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触发大鼠内侧视前神经元GABA释放的异质性突触前钙通道类型

Heterogeneous presynaptic Ca2+ channel types triggering GABA release onto medial preoptic neurons from rat.

作者信息

Haage D, Karlsson U, Johansson S

机构信息

Department of Physiology, Umea University, S-901 87 Umea, Sweden.

出版信息

J Physiol. 1998 Feb 15;507 ( Pt 1)(Pt 1):77-91. doi: 10.1111/j.1469-7793.1998.077bu.x.

Abstract
  1. Voltage-dependent Ca2+ channels triggering GABA release onto neurons from the medial preoptic nucleus of rat were investigated. Acutely dissociated neurons with adherent functional synaptic terminals were investigated by tight-seal whole-cell recordings from the postsynaptic cells. 2. Spontaneous current events similar to miniature postsynaptic currents were recorded. They were blocked by bicuculline (100 microM), showed a roughly unimodal amplitude distribution and a reversal potential consistent with a Cl- current, and were therefore attributed to GABAA receptors activated by synaptically released GABA. 3. Application of 140 mM KCl, expected to depolarize presynaptic terminals, evoked currents that were ascribed to a more massive release of GABA. The KCl-induced synaptic currents were abolished in Ca2+-free solutions and showed a roughly hyperbolic relation to external Ca2+ concentration with half-saturation at 0.15 mM. They further depended on the concentration of applied KCl in a way expected for high-threshold Ca2+ channels. 4. The KCl-evoked synaptic currents were completely blocked by 200 microM Cd2+, but only partially blocked by 200 microM Ni2+. The KCl-evoked synaptic currents were insensitive to the L-type Ca2+ channel blocker nifedipine (10 microM). However, the synaptic currents were sensitive to either 1 microM omega-conotoxin GVIA, 25 nM omega-agatoxin IVA or 1 microM omega-conotoxin MVIIC. 6. It was concluded that, in many presynaptic terminals, the Ca2+ influx triggering GABA release onto medial preoptic neurons is mainly mediated by one predominant type of high- threshold Ca2+ channel that may be either of N-, P- or Q-type. 7. It was further concluded that terminals with similar predominant channel types often were clustered on the same postsynaptic cell.
摘要
  1. 研究了触发大鼠内侧视前核神经元释放γ-氨基丁酸(GABA)的电压依赖性Ca2+通道。通过对突触后细胞进行紧密封全细胞记录,研究了带有附着功能性突触终末的急性分离神经元。2. 记录到了类似于微小突触后电流的自发电流事件。它们被荷包牡丹碱(100微摩尔)阻断,呈现出大致单峰的幅度分布以及与Cl-电流一致的反转电位,因此被归因于由突触释放的GABA激活的GABAA受体。3. 应用140毫摩尔氯化钾,预期会使突触前终末去极化,引发的电流被归因于更大量的GABA释放。氯化钾诱导的突触电流在无钙溶液中被消除,并且与细胞外钙浓度呈现大致的双曲线关系,半饱和浓度为0.15毫摩尔。它们还以高阈值Ca2+通道预期的方式依赖于所施加氯化钾的浓度。4. 氯化钾诱发的突触电流被200微摩尔镉离子完全阻断,但仅被200微摩尔镍离子部分阻断。氯化钾诱发的突触电流对L型Ca2+通道阻滞剂硝苯地平(10微摩尔)不敏感。然而,突触电流对1微摩尔ω-芋螺毒素GVIA、25纳摩尔ω-蛛毒素IVA或1微摩尔ω-芋螺毒素MVIIC敏感。6. 得出的结论是,在许多突触前终末,触发向内侧视前神经元释放GABA的Ca2+内流主要由一种主要类型的高阈值Ca2+通道介导,该通道可能是N型、P型或Q型。7. 进一步得出的结论是,具有相似主要通道类型的终末通常聚集在同一个突触后细胞上。

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