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Interaction between Purkinje Cells and Inhibitory Interneurons May Create Adjustable Output Waveforms to Generate Timed Cerebellar Output

机译:浦肯野细胞与抑制性中间神经元之间的相互作用可能会产生可调节的输出波形,以产生定时的小脑输出

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摘要

We develop a new model that explains how the cerebellum may generate the timing in classical delay eyeblink conditioning. Recent studies show that both Purkinje cells (PCs) and inhibitory interneurons (INs) have parallel signal processing streams with two time scales: an AMPA receptor-mediated fast process and a metabotropic glutamate receptor (mGluR)-mediated slow process. Moreover, one consistent finding is an increased excitability of PC dendrites (in Larsell's lobule HVI) in animals when they acquire the classical delay eyeblink conditioning naturally, in contrast to in vitro studies, where learning involves long-term depression (LTD). Our model proposes that the delayed response comes from the slow dynamics of mGluR-mediated IP3 activation, and the ensuing calcium concentration change, and not from LTP/LTD. The conditioned stimulus (tone), arriving on the parallel fibers, triggers this slow activation in INs and PC spines. These excitatory (from PC spines) and inhibitory (from INs) signals then interact at the PC dendrites to generate variable waveforms of PC activation. When the unconditioned stimulus (puff), arriving on the climbing fibers, is coupled frequently with this slow activation the waveform is amplified (due to an increased excitability) and leads to a timed pause in the PC population. The disinhibition of deep cerebellar nuclei by this timed pause causes the delayed conditioned response. This suggested PC-IN interaction emphasizes a richer role of the INs in learning and also conforms to the recent evidence that mGluR in the cerebellar cortex may participate in slow motor execution. We show that the suggested mechanism can endow the cerebellar cortex with the versatility to learn almost any temporal pattern, in addition to those that arise in classical conditioning.
机译:我们开发了一个新模型,该模型解释了小脑如何在经典延迟眨眼条件下产生时间。最近的研究表明,浦肯野细胞(PC)和抑制性中间神经元(IN)具有并行的信号处理流,具有两个时间尺度:AMPA受体介导的快速过程和代谢型谷氨酸受体(mGluR)介导的缓慢过程。此外,一个一致的发现是,当动物自然获得经典的延迟眨眼条件时,它们在动物中的PC树突(在Larsell小叶HVI中)的兴奋性增加,这与体外研究(学习涉及长期抑郁症(LTD))相反。我们的模型提出延迟响应来自mGluR介导的IP3激活的缓慢动力学以及随之而来的钙浓度变化,而不是LTP / LTD。到达平行纤维的条件刺激(音调)触发IN和PC脊柱的这种缓慢激活。然后,这些兴奋性信号(来自PC棘)和抑制信号(来自INs)在PC树突处相互作用,以生成PC激活的可变波形。当到达攀爬纤维的无条件刺激(吹气)经常与这种缓慢的激活相结合时,波形会被放大(由于增加的兴奋性),并导致PC群体中的定时停顿。定时停顿对小脑深核的抑制作用导致条件性反应延迟。这表明PC-IN相互作用强调了IN在学习中的作用,并且也符合小脑皮层中的mGluR可能参与慢运动执行的最新证据。我们表明,建议的机制可以赋予小脑皮层多种功能,以学习除经典条件下出现的那些时间模式以外的几乎任何时间模式。

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    Hong, Simon; Optican, Lance M.;

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  • 年度 2008
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  • 原文格式 PDF
  • 正文语种 {"code":"en","name":"English","id":9}
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