J. Classen: University of Leipzig, Department of Neurology, Liebigstr. 20, Leipzig 04103, Germany.
J Physiol. 2013 Oct 1;591(19):4903-20. doi: 10.1113/jphysiol.2013.253989. Epub 2013 Jul 15.
Synaptic weight changes induced by temporal correlations between the spikes of pre- and postsynaptic neurons are referred to as spike-timing-dependent plasticity (STDP). Transcranial magnetic stimulation (TMS) induces long-lasting effects on corticospinal excitability, if it is repetitively paired with stimulation of afferents from a corresponding contralateral hand region at short intervals (paired associative stimulation, PAS). PAS-induced plasticity has been linked with synaptic STDP. We aimed to investigate which elements of the cortical microcircuitry sustain and govern PAS-induced depression of corticospinal excitability in the target muscle representation (and enhancement of excitability in its functional surround). We show that the time window during which the interaction between both stimulus-induced cortical events leads to immediate post-interventional depression is short (<4.5 ms). The depressant PAS effects at the target representation were completely blocked by applying a subthreshold magnetic pulse 3 ms before the principal TMS pulse, even when the strength of the latter was adjusted to generate a motor-evoked potential of similar amplitude to that with the unconditioned magnetic pulse. Epidural recordings from the cervical cord of a patient showed that under this condition late TMS-evoked I-waves remain suppressed. When the intensity of the TMS component during PAS was lowered - sufficient to allow activation of inhibitory neurons, but insufficient to activate corticospinal neurons - excitability of short-latency intracortical inhibition remained unchanged. PAS-induced facilitation in the functional surround followed the same pattern as the centre-depressant effects. These findings may suggest that excitability-depressant PAS-induced effects are due to weakening of excitatory synapses between upper cortical layer principal neurons, but not those located on the corticospinal neuron, or inhibitory synapses. Inhibitory interneurons involved in short-latency intracortical inhibition are gate-keepers to producing centre-depressant/surround-facilitatory PAS effects. Based on these and earlier findings we propose a model specifying the composition and laminar location of the involved microcircuit of PAS-induced plasticity that may enhance its utility as a model of STDP in humans.
突触权重变化由突触前神经元和突触后神经元的尖峰之间的时间相关性引起,被称为尖峰时间依赖性可塑性(STDP)。如果经颅磁刺激(TMS)以短时间间隔重复与来自相应对侧手部区域的传入刺激配对(联合关联刺激,PAS),则会对皮质脊髓兴奋性产生持久的影响。PAS 诱导的可塑性与突触 STDP 有关。我们旨在研究皮质微电路的哪些元素维持和控制 PAS 诱导的皮质脊髓兴奋性在靶肌肉代表中的抑制(以及兴奋性在其功能周围的增强)。我们表明,两个刺激诱导的皮质事件之间相互作用导致即时干预后抑制的时间窗口很短(<4.5ms)。在主 TMS 脉冲前 3ms 施加亚阈值磁脉冲可完全阻断靶代表处的抑制性 PAS 效应,即使后者的强度调整为产生与未调节磁脉冲相似幅度的运动诱发电位也是如此。对一名患者颈脊髓的硬膜外记录显示,在这种情况下,延迟的 TMS 诱发的 I 波仍然受到抑制。当 PAS 期间 TMS 成分的强度降低时 - 足以激活抑制神经元,但不足以激活皮质脊髓神经元 - 短潜伏期内皮质抑制的兴奋性保持不变。功能周围的 PAS 诱导的易化遵循与中心抑制效应相同的模式。这些发现可能表明,兴奋性抑制性 PAS 诱导的效应是由于上皮质层主神经元之间的兴奋性突触减弱所致,但不是位于皮质脊髓神经元上的兴奋性突触或抑制性突触减弱所致。参与短潜伏期内皮质抑制的抑制性中间神经元是产生中心抑制/周围促进 PAS 效应的守门员。基于这些和早期的发现,我们提出了一个模型,指定了 PAS 诱导的可塑性涉及的微电路的组成和分层位置,这可能增强其作为人类 STDP 模型的实用性。
