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啮齿动物运动神经元兴奋性的突触控制:从数月到毫秒

Synaptic control of motoneuron excitability in rodents: from months to milliseconds.

作者信息

Funk G D, Parkis M A, Selvaratnam S R, Robinson D M, Miles G B, Peebles K C

机构信息

Department of Physiology, Faculty of Medicine and Health Science, University of Auckland, New Zealand.

出版信息

Clin Exp Pharmacol Physiol. 2000 Jan-Feb;27(1-2):120-5. doi: 10.1046/j.1440-1681.2000.03202.x.

Abstract
  1. Motoneurons (MN) shape motor patterns by transforming inputs into action potential output. This transformation, excitability, is determined by an interaction between synaptic inputs and intrinsic membrane properties. Excitability is not static, but changes over multiple time scales. The purpose of the present paper is to review our recent data on synaptic factors important in the dynamic control of MN excitability over time scales ranging from weeks to milliseconds. 2. Developmental changes in modulation of MN excitability are well established. Noradrenergic potentiation of hypoglossal (XII) MN inspiratory activity in rhythmically active medullary slice preparations from rodents increases during the first two postnatal weeks. This is due to increasing alpha 1- and beta-adrenoceptor excitatory mechanisms and to a decreasing inhibitory mechanism mediated by alpha 2-adrenoceptors. Over a similar period, ATP potentiation of XII inspiratory activity does not change. 3. Motoneuron excitability may also change on a faster time scale, such as between different behaviours or different phases of a behaviour. Examination of this has been confounded by the fact that excitatory synaptic drives underlying behaviour can obscure smaller concurrent changes in excitability. Using the rhythmically active neonatal rat brain-stem-spinal cord preparation, we blocked excitatory inspiratory drive to phrenic MN (PMN) to reveal a reduction in PMN excitability specific to the inspiratory phase that: (i) arises from an inhibitory GABAergic input; (ii) is not mediated by recurrent pathways; and (iii) is proportional to and synchronous with the excitatory inspiratory input. We propose that the proportionality of the concurrent inhibitory and excitatory drives provides a means for phase-specific modulation of PMN gain. 4. Modulation across such diverse time scales emphasizes the active role that synaptic factors play in controlling MN excitability and shaping behaviour.
摘要
  1. 运动神经元(MN)通过将输入转化为动作电位输出,从而塑造运动模式。这种转化,即可兴奋性,由突触输入与内在膜特性之间的相互作用决定。可兴奋性并非一成不变,而是会在多个时间尺度上发生变化。本文的目的是回顾我们最近关于突触因子的数据,这些因子在从数周至毫秒的时间尺度上对MN兴奋性的动态控制中起着重要作用。2. MN兴奋性调制的发育变化已得到充分证实。在啮齿动物有节律活动的延髓切片标本中,去甲肾上腺素能增强舌下神经(XII)MN的吸气活动,在出生后的前两周内增强。这是由于α1和β肾上腺素能受体兴奋性机制增加,以及由α2肾上腺素能受体介导的抑制机制减弱。在相似的时间段内,XII吸气活动的ATP增强作用没有变化。3. 运动神经元的兴奋性也可能在更快的时间尺度上发生变化,比如在不同行为之间或行为的不同阶段。对此的研究一直受到这样一个事实的困扰,即行为背后的兴奋性突触驱动可能会掩盖兴奋性同时发生的较小变化。利用有节律活动的新生大鼠脑干脊髓标本,我们阻断了膈运动神经元(PMN)的兴奋性吸气驱动,以揭示仅在吸气阶段PMN兴奋性的降低,这种降低:(i)源于抑制性GABA能输入;(ii)不是由反馈通路介导的;(iii)与兴奋性吸气输入成比例且同步。我们提出,同时存在的抑制性和兴奋性驱动的比例性为PMN增益的相位特异性调制提供了一种方式。4. 在如此不同的时间尺度上进行调制,强调了突触因子在控制MN兴奋性和塑造行为中所起的积极作用。

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