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鞘内给药对大鼠脊髓伤害性感觉活动的抑制作用:地西泮的效应

Depression of nociceptive sensory activity in the rat spinal cord due to the intrathecal administration of drugs: effect of diazepam.

作者信息

Jurna I

出版信息

Neurosurgery. 1984 Dec;15(6):917-20.

PMID:6096760
Abstract

The intrathecal (i.t.) administration of morphine inhibits nociceptive motor responses and activity in ascending axons evoked by stimulation of nociceptive afferent nerve fibers (nociceptive sensory response) in the rat. The i.t. administration of cholecystokinin octapeptide and ceruletide inhibits nociceptive motor responses, but does not affect ascending nociceptive activity. This shows that drug-induced depression of nociceptive motor responses is not always associated with depression of the nociceptive sensory response of the spinal cord. The microiontophoretic application of substance P excites single dorsal horn neurons that respond to noxious stimulation, whereas the i.t. administration of substance P inhibits both nociceptive motor and sensory responses. Thus, the results obtained from the i.t. administration of a drug may differ from those obtained from its application to single spinal neurons. Diazepam inhibits spinal reflexes and may reduce pain sensation in humans. To assess whether a spinal action is involved in the pain-relieving effect of diazepam, experiments were carried out on spinalized rats in which activity evoked by the stimulation of nociceptive and nonnociceptive afferent nerve fibers of the sural nerve was recorded from single ascending axons below the site of spinal cord transection. Diazepam, 20 micrograms i.t., reduced activity evoked by afferent A delta and C fiber stimulation and by stimulation of afferent A beta fibers. The depressant effect caused by diazepam, 2 mg/kg i.v., on C fiber-evoked ascending activity was reduced by the i.t. injection of the benzodiazepine antagonist, Ro 15-1788 (40 micrograms), an imidazodiazepine. It is concluded that the depression by diazepam of C fiber-evoked ascending activity contributes to pain relief caused by the drug.

摘要

鞘内注射吗啡可抑制大鼠伤害性传入神经纤维受刺激所诱发的伤害性运动反应及上行轴突的活动(伤害性感觉反应)。鞘内注射八肽胆囊收缩素和蛙皮素可抑制伤害性运动反应,但不影响上行伤害性活动。这表明药物诱导的伤害性运动反应抑制并不总是与脊髓伤害性感觉反应的抑制相关。微量离子电泳施加P物质可兴奋对伤害性刺激有反应的单个背角神经元,而鞘内注射P物质则可抑制伤害性运动和感觉反应。因此,鞘内给药所得结果可能与将药物应用于单个脊髓神经元所得结果不同。地西泮可抑制脊髓反射,并可能减轻人类的疼痛感。为评估脊髓作用是否参与地西泮的镇痛效果,对脊髓横断大鼠进行了实验,在脊髓横断部位下方的单个上行轴突记录腓肠神经伤害性和非伤害性传入神经纤维受刺激所诱发的活动。鞘内注射20微克地西泮可降低Aδ和C纤维传入刺激以及Aβ纤维传入刺激所诱发的活动。静脉注射2毫克/千克地西泮对C纤维诱发的上行活动的抑制作用,可被鞘内注射苯二氮䓬拮抗剂Ro 15 - 1788(40微克)(一种咪唑并二氮䓬)所减弱。得出的结论是,地西泮对C纤维诱发的上行活动的抑制作用有助于该药物引起的疼痛缓解。

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