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高频外周成分的脊髓靶向配对关联刺激可在健康受试者中诱导脊髓水平的可塑性。

Spinally targeted paired associated stimulation with high-frequency peripheral component induces spinal level plasticity in healthy subjects.

作者信息

Nätkynmäki Anna, Lauronen Leena, Haakana Piia, Kirveskari Erika, Avela Janne, Shulga Anastasia

机构信息

BioMag Laboratory, HUS Diagnostic Center, Helsinki University Hospital, University of Helsinki and Aalto University School of Science, Helsinki, Finland.

Faculty of Sport and Health Sciences, University of Jyväskylä, Jyväskylä, Finland.

出版信息

Sci Rep. 2024 Dec 28;14(1):31052. doi: 10.1038/s41598-024-82271-4.

Abstract

A novel variant of paired-associative stimulation (PAS) consisting of high-frequency peripheral nerve stimulation (PNS) and high-intensity transcranial magnetic stimulation (TMS) above the motor cortex, called high-PAS, can lead to improved motor function in patients with incomplete spinal cord injury. In PAS, the interstimulus interval (ISI) between the PNS and TMS pulses plays a significant role in the location of the intended effect of the induced plastic changes. While conventional PAS protocols (single TMS pulse often applied with intensity close to resting motor threshold, and single PNS pulse) usually require precisely defined ISIs, high-PAS can induce plasticity at a wide range of ISIs and also in spite of small ISI errors, which is helpful in clinical settings where precise ISI determination can be challenging. However, this also makes the determination of high-PAS level of plasticity induction more challenging and calls for more research on the mechanism of action of high-PAS. We sought to determine if the TMS-induced orthodromic activation in upper motor neurons and PNS-induced antidromic activation in lower motor neurons arriving simultaneously to the intervening synapses at the spinal cord level can be shown to induce acute changes at the targeted location, unlike an otherwise identical but cortically targeted equivalent. Ten healthy subjects participated in two separate sessions, where high-PAS induced activation was set to target spinal (SPINAL) or cortical (CORTICAL) levels with ISI manipulation between otherwise identically applied TMS and PNS pulses. The outcomes were assessed with motor-evoked potentials (MEPs) and Hoffmann (H)-reflex before (PRE), immediately after, and 30 and 60 min after (POST, POST30, POST60) the intervention. MEPs were significantly enhanced in both interventions. In the SPINAL but not in the CORTICAL session, maximal H-reflex amplitudes significantly increased at two timepoints, indicating an increase in spinal excitability. The H/M ratio (maximal H-reflex normalized to maximal M-wave) also showed a significant increase from PRE to POST30 timepoint in the SPINAL session when compared with the CORTICAL equivalent. These results confirm that spinally targeted high-PAS with individualized ISIs indeed has an effect at the spinal level in the sensorimotor system. High-PAS is a novel PAS variant that has shown promising results in motor rehabilitation of individuals with SCI and these new findings contribute to the understanding of its mechanism of action. This provides further evidence for high-PAS as an option for clinical settings to target plasticity at different levels of the corticospinal tract.

摘要

一种新型的配对联想刺激(PAS)变体,由高频外周神经刺激(PNS)和运动皮层上方的高强度经颅磁刺激(TMS)组成,称为高PAS,可改善不完全性脊髓损伤患者的运动功能。在PAS中,PNS和TMS脉冲之间的刺激间隔(ISI)在诱导可塑性变化的预期效果位置中起着重要作用。虽然传统的PAS方案(通常施加强度接近静息运动阈值的单个TMS脉冲和单个PNS脉冲)通常需要精确定义的ISI,但高PAS可以在很宽的ISI范围内诱导可塑性,并且即使存在小的ISI误差也能诱导可塑性,这在精确的ISI测定具有挑战性的临床环境中很有帮助。然而,这也使得确定高PAS诱导可塑性的水平更具挑战性,需要对高PAS的作用机制进行更多研究。我们试图确定,与另一种相同但针对皮层的等效刺激不同,TMS在上运动神经元中诱导的顺行激活和PNS在下运动神经元中诱导的逆行激活同时到达脊髓水平的中间突触时,是否能在目标位置诱导急性变化。十名健康受试者参加了两个单独的实验环节,其中高PAS诱导激活被设定为针对脊髓(SPINAL)或皮层(CORTICAL)水平,并在其他方面相同的TMS和PNS脉冲之间进行ISI操作。在干预前(PRE)、干预后即刻、干预后30分钟和60分钟(POST、POST30、POST60),通过运动诱发电位(MEP)和霍夫曼(H)反射评估结果。两种干预中MEP均显著增强。在脊髓刺激但非皮层刺激的实验环节中,最大H反射幅度在两个时间点显著增加,表明脊髓兴奋性增加。与皮层刺激等效情况相比,脊髓刺激实验环节中从PRE到POST30时间点,H/M比值(最大H反射相对于最大M波进行归一化)也显著增加。这些结果证实,具有个体化ISI的脊髓靶向高PAS确实在感觉运动系统的脊髓水平上有作用。高PAS是一种新型的PAS变体,已在脊髓损伤个体的运动康复中显示出有前景的结果,这些新发现有助于理解其作用机制。这为高PAS作为临床环境中针对皮质脊髓束不同水平可塑性的一种选择提供了进一步的证据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c5cc/11680591/821ed5d1315c/41598_2024_82271_Fig1_HTML.jpg

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