氧化亚氮再探讨:强效抗痛觉过敏特性的证据。
Nitrous oxide revisited: evidence for potent antihyperalgesic properties.
作者信息
Richebé Philippe, Rivat Cyril, Creton Cyril, Laulin Jean-Paul, Maurette Pierre, Lemaire Marc, Simonnet Guy
机构信息
Department of Anesthesia and Intensive Care II, Centre Hospitalier et Universitaire de Bordeaux, Bordeaux, France.
出版信息
Anesthesiology. 2005 Oct;103(4):845-54. doi: 10.1097/00000542-200510000-00024.
BACKGROUND
Although opioids are unsurpassed analgesics for surgery, they also induce an N-methyl-D-aspartate-dependent enhancement of postoperative hyperalgesia. Because nitrous oxide (N2O) has anti-N-methyl-D-aspartate properties, the purpose of this study was to evaluate nitrous oxide ability to prevent such an opioid-induced hyperalgesia in rats.
METHODS
First, preventive effects of 50/50% N2O-O2 on the development of delayed hyperalgesia observed after inflammatory pain (hind paw carrageenan injection on D0) were examined for several days. Second, the ability of nitrous oxide (10-40%) to limit opioid-induced hyperalgesia induced by fentanyl was evaluated in nonsuffering rats. Third, antihyperalgesic effects of various nitrous oxide concentrations (20-50%) were assessed in both inflammatory and incisional pain models in fentanyl-treated rats (4 x 100 microg/kg subcutaneously). Finally, the analgesic effect of a single dose of morphine was evaluated 24 h after fentanyl administration and nitrous oxide (D0) to assess its preventive effect on acute morphine tolerance in both nonsuffering and hind paw-incised rats.
RESULTS
When applied on D0, nitrous oxide reduced delayed hyperalgesia induced by inflammation. Exposure to nitrous oxide on D0 also reduced opioid-induced hyperalgesia in nonsuffering rats in a dose-dependent manner. In fentanyl-treated rats with inflammatory or incisional pain, nitrous oxide strongly limited both magnitude and duration of hyperalgesia. Moreover, nitrous oxide exposure on D0 opposed development of acute tolerance to analgesic effects of morphine administered on D1 in both nonsuffering and incised fentanyl-treated rats.
CONCLUSIONS
Nitrous oxide, an N-methyl-D-aspartate receptor antagonist, prevented the enhancement of pain sensitivity induced by both nociceptive inputs and fentanyl and opposed acute morphine tolerance. Results suggest that perioperative nitrous oxide use reduces exaggerated postoperative pain and morphine consumption.
背景
尽管阿片类药物是手术中无与伦比的镇痛药,但它们也会诱导一种依赖N-甲基-D-天冬氨酸的术后痛觉过敏增强。由于氧化亚氮(N2O)具有抗N-甲基-D-天冬氨酸特性,本研究的目的是评估氧化亚氮预防大鼠此类阿片类药物诱导的痛觉过敏的能力。
方法
首先,检测50/50% N2O-O2对炎症性疼痛(D0日在后爪注射角叉菜胶)后观察到的延迟性痛觉过敏发展的预防作用,持续数天。其次,在未遭受疼痛的大鼠中评估氧化亚氮(10-40%)限制芬太尼诱导的阿片类药物诱导的痛觉过敏的能力。第三,在芬太尼处理的大鼠(4×100μg/kg皮下注射)的炎症性和切口性疼痛模型中评估不同浓度氧化亚氮(20-50%)的抗痛觉过敏作用。最后,在芬太尼给药和氧化亚氮处理(D0)24小时后评估单剂量吗啡的镇痛效果,以评估其对未遭受疼痛和后爪切开大鼠急性吗啡耐受性的预防作用。
结果
在D0日应用时,氧化亚氮可减轻炎症诱导的延迟性痛觉过敏。D0日暴露于氧化亚氮也以剂量依赖的方式减轻了未遭受疼痛大鼠中阿片类药物诱导的痛觉过敏。在患有炎症性或切口性疼痛的芬太尼处理的大鼠中,氧化亚氮强烈限制了痛觉过敏的程度和持续时间。此外,D0日暴露于氧化亚氮可对抗未遭受疼痛和切开的芬太尼处理的大鼠中D1日给予吗啡的镇痛效果的急性耐受性的发展。
结论
氧化亚氮作为一种N-甲基-D-天冬氨酸受体拮抗剂,可预防伤害性刺激输入和芬太尼诱导的疼痛敏感性增强,并对抗急性吗啡耐受性。结果表明,围手术期使用氧化亚氮可减轻术后过度疼痛并减少吗啡用量。
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