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右旋苯丙胺可加速大鼠大剂量芬太尼给药后意识和呼吸驱动力的恢复。

D-Amphetamine Accelerates Recovery of Consciousness and Respiratory Drive After High-Dose Fentanyl in Rats.

作者信息

Moody Olivia A, Zhang Edlyn R, Arora Vipin, Kato Risako, Cotten Joseph F, Solt Ken

机构信息

Department of Anesthesia, Critical Care and Pain Medicine, Massachusetts General Hospital, Boston, MA, United States.

Department of Anaesthesia, Harvard Medical School, Boston, MA, United States.

出版信息

Front Pharmacol. 2020 Nov 12;11:585356. doi: 10.3389/fphar.2020.585356. eCollection 2020.

Abstract

In the United States, fentanyl causes approximately 60,000 drug overdose deaths each year. Fentanyl is also frequently administered as an analgesic in the perioperative setting, where respiratory depression remains a common clinical problem. Naloxone is an efficacious opioid antagonist, but it possesses a short half-life and undesirable side effects. This study was conducted to test the hypothesis that d-amphetamine ameliorates respiratory depression and hastens the return of consciousness following high-dose fentanyl. Behavioral endpoints (first head movement, two paws down, and return of righting), arterial blood gas analysis and local field potential recordings from the prefrontal cortex were conducted in adult rats after intravenous administration of of fentanyl (55 µg/kg) at a dose sufficient to induce loss of righting and respiratory depression, followed by intravenous d-amphetamine (3 mg/kg) or saline (vehicle). D-amphetamine accelerated the time to return of righting by 36.6% compared to saline controls. D-amphetamine also hastened recovery of arterial pH, and the partial pressure of CO2, O2 and sO2 compared to controls, with statistically significant differences in pH after 5 min and 15 min. Local field potential recordings from the prefrontal cortex showed that within 5 min of d-amphetamine administration, the elevated broadband power <20 Hz produced by fentanyl had returned to awake baseline levels, consistent with the return of consciousness. Overall, d-amphetamine attenuated respiratory acidosis, increased arterial oxygenation, and accelerated the return of consciousness in the setting of fentanyl intoxication. This suggests that d-amphetamine may be a useful adjunct or alternative to opioid receptor antagonists such as naloxone.

摘要

在美国,芬太尼每年导致约6万例药物过量死亡。芬太尼在围手术期也常被用作镇痛药,而呼吸抑制仍是一个常见的临床问题。纳洛酮是一种有效的阿片类拮抗剂,但它半衰期短且有不良副作用。本研究旨在验证以下假设:右旋苯丙胺可改善高剂量芬太尼引起的呼吸抑制并加速意识恢复。在成年大鼠静脉注射足以导致翻正反射消失和呼吸抑制的芬太尼(55μg/kg)后,进行行为学指标(首次头部移动、双爪着地和翻正反射恢复)、动脉血气分析以及前额叶皮质局部场电位记录,随后分别静脉注射右旋苯丙胺(3mg/kg)或生理盐水(溶剂对照)。与生理盐水对照组相比,右旋苯丙胺使翻正反射恢复时间加快了36.6%。与对照组相比,右旋苯丙胺还加速了动脉血pH值、二氧化碳分压、氧分压和氧饱和度的恢复,5分钟和15分钟后的pH值有统计学显著差异。前额叶皮质局部场电位记录显示,在注射右旋苯丙胺后5分钟内,芬太尼引起的20Hz以下宽带功率升高已恢复到清醒基线水平,这与意识恢复一致。总体而言,右旋苯丙胺减轻了呼吸性酸中毒,增加了动脉氧合,并加速了芬太尼中毒时的意识恢复。这表明右旋苯丙胺可能是纳洛酮等阿片受体拮抗剂的有用辅助药物或替代品。

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