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从大鼠视觉皮层V层细胞记录到的兴奋性突触电位的NMDA和非NMDA受体成分。

NMDA- and non-NMDA-receptor components of excitatory synaptic potentials recorded from cells in layer V of rat visual cortex.

作者信息

Jones K A, Baughman R W

机构信息

Department of Neurobiology, Harvard Medical School, Boston, Massachusetts 02115.

出版信息

J Neurosci. 1988 Sep;8(9):3522-34. doi: 10.1523/JNEUROSCI.08-09-03522.1988.

Abstract

The pharmacological properties of excitatory synapses on pyramidal cells in layer V of rat visual cortex were investigated by recording EPSPs intracellularly in tissue slices. The EPSPs were evoked by electrically stimulating cells in layer II/III or axons in white matter. All of the layer V neurons were pyramidal in nature as determined by injections of Lucifer yellow or by electrophysiological criteria. Application of the broadly acting antagonists kynurenic acid and gamma-D-glutamylglycine reversibly antagonized the EPSPs from both presynaptic sources in a dose-dependent manner: 1 and 5 mM kynurenic acid produced 63 and 79% reductions, respectively, of control responses. The specific NMDA antagonist APV (50 microM) caused a small reduction in peak amplitude and a more significant reduction in the duration of the falling phase of EPSPs. When slices were bathed in Mg2+-free medium, the amplitude of the EPSP increased substantially. Under these conditions APV reduced the size of the EPSP to that observed with APV in the presence of 1 mM Mg2+. The voltage sensitivities of the APV-sensitive and APV-insensitive components of the layer II/III-evoked EPSPs were examined. The APV-insensitive component was not voltage dependent and had an extrapolated reversal potential of -10 mV. In contrast, the APV-sensitive component showed an NMDA-like voltage dependency; it was greatest at the most positive potentials tested (-45 mV) and nearly absent at membrane potentials below rest. At potentials near threshold, the APV-sensitive component contributed approximately half of the total response. Although the time to peak and decay were longer for the APV-sensitive component, the latency was the same as that of the APV-insensitive component. These results provide evidence that the layer II/III to V pathway, which comprises a major interlaminar circuit in cortex, is mediated directly through NMDA as well as non-NMDA receptors located on the layer V cells. This finding has implications for the role of this circuit in cortical visual plasticity.

摘要

通过在组织切片中细胞内记录兴奋性突触后电位(EPSP),研究了大鼠视觉皮层第V层锥体细胞上兴奋性突触的药理学特性。EPSP由电刺激第II/III层细胞或白质中的轴突诱发。通过注射路西法黄或根据电生理标准确定,所有第V层神经元本质上都是锥体神经元。应用广泛作用的拮抗剂犬尿烯酸和γ-D-谷氨酰甘氨酸以剂量依赖的方式可逆地拮抗来自两个突触前来源的EPSP:1 mM和5 mM犬尿烯酸分别使对照反应降低63%和79%。特异性N-甲基-D-天冬氨酸(NMDA)拮抗剂氨基吡啶酮(APV,50 μM)使EPSP的峰值幅度略有降低,而下降相的持续时间则有更显著的降低。当切片浸泡在无镁培养基中时,EPSP的幅度大幅增加。在这些条件下,APV将EPSP的大小降低到在1 mM镁存在下用APV观察到的大小。检查了第II/III层诱发的EPSP中对APV敏感和不敏感成分的电压敏感性。对APV不敏感的成分不依赖电压,其外推反转电位为-10 mV。相比之下,对APV敏感的成分表现出类似NMDA的电压依赖性;在测试的最正电位(-45 mV)时最大,在静息以下的膜电位时几乎不存在。在接近阈值的电位下,对APV敏感的成分约占总反应的一半。虽然对APV敏感成分的峰值时间和衰减时间较长,但其潜伏期与对APV不敏感成分相同。这些结果提供了证据,表明第II/III层到第V层的通路(构成皮层中的一个主要层间回路)直接通过位于第V层细胞上的NMDA受体以及非NMDA受体介导。这一发现对该回路在皮层视觉可塑性中的作用具有启示意义。

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