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Catecholaminergic consolidation of motor cortical neuroplasticity in humans.

机译:人体运动皮质神经可塑性的儿茶酚胺能巩固。

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Amphetamine, a catecholaminergic re-uptake-blocker, is able to improve neuroplastic mechanisms in humans. However, so far not much is known about the underlying physiological mechanisms. Here, we study the impact of amphetamine on NMDA receptor-dependent long-lasting excitability modifications in the human motor cortex elicited by weak transcranial direct current stimulation (tDCS). Amphetamine significantly enhanced and prolonged increases in anodal, tDCS-induced, long-lasting excitability. Under amphetamine premedication, anodal tDCS resulted in an enhancement of excitability which lasted until the morning after tDCS, compared to approximately 1 h in the placebo condition. Prolongation of the excitability enhancement was most pronounced for long-term effects; the duration of short-term excitability enhancement was only slightly increased. Since the additional application of the NMDA receptor antagonist dextromethorphane blocked any enhancement of tDCS-driven excitability under amphetamine, we conclude that amphetamine consolidates the tDCS-induced neuroplastic effects, but does not initiate them. The fact that propanolol, a beta-adrenergic antagonist, diminished the duration of the tDCS-generated after-effects suggests that adrenergic receptors play a certain role in the consolidation of NMDA receptor-dependent motor cortical excitability modifications in humans. This result may enable researchers to optimize neuroplastic processes in the human brain on the rational basis of purpose-designed pharmacological interventions.
机译:苯丙胺是一种儿茶酚胺能再摄取阻滞剂,能够改善人类的神经形成机制。然而,到目前为止,关于潜在的生理机制知之甚少。在这里,我们研究了苯丙胺对弱经颅直流电刺激(tDCS)引起的人运动皮层中NMDA受体依赖性持久兴奋性修饰的影响。苯丙胺可显着增强并延长tDCS诱导的持久兴奋性对阳极的影响。在安非他明的用药前,阳极tDCS导致兴奋性增强,这种兴奋性一直持续到tDCS后的早晨,而在安慰剂条件下大约为1 h。兴奋性增强的延长对长期影响最为明显。短期兴奋性增强的持续时间仅略有增加。由于NMDA受体拮抗剂右美沙芬的额外应用可阻止安非他明在tDCS驱动的兴奋性方面的任何增强,因此我们得出结论,苯丙胺巩固了tDCS诱导的神经塑性作用,但并未引发它们。丙醇(一种β-肾上腺素拮抗剂)减少了tDCS产生的后遗症的持续时间这一事实表明,肾上腺素能受体在巩固人类NMDA受体依赖性运动皮层兴奋性修饰中起一定作用。该结果可能使研究人员能够在针对目的设计的药理学干预措施的合理基础上优化人脑中的神经形成过程。

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