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谷氨酸介导海马切片培养物中的缓慢突触反应。

Glutamate mediates a slow synaptic response in hippocampal slice cultures.

作者信息

Charpak S, Gähwiler B H

机构信息

Brain Research Institute, University of Zürich, Switzerland.

出版信息

Proc Biol Sci. 1991 Mar 22;243(1308):221-6. doi: 10.1098/rspb.1991.0035.

DOI:10.1098/rspb.1991.0035
PMID:1675800
Abstract

Glutamate (GLU) mediates its 'fast' excitatory transmitter action in the brain by directly gating cation-selective ion channels ('ionotropic' receptors). However, GLU can also activate another type of receptor, coupled to phospholipase C ('metabotropic' receptor). In hippocampal cells, stimulation of this metabotropic receptor by GLU, or by a racemic mixture of (1S-3R and 1R-3S) 1-aminocyclopentyl-1,3-dicarboxylate (ACPD), induces a slower excitation mediated by inhibition of K+ currents. We have assessed whether this slow form of metabotropic receptor excitation can contribute to the effects of synaptically released GLU in hippocampal slice cultures, by recording the responses of CA3 pyramidal cells to afferent mossy fibre stimulation. When the fast ionotropic response was blocked pharmacologically, mossy fibre stimulation produced a slow depolarizing postsynaptic potential associated with a decrease in membrane conductance, a depression of the slow after-hyperpolarization following a train of action potentials, and reduced accommodation during the action potential train. Under voltage-clamp, mossy fibre stimulation produced a slow voltage-dependent inward current which resembled that produced by application of exogenous ACPD or quisqualate (QUIS), and which was occluded by these metabotropic agonists. We therefore suggest that synaptically released GLU can induce two types of postsynaptic responses: a fast excitation through activation of ionotropic receptors and a slower excitation associated with inhibition of K+ conductances through activation of metabotropic receptors. This is analogous to the dual action of acetylcholine on ionotropic (nicotinic) and metabotropic (muscarinic) receptors.

摘要

谷氨酸(GLU)通过直接开启阳离子选择性离子通道(“离子otropic”受体)在大脑中介导其“快速”兴奋性递质作用。然而,GLU还可激活另一种与磷脂酶C偶联的受体(“代谢otropic”受体)。在海马细胞中,GLU或(1S - 3R和1R - 3S)1 - 氨基环戊基 - 1,3 - 二羧酸(ACPD)的外消旋混合物对这种代谢otropic受体的刺激会诱导一种由抑制钾离子电流介导的较慢的兴奋。我们通过记录CA3锥体细胞对传入苔藓纤维刺激的反应,评估了这种代谢otropic受体兴奋的慢形式是否有助于海马切片培养物中突触释放的GLU的作用。当通过药理学方法阻断快速离子otropic反应时,苔藓纤维刺激产生了一个缓慢的去极化突触后电位,伴有膜电导降低、一串动作电位后的慢后超极化抑制以及动作电位串期间的适应性降低。在电压钳制下苔藓纤维刺激产生了一个缓慢的电压依赖性内向电流,类似于应用外源性ACPD或喹啉酸(QUIS)所产生的电流,并且被这些代谢otropic激动剂所阻断。因此,我们认为突触释放的GLU可诱导两种类型的突触后反应:通过激活离子otropic受体产生的快速兴奋和通过激活代谢otropic受体抑制钾离子电导相关的较慢兴奋。这类似于乙酰胆碱对离子otropic(烟碱型)和代谢otropic(毒蕈碱型)受体的双重作用。

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Metabotropic excitatory amino acid receptor activation stimulates phospholipase D in hippocampal slices.促代谢型兴奋性氨基酸受体激活可刺激海马切片中的磷脂酶D。
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