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S(+)-氯胺酮可减弱脊髓α运动神经元处或其远端的肌源性运动诱发电位。

S(+)-ketamine attenuates myogenic motor-evoked potentials at or distal to the spinal alpha-motoneuron.

作者信息

Scheufler Kai-Michael, Thees Christof, Nadstawek Joachim, Zentner Josef

机构信息

Department of NeurosurgeryUniversity of Freiburg, Germany.

出版信息

Anesth Analg. 2003 Jan;96(1):238-44, table of contents. doi: 10.1097/00000539-200301000-00048.

Abstract

UNLABELLED

We investigated the effect of S(+)-ketamine on spinal cord evoked potentials (ESCPs) and myogenic motor-evoked potentials after electrical stimulation of the motor cortex in a rabbit model. This study was designed to characterize the relationship between ESCP characteristics and corresponding changes in compound muscle action potentials (CMAPs) derived from fore and hind limbs. Direct (D) and indirect (I) corticospinal volleys (ESCP) from the upper and lower thoracic spinal cord, recorded by two bipolar epidural electrodes, were assessed during IV administration of 0.02, 0.05, 0.1, and 0.2 mg. kg(-1) x min(-1) of S(+)-ketamine, each before and after neuromuscular blockade (0.4 mg/kg of cisatracurium), in 16 New Zealand White rabbits after single-pulse bipolar electrical stimulation of the motor cortex at 50 (threshold), 60, and 70 V. CMAP amplitudes at fore and hind limbs were significantly suppressed (P < 0.01) during infusion at 0.1 and 0.2 mL x kg(-1) x min(-1), whereas neither corresponding D- nor I-waves were altered. Similar findings were obtained during variation of stimulus amplitude (50-70 V). Multivariate regression analysis of CMAP amplitudes and various ESCP characteristics demonstrated no apparent interparametric association. These findings indicate that S(+)-ketamine modulates CMAP independent from corticospinal D- and I-wave-mediated facilitation at or distal to the spinal alpha-motoneuron.

IMPLICATIONS

S(+)-Ketamine combines several anesthetic properties suitable for total IV neuroanesthesia, including minimal effects on neurophysiological monitoring. Recording of neural and myogenic responses after electrical stimulation of the motor cortex indicates that S(+)-ketamine modulates myogenic motor-evoked potentials by a peripheral mechanism at or distal to the spinal alpha-motoneuron.

摘要

未标记

我们在兔模型中研究了S(+)-氯胺酮对脊髓诱发电位(ESCPs)以及运动皮层电刺激后肌源性运动诱发电位的影响。本研究旨在描述ESCP特征与来自前肢和后肢的复合肌肉动作电位(CMAPs)相应变化之间的关系。在16只新西兰白兔中,通过两个双极硬膜外电极记录来自胸段脊髓上下部的直接(D)和间接(I)皮质脊髓冲动(ESCP),在静脉注射0.02、0.05、0.1和0.2mg·kg⁻¹·min⁻¹的S(+)-氯胺酮期间,每次在神经肌肉阻滞(0.4mg/kg顺式阿曲库铵)前后,以50(阈值)、60和70V对运动皮层进行单脉冲双极电刺激。在前肢和后肢输注0.1和0.2mL·kg⁻¹·min⁻¹期间,CMAP振幅显著受到抑制(P<0.01),而相应的D波和I波均未改变。在刺激幅度变化(50 - 70V)期间也获得了类似的结果。CMAP振幅与各种ESCP特征的多变量回归分析未显示明显的参数间关联。这些发现表明,S(+)-氯胺酮在脊髓α运动神经元或其远端调节CMAP,独立于皮质脊髓D波和I波介导的易化作用。

启示

S(+)-氯胺酮具有几种适合全静脉神经麻醉的麻醉特性,包括对神经生理监测的影响最小。运动皮层电刺激后神经和肌源性反应的记录表明,S(+)-氯胺酮通过脊髓α运动神经元或其远端的外周机制调节肌源性运动诱发电位。

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