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脊髓压迫后疼痛大鼠模型中临床药物的行为特征及作用

Behavioral characterization and effect of clinical drugs in a rat model of pain following spinal cord compression.

作者信息

Hama Aldric, Sagen Jacqueline

机构信息

University of Miami, Miller School of Medicine, The Miami Project to Cure Paralysis, 1095 NW 14th Terrace (R-48), Miami, FL 33136, USA.

出版信息

Brain Res. 2007 Dec 14;1185:117-28. doi: 10.1016/j.brainres.2007.09.013. Epub 2007 Sep 16.

Abstract

Chronic pain symptoms, including spontaneous unevoked pain and evoked cutaneous hypersensitivity, appear following spinal cord injury (SCI). A reliable preclinical model is needed to develop effective analgesic treatments for these symptoms. A previously described rat model of SCI pain was modified and behaviorally characterized and used to test clinically available drugs. A segment of the mid-thoracic spinal cord was compressed for 60 s with a micro-vascular clip. The sensitivity of the hind paws to noxious heat (Hargreaves test), innocuous tactile (von Frey filaments), and cooling (acetone) stimuli were determined once per week beginning 1 week following spinal compression. Spinal cord compression led to long lasting hypersensitivity to stimuli, lasting for at least 12 weeks post-surgery. Systemic baclofen, gabapentin, tramadol, and morphine dose-dependently attenuated tactile hypersensitivity. No effect on tactile hypersensitivity was observed with amitriptyline, carbamazepine, rofecoxib, and diazepam. Baclofen and morphine also dose-dependently ameliorated heat hypersensitivity. In contrast, no effect on heat hypersensitivity was observed with amitriptyline, carbamazepine, diazepam and gabapentin. The current data suggest that the model can potentially differentiate those drugs with analgesic efficacy from those that do not have efficacy in SCI pain. Thus, the model may be useful for rapid screening and clinical translation of promising SCI pain therapies.

摘要

脊髓损伤(SCI)后会出现慢性疼痛症状,包括自发性非诱发疼痛和诱发的皮肤超敏反应。需要一个可靠的临床前模型来开发针对这些症状的有效镇痛治疗方法。对先前描述的SCI疼痛大鼠模型进行了修改并进行行为特征分析,并用于测试临床可用药物。用微血管夹将胸段脊髓的一段压缩60秒。自脊髓压迫后1周开始,每周测定一次后爪对有害热(哈格里夫斯试验)、无害触觉(von Frey细丝)和冷却(丙酮)刺激的敏感性。脊髓压迫导致对刺激的长期超敏反应,持续至手术后至少12周。全身性巴氯芬、加巴喷丁、曲马多和吗啡剂量依赖性地减轻触觉超敏反应。阿米替林、卡马西平、罗非考昔和地西泮对触觉超敏反应无影响。巴氯芬和吗啡也剂量依赖性地改善热超敏反应。相比之下,阿米替林、卡马西平、地西泮和加巴喷丁对热超敏反应无影响。目前的数据表明,该模型有可能区分具有镇痛效果的药物和对SCI疼痛无效的药物。因此,该模型可能有助于对有前景的SCI疼痛治疗方法进行快速筛选和临床转化。

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