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加巴喷丁对完全性脊髓损伤后肌肉痉挛以及诱发性和自发性自主神经反射异常的影响。

Effects of gabapentin on muscle spasticity and both induced as well as spontaneous autonomic dysreflexia after complete spinal cord injury.

作者信息

Rabchevsky Alexander G, Patel Samir P, Lyttle Travis S, Eldahan Khalid C, O'Dell Christopher R, Zhang Yi, Popovich Phillip G, Kitzman Patrick H, Donohue Kevin D

机构信息

Spinal Cord and Brain Injury Research Center, University of Kentucky Lexington, KY, USA.

出版信息

Front Physiol. 2012 Aug 15;3:329. doi: 10.3389/fphys.2012.00329. eCollection 2012.

Abstract

We recently reported that the neuropathic pain medication, gabapentin (GBP; Neurontin), significantly attenuated both noxious colorectal distension (CRD)-induced autonomic dysreflexia (AD) and tail pinch-induced spasticity compared to saline-treated cohorts 2-3 weeks after complete high thoracic (T4) spinal cord injury (SCI). Here we employed long-term blood pressure telemetry to test, firstly, the efficacy of daily versus acute GBP treatment in modulating AD and tail spasticity in response to noxious stimuli at 2 and 3 weeks post-injury. Secondly, we determined whether daily GBP alters baseline cardiovascular parameters, as well as spontaneous AD events detected using a novel algorithm based on blood pressure telemetry data. At both 14 and 21 days after SCI, irrespective of daily treatment, acute GBP given 1 h prior to stimulus significantly attenuated CRD-induced AD and pinch-evoked tail spasticity; conversely, acute saline had no such effects. Moreover, daily GBP did not alter 24 h mean arterial pressure (MAP) or heart rate (HR) values compared to saline treatment, nor did it reduce the incidence of spontaneous AD events compared to saline over the three week assessment period. Power spectral density (PSD) analysis of the MAP signals demonstrated relative power losses in mid frequency ranges (0.2-0.8 Hz) for all injured animals relative to low frequency MAP power (0.02-0.08 Hz). However, there was no significant difference between groups over time post-injury; hence, GBP had no effect on the persistent loss of MAP fluctuations in the mid frequency range after injury. In summary, the mechanism(s) by which acute GBP treatment mitigate aberrant somatosensory and cardiophysiological responses to noxious stimuli after SCI remain unclear. Nevertheless, with further refinements in defining the dynamics associated with AD events, such as eliminating requisite concomitant bradycardia, the objective repeatability of automatic detection of hypertensive crises provides a potentially useful tool for assessing autonomic function pre- and post-SCI, in conjunction with experimental pharmacotherapeutics for neuropathic pain, such as GBP.

摘要

我们最近报道,与生理盐水处理组相比,在完全性高位胸段(T4)脊髓损伤(SCI)2 - 3周后,神经性疼痛药物加巴喷丁(GBP;Neurontin)能显著减轻有害性结肠扩张(CRD)诱发的自主神经反射异常(AD)以及尾部夹捏诱发的痉挛。在此,我们采用长期血压遥测技术进行测试,首先,在损伤后2周和3周,比较每日给予GBP治疗与急性给予GBP治疗对调节AD和尾部痉挛以应对有害刺激的效果。其次,我们确定每日给予GBP是否会改变基线心血管参数,以及使用基于血压遥测数据的新算法检测到的自发性AD事件。在SCI后的第14天和第21天,无论每日治疗情况如何,在刺激前1小时给予急性GBP能显著减轻CRD诱发的AD和夹捏诱发的尾部痉挛;相反,急性给予生理盐水则无此效果。此外,与生理盐水治疗相比,每日给予GBP并未改变24小时平均动脉压(MAP)或心率(HR)值,在为期三周的评估期内,与生理盐水相比,它也未降低自发性AD事件的发生率。对MAP信号的功率谱密度(PSD)分析表明,相对于低频MAP功率(0.02 - 0.08Hz),所有受伤动物在中频范围(0.2 - 0.8Hz)的相对功率损失。然而,损伤后不同时间组间无显著差异;因此,GBP对损伤后中频范围内MAP波动的持续损失无影响。总之,急性GBP治疗减轻SCI后对有害刺激的异常体感和心脏生理反应的机制仍不清楚。然而,随着在定义与AD事件相关的动态变化方面的进一步完善,例如消除必要伴随的心动过缓,自动检测高血压危象的客观可重复性为评估SCI前后的自主神经功能提供了一个潜在有用的工具,同时可结合用于神经性疼痛的实验性药物治疗,如GBP。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3892/3429097/0bfb24ee9ecd/fphys-03-00329-g0001.jpg

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