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浦肯野细胞兴奋性突触后电位的配对特异性长期抑制源于兔小脑切片中的经典条件反射程序。

Pairing-specific long-term depression of Purkinje cell excitatory postsynaptic potentials results from a classical conditioning procedure in the rabbit cerebellar slice.

作者信息

Schreurs B G, Oh M M, Alkon D L

机构信息

Laboratory of Adaptive Systems, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, Maryland 20892, USA.

出版信息

J Neurophysiol. 1996 Mar;75(3):1051-60. doi: 10.1152/jn.1996.75.3.1051.

Abstract
  1. Using a rabbit cerebellar slice preparation, we stimulated a classical conditioning procedure by stimulating parallel fiber inputs to Purkinje cells with the use of a brief, high-frequency train of eight constant-current pulses 80 ms before climbing fiber inputs to the same Purkinje cell were stimulated with the use of a brief, lower frequency train of three constant-current pulses. In all experiments, we assessed the effects of stimulation by measuring the peak amplitude of Purkinje cell excitatory postsynaptic potentials (EPSPs) to single parallel fiber test pulses. 2. Intradendritically recorded Purkinje cell EPSPs underwent a long-term (> 20 min) reduction in peak amplitude (30%) after paired stimulation of the parallel and climbing fibers but not after unpaired or parallel fiber alone stimulation. We call this phenomenon pairing-specific long-term depression (PSD). 3. Facilitation of the peak amplitude of a second EPSP elicited by a parallel fiber train occurred both before and after paired stimulation suggesting that the locus of depression was not presynaptic. Depression of the peak amplitude of a depolarizing response to focal application of glutamate following pairings of parallel and climbing fiber stimulation added support to a suggested postsynaptic locus of the PSD effect. 4. The application of aniracetam potentiated EPSP peak amplitude by 40%, but these values returned to baseline as a result of pairings. With the removal of aniracetam from the bath 20 min after pairings, normal levels of pairing-specific EPSP depression were observed, indicating that the effect did not result from direct desensitization of alpha-amino-3-hydroxy-5-methyl-4-isoxazole-proprionic acid (AMPA) receptors. 5. Incubation of slices in the protein kinase inhibitor H-7 potentiated EPSP peak amplitudes slightly (9%), but peak amplitudes returned to baseline levels after pairings. The net reduction in EPSP peak amplitude of < 10% after pairings suggested that H-7 partially blocked PSD and that, in turn, PSD involved protein kinases. 6. The means of induction and the specificity of those means suggest that the phenomenology of PSD is fundamentally different from that of long-term depression. PSD only occurs with pairings of trains of parallel fiber and climbing fiber stimulation; it occurs without the need for bicuculline; and it can overcome the blocking effects of aniracetam. 7. Nevertheless, the involvement of protein kinases and the potential role of calcium suggest that the mechanisms involved in the induction of PSD and long-term depression have a number of features in common. 8. Because of the pairing-specific nature of the long-term synaptic depression observed in these experiments, PSD provides a mechanism that may contribute to the role of the cerebellar cortex in classical conditioning.
摘要
  1. 我们采用兔小脑薄片标本,在对同一浦肯野细胞的攀缘纤维输入施加一串三个恒流脉冲的短串、低频刺激之前80毫秒,对其平行纤维输入施加一串八个恒流脉冲的短串、高频刺激,以此激发经典条件反射程序。在所有实验中,我们通过测量浦肯野细胞对单个平行纤维测试脉冲的兴奋性突触后电位(EPSP)的峰值幅度来评估刺激的效果。2. 对平行纤维和攀缘纤维进行配对刺激后,胞内记录的浦肯野细胞EPSP的峰值幅度出现长期(>20分钟)降低(30%),而在未配对刺激或仅平行纤维刺激后则未出现这种情况。我们将这种现象称为配对特异性长时程抑制(PSD)。3. 平行纤维串引发的第二个EPSP的峰值幅度在配对刺激前后均出现增强,这表明抑制位点不在突触前。平行纤维和攀缘纤维刺激配对后,对局部应用谷氨酸的去极化反应的峰值幅度降低,这为PSD效应的突触后位点提供了支持。4. 阿尼西坦的应用使EPSP峰值幅度增强了40%,但这些值在配对后恢复到基线水平。配对20分钟后从浴槽中去除阿尼西坦,观察到配对特异性EPSP抑制的正常水平,这表明该效应不是由α-氨基-3-羟基-5-甲基-4-异恶唑丙酸(AMPA)受体的直接脱敏引起的。5. 将薄片在蛋白激酶抑制剂H-7中孵育,EPSP峰值幅度略有增强(9%),但配对后峰值幅度恢复到基线水平。配对后EPSP峰值幅度净降低<10%,这表明H-7部分阻断了PSD,进而表明PSD涉及蛋白激酶。6. 诱导方式及其特异性表明,PSD的现象学与长时程抑制有根本不同。PSD仅在平行纤维串和攀缘纤维刺激配对时出现;无需荷包牡丹碱即可出现;并且它可以克服阿尼西坦的阻断作用。7. 然而,蛋白激酶的参与和钙可能发挥的作用表明,PSD和长时程抑制的诱导机制有许多共同特征。8. 由于在这些实验中观察到的长时程突触抑制具有配对特异性,PSD提供了一种可能有助于小脑皮质在经典条件反射中发挥作用的机制。

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