰胆碱受体开放有关的局部和全局钙信号。

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摘要

Neuronal nicotinic acetylcholine receptors (nAChRs) are Ca(2+)-permeable ligand-gated channels widely expressed in the central and peripheral nervous system. One of the most Ca(2+) selective isoform is the homopentameric alpha7-nAChR implicated in schizophrenia. The activity of alpha7-nAChRs is usually recorded electrophysiologically, which limits the amount of information obtained. Here, we used fluorescence imaging to record Ca(2+) transients associated with activation of the alpha7-nAChR in neuroblastoma cells stably expressing human alpha7-nAChRs. Application of nicotine (50 microM) consistently evoked transient (30s), stereotyped Ca(2+) responses that were inhibited by the selective alpha7-nAChRs antagonists methyllycaconitine (MLA) and alpha-bungarotoxin, and greatly increased and prolonged by the allosteric modulator PNU-120596 (1 microM). Unexpectedly, brief (1-5s), repetitive Ca(2+) transients of sub-micrometric dimension were observed in filopodia of cells expressing alpha7-nAChR. PNU-120596 increased the frequency and slowed the decay kinetics of these miniature Ca(2+) elevations, which were insensitive to ryanodine, preserved during hyperpolarisation, and prevented by MLA, alpha-bungarotoxin, or Ca(2+) removal. Global Ca(2+) responses were also recorded in ganglion cells of embryo chicken retina during co-application of PNU-120596 and nicotine, together with whole-cell currents and brief current bursts. These data demonstrate that Ca(2+) signals generated by alpha7-nAChRs can be recorded optically both in cell lines and in intact tissues. The possibility to image miniature Ca(2+) signals enables to map the location of functional alpha7-nAChR channel clusters within cells and to analyze their single channel properties optically. Deciphering the rich pattern of intracellular Ca(2+) signals generated by the activity of the alpha7-nAChRs will reveal the physiological role of these receptor-channels.
机译:神经元的烟碱型乙酰胆碱受体(nAChRs)是Ca(2+)可渗透配体门控的通道,广泛表达在中央和周围的神经系统。最Ca(2+)选择性同工型之一是精神分裂症涉及的同五聚体alpha7-nAChR。通常以电生理学方式记录alpha7-nAChRs的活性,这限制了获得的信息量。在这里,我们使用荧光成像来记录与稳定表达人类alpha7-nAChRs的神经母细胞瘤细胞中的alpha7-nAChR激活相关的Ca(2+)瞬变。尼古丁(50 microM)的应用持续引起短暂的(30s),刻板的Ca(2+)反应,该反应被选择性的alpha7-nAChRs拮抗剂甲基甘可尼丁(MLA)和α-真菌毒素所抑制,并且通过变构调节剂PNU大大增加和延长了时间-120596(1 microM)。出乎意料的是,在表达α7-nAChR的细胞的丝状伪足中观察到了短暂的(1-5s)次重复的亚微米级Ca(2+)瞬变。 PNU-120596增加了频率并减缓了这些微型Ca(2+)升高的衰减动力学,这些升高对ryanodine不敏感,在超极化过程中得以保留,并通过MLA,α-邦格鲁毒素或Ca(2+)去除得以阻止。全球Ca(2+)响应也记录在PNU-120596和尼古丁的共同应用过程中,胚胎鸡视网膜的神经节细胞,连同全细胞电流和短暂的电流爆发。这些数据表明,由alpha7-nAChRs生成的Ca(2+)信号可以光学记录在细胞系和完整组织中。成像微型Ca(2+)信号的可能性使您能够映射功能性alpha7-nAChR通道簇在细胞内的位置,并光学分析其单通道特性。解密由alpha7-nAChRs的活性产生的胞内Ca(2+)信号的丰富模式将揭示这些受体通道的生理作用。

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