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初级传入神经在七鳃鳗中引发由兴奋性氨基酸受体介导的兴奋性突触后电位(EPSP),这些电位受到突触前GABAB受体的调节。

Primary afferents evoke excitatory amino acid receptor-mediated EPSPs that are modulated by presynaptic GABAB receptors in lamprey.

作者信息

Christenson J, Grillner S

机构信息

Nobel Institute for Neurophysiology, Karolinska Institute, Stockholm, Sweden.

出版信息

J Neurophysiol. 1991 Dec;66(6):2141-9. doi: 10.1152/jn.1991.66.6.2141.

Abstract
  1. The primary afferent neurons (dorsal cells) are of two types in lamprey, which are fast (touch) and slowly adapting (pressure), respectively. Intracellular stimulation of such sensory neurons evokes mono- and polysynaptic excitatory postsynaptic potentials (EPSPs) in spinobulbar neurons (giant interneurons) and in unidentified interneurons. Paired intracellular recordings between identified sensory cells and spinobulbar neurons made it possible to study the synaptic transmission in detail. It is shown that both touch and pressure primary afferents utilize excitatory amino acid (EAA) transmission and, furthermore, that these effects are subject to a presynaptic GABAB receptor modulation. 2. The monosynaptic mixed electrical and chemical EPSPs in giant interneurons had a mean peak amplitude of 3.2 +/- 1.3 (SD) mV, a time to peak of 4.7 +/- 1.2 ms, and a duration at one-half peak amplitude of 9.4 +/- 3.2 ms. Corresponding results were obtained with dorsal root or dorsal column stimulation. Seventy percent of the fast-adapting dorsal cells of the "touch" type evoked monosynaptic mixed EPSPs in giant interneurons, whereas only 3% of the slowly adapting "pressure" dorsal cells did. 3. The chemical part of the monosynaptic EPSPs evoked in giant interneurons was, in all cases tested, blocked by application of EAA antagonists, like the nonselective antagonist kynurenic acid (KYAC; 2 mM). The selective kainate/alpha-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid (AMPA) receptor antagonist 6-cyano-7-nitroquinoxaline-2,3-dione (CNQX; 5 microM) had a similar effect, whereas the selective N-methyl-D-aspartate (NMDA) receptor antagonist 2-aminophosphono-5-valeric acid (AP-5; 200-400 microM) did not change the EPSP, even in the absence of magnesium ions. 4. The monosynaptic excitatory synaptic transmission was modulated by application of the selective GABAB receptor agonist L-baclofen (5-10 mM local droplet application or 100-1,000 microM bath applied) or by gamma-aminobutyric acid (GABA; 100-1,000 microM), also when GABAA receptor-evoked effects were blocked by bicuculline (10 microM). L-baclofen or GABA in combination with bicuculline did not evoke any effects in the postsynaptic neuron on membrane potential, input resistance, or spike threshold. Therefore the effects of the GABAB receptor activation most likely occurs at the presynaptic afferent level. 5. In conclusion, the monosynaptic excitation from skin mechanoreceptors evoked in spinobulbar neurons is mediated by EAA receptors of the kainate/AMPA type. GABAB receptor activation causes a depression of this EPSP, most likely because of a presynaptic action. GABA interneurons are known to form close appositions on sensory axons in the lamprey.
摘要
  1. 七鳃鳗的初级传入神经元(背侧细胞)有两种类型,分别是快速适应型(触觉)和缓慢适应型(压力觉)。对这类感觉神经元进行细胞内刺激,可在脊髓 - 延髓神经元(巨中间神经元)和未明确的中间神经元中诱发单突触和多突触兴奋性突触后电位(EPSP)。在已识别的感觉细胞和脊髓 - 延髓神经元之间进行成对细胞内记录,使得详细研究突触传递成为可能。结果表明,触觉和压力觉的初级传入神经元均利用兴奋性氨基酸(EAA)传递,此外,这些效应还受到突触前GABAB受体的调制。2. 巨中间神经元中的单突触混合电和化学EPSP的平均峰值幅度为3.2±1.3(标准差)mV,峰值时间为4.7±1.2 ms,半峰幅度持续时间为9.4±3.2 ms。通过刺激背根或背柱也获得了相应结果。“触觉”型的快速适应背侧细胞中有70%在巨中间神经元中诱发单突触混合EPSP,而“压力觉”型的缓慢适应背侧细胞中只有3%能诱发。3. 在所有测试的情况下,应用EAA拮抗剂,如非选择性拮抗剂犬尿氨酸(KYAC;2 mM),可阻断巨中间神经元中诱发的单突触EPSP的化学部分。选择性海人藻酸/α - 氨基 - 3 - 羟基 - 5 - 甲基 - 4 - 异恶唑丙酸(AMPA)受体拮抗剂6 - 氰基 - 7 - 硝基喹喔啉 - 2,3 - 二酮(CNQX;5 μM)有类似作用,而选择性N - 甲基 - D - 天冬氨酸(NMDA)受体拮抗剂2 - 氨基膦酰基 - 5 - 戊酸(AP - 5;200 - 400 μM)即使在没有镁离子的情况下也不会改变EPSP。4. 应用选择性GABAB受体激动剂L -巴氯芬(5 - 10 mM局部滴加或100 - 1000 μM浴槽应用)或γ -氨基丁酸(GABA;100 - 1000 μM)可调制单突触兴奋性突触传递,即使在GABAA受体诱发的效应被荷包牡丹碱(10 μM)阻断时也是如此。L -巴氯芬或GABA与荷包牡丹碱联合使用对突触后神经元的膜电位、输入电阻或动作电位阈值没有任何影响。因此,GABAB受体激活的效应很可能发生在突触前传入水平。5. 总之,脊髓 - 延髓神经元中由皮肤机械感受器诱发的单突触兴奋是由海人藻酸/AMPA型EAA受体介导的。GABAB受体激活导致该EPSP降低,很可能是由于突触前作用。已知GABA中间神经元在七鳃鳗的感觉轴突上形成紧密连接。

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