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通过连续微量渗透泵鞘内输注法测定大鼠脊髓的交叉耐受性。

Determination of cross tolerance in rat spinal cord using intrathecal infusion via sequential mini-osmotic pumps.

作者信息

Loomis C W, Milne B, Cervenko F W

出版信息

Pharmacol Biochem Behav. 1987 Jan;26(1):131-9. doi: 10.1016/0091-3057(87)90545-4.

Abstract

Continuous intrathecal (IT) infusion via ALZET mini-osmotic pumps was used to induced spinal tolerance to morphine in the rat. Naloxone (1 mg/kg IP), injected on day 3 of continuous IT morphine (10 micrograms/hr), produced mild withdrawal symptoms in all morphine-treated animals. In rats pretreated with continuous IT morphine (10 micrograms/hr) or saline, systemic morphine (2, 4, 8, 10 and 15 mg/kg IP) produced equivalent, dose-dependent antinociception using the tail-flick and paw pressure tests. The rostral and caudal distribution of methylene blue dye in rat spinal cord was determined on days 1-7 of continuous IT infusion. The dye remained localized near the catheter tip throughout infusion; maximum distribution was 1.5 cm rostrally and 1.0 cm caudally. The data indicate that morphine, infused at the rate of 10 micrograms/hr, does not undergo extensive redistribution in the spinal cord. A sequential, double mini-osmotic pump technique for cross tolerance studies in rat spinal cord is described. In rats pretreated with continuous IT norepinephrine for 4 days, the antinociceptive actions of continuous IT morphine were reduced but not significantly different from saline-pretreated animals. These data suggest that morphine, injected into the spinal cord, does not produce behavioural analgesia by activation of local adrenergic systems.

摘要

通过ALZET微型渗透泵进行连续鞘内(IT)输注,用于诱导大鼠对吗啡产生脊髓耐受性。在连续鞘内输注吗啡(10微克/小时)的第3天注射纳洛酮(1毫克/千克,腹腔注射),在所有接受吗啡治疗的动物中均产生了轻度戒断症状。在用连续鞘内吗啡(10微克/小时)或生理盐水预处理的大鼠中,使用甩尾和爪压试验,全身性吗啡(2、4、8、10和15毫克/千克,腹腔注射)产生了等效的、剂量依赖性的抗伤害感受作用。在连续鞘内输注的第1至7天,测定了亚甲蓝染料在大鼠脊髓中的头端和尾端分布。在整个输注过程中,染料一直局限于导管尖端附近;最大分布在头端1.5厘米和尾端1.0厘米处。数据表明,以10微克/小时的速率输注的吗啡在脊髓中不会发生广泛的重新分布。描述了一种用于大鼠脊髓交叉耐受性研究的顺序双微型渗透泵技术。在用连续鞘内去甲肾上腺素预处理4天的大鼠中,连续鞘内吗啡的抗伤害感受作用降低,但与生理盐水预处理的动物相比无显著差异。这些数据表明,注入脊髓的吗啡不会通过激活局部肾上腺素能系统产生行为性镇痛。

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