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甘氨酸能传递的发育影响:NMDA受体介导的兴奋性突触后电位的调节

Developmental influence of glycinergic transmission: regulation of NMDA receptor-mediated EPSPs.

作者信息

Kotak V C, Sanes D H

机构信息

Center for Neural Science, New York University, New York 10003, USA.

出版信息

J Neurosci. 1996 Mar 1;16(5):1836-43. doi: 10.1523/JNEUROSCI.16-05-01836.1996.

Abstract

The influence of excitatory transmission on postsynaptic structure is well established in developing animals, but little is known about the role of synaptic inhibition. We addressed this issue in developing gerbils with two manipulations designed to decrease glycinergic transmission in an auditory nucleus, the lateral superior olive (LSO), before the onset of sound-evoked activity. First, contralateral cochlear ablation functionally denervated the glycinergic pathway from the medial nucleus of the trapezoid body (MNTB) to the LSO, while leaving the excitatory pathway intact. Second, continuous release of a glycine receptor antagonist, strychnine (SN), was used to decrease transmission. The strength of excitatory and inhibitory synapses was examined with whole-cell recordings from LSO neurons in a brain-slice preparation. The percentage of LSO neurons exhibiting MNTB-evoked IPSPs was reduced in both ablated and SN-treated animals. In those neurons displaying IPSPs, the amplitude was significantly reduced. This decrease was accompanied by an 8 mV depolarization in the IPSP equilibrium potential. In contrast, the ipsilaterally evoked EPSPs were of unusually long duration in experimental animals. These long-duration EPSPs were significantly shortened by hyperpolarizing the neuron to -90 mV or exposing them to aminophosphonopentanoic acid (AP-5), an NMDA receptor antagonist. Membrane hyperpolarization and AP-5 had little effect in control neurons. In addition, LSO neurons from ablated or SN-treated animals displayed broad rebound depolarizations after membrane hyperpolarization, and these were abolished in the presence of Ni2+. Because both cochlear ablation and SN-rearing were initiated before the onset of sound-evoked activity, the results suggest that spontaneous glycinergic transmission influences the development of postsynaptic properties, including the IPSP reversal potential, NMDA receptor function, and a Ca2+ conductance.

摘要

在发育中的动物中,兴奋性传递对突触后结构的影响已得到充分证实,但关于突触抑制的作用却知之甚少。我们通过两种操作来研究发育中的沙鼠体内的这一问题,这两种操作旨在在声音诱发活动开始之前降低听觉核团外侧上橄榄核(LSO)中的甘氨酸能传递。首先,对侧耳蜗切除术在功能上去除了从梯形体内侧核(MNTB)到LSO的甘氨酸能通路,同时使兴奋性通路保持完整。其次,持续释放甘氨酸受体拮抗剂士的宁(SN)来减少传递。在脑片制备中,通过对LSO神经元进行全细胞记录来检测兴奋性和抑制性突触的强度。在接受耳蜗切除和SN处理的动物中,表现出MNTB诱发的抑制性突触后电位(IPSP)的LSO神经元百分比均降低。在那些显示出IPSP的神经元中,其幅度显著降低。这种降低伴随着IPSP平衡电位8 mV的去极化。相比之下,在实验动物中,同侧诱发的兴奋性突触后电位(EPSP)持续时间异常长。通过将神经元超极化至-90 mV或使其暴露于NMDA受体拮抗剂氨基膦酰戊酸(AP-5),这些长时间的EPSP会显著缩短。膜超极化和AP-5对对照神经元几乎没有影响。此外,来自接受耳蜗切除或SN处理动物的LSO神经元在膜超极化后表现出广泛的反弹去极化,而在存在Ni2+的情况下这些去极化被消除。由于耳蜗切除和SN饲养均在声音诱发活动开始之前启动,结果表明自发的甘氨酸能传递会影响突触后特性的发育,包括IPSP反转电位、NMDA受体功能和Ca2+电导。

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