Alessandra Cipriano, Glen Apseloff, Ram P Kapil, Ellie He, Manjunath Shet, Stephen C Harris
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Each participant received each opioid antagonist twice per a randomized crossover schedule. Reversal of respiratory depression, pharmacokinetics, and safety were investigated. Participants showed rapid increases in plasma opioid antagonist concentrations, and meaningful reversal of depressed MV tended to occur earlier with IM nalmefene and IM naloxone than with IN naloxone. Compared to naloxone, nalmefene provided extended exposure, and mean MV was maintained at a higher level. All participants experienced treatment-related adverse events, but none were severe, serious, or led to study drug discontinuation. This study provides evidence that IM nalmefene 1 mg achieves reversal of fentanyl-induced respiratory depression similar to or better than that achieved with standard-of-care naloxone treatments. No new safety concerns were raised for IM nalmefene at the tested dose. 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引用次数: 0
摘要
阿片类药物过量死亡人数的增加,尤其是涉及强效长效合成阿片类药物的死亡人数的增加,导致人们呼吁使用更强效、更长效的阿片类药物过量逆转剂。我们利用阿片类药物诱导的呼吸抑制模型,研究了纳洛酮和长效阿片类药物拮抗剂纳美芬在长达 100 分钟的时间内逆转持续静脉注射芬太尼的作用的起效时间和作用过程。在根据呼吸分量(MV)的减少确定芬太尼诱导的呼吸抑制后,健康、中等经验的阿片类药物使用者分别接受了 1 毫克纳美芬(IM)、2 毫克纳洛酮(IM)或 4 毫克纳洛酮(IN)。每位受试者按随机交叉计划接受每种阿片类拮抗剂治疗两次。对呼吸抑制的逆转、药代动力学和安全性进行了研究。受试者的血浆阿片类拮抗剂浓度迅速升高,与 IN 纳洛酮相比,IM 纳美芬和 IM 纳洛酮往往更早出现有意义的呼吸抑制逆转。与纳洛酮相比,纳美芬的暴露时间更长,平均血浆拮抗剂浓度维持在更高水平。所有参与者都出现了与治疗相关的不良反应,但没有严重不良反应或导致停药。这项研究证明,1 毫克纳美芬 IM 可逆转芬太尼诱导的呼吸抑制,其效果与纳洛酮标准护理疗法相似或更好。在测试剂量下,即时注射纳美芬没有引起新的安全性问题。纳美芬注射液的药代动力学和药效学特性使其成为逆转阿片类药物过量的重要治疗选择,特别是考虑到涉及强效长效合成阿片类药物的过量用药现象日益普遍。
Time Course of Reversal of Fentanyl-Induced Respiratory Depression in Healthy Subjects by Intramuscular Nalmefene and Intramuscular and Intranasal Naloxone.
The increase in opioid overdose deaths, particularly involving potent, long-acting synthetic opioids, has led to calls for stronger, longer-acting opioid-overdose-reversal agents. Using an opioid-induced respiratory depression model, we investigated the onset and time course of action of naloxone and a long-acting opioid antagonist, nalmefene, in reversing the effects of an ongoing intravenous fentanyl infusion over a period of up to 100 min. Healthy, moderately experienced opioid users received intramuscular (IM) nalmefene 1 mg, IM naloxone 2 mg, or intranasal (IN) naloxone 4 mg after fentanyl-induced respiratory depression was established based on reduction in respiratory minute volume (MV). Each participant received each opioid antagonist twice per a randomized crossover schedule. Reversal of respiratory depression, pharmacokinetics, and safety were investigated. Participants showed rapid increases in plasma opioid antagonist concentrations, and meaningful reversal of depressed MV tended to occur earlier with IM nalmefene and IM naloxone than with IN naloxone. Compared to naloxone, nalmefene provided extended exposure, and mean MV was maintained at a higher level. All participants experienced treatment-related adverse events, but none were severe, serious, or led to study drug discontinuation. This study provides evidence that IM nalmefene 1 mg achieves reversal of fentanyl-induced respiratory depression similar to or better than that achieved with standard-of-care naloxone treatments. No new safety concerns were raised for IM nalmefene at the tested dose. The pharmacokinetic and pharmacodynamic properties of IM nalmefene position it as an important treatment option in opioid overdose reversal, particularly given the increasing prevalence of overdoses involving potent, long-acting synthetic opioids.
期刊介绍:
The Journal of Clinical Pharmacology (JCP) is a Human Pharmacology journal designed to provide physicians, pharmacists, research scientists, regulatory scientists, drug developers and academic colleagues a forum to present research in all aspects of Clinical Pharmacology. This includes original research in pharmacokinetics, pharmacogenetics/pharmacogenomics, pharmacometrics, physiologic based pharmacokinetic modeling, drug interactions, therapeutic drug monitoring, regulatory sciences (including unique methods of data analysis), special population studies, drug development, pharmacovigilance, womens’ health, pediatric pharmacology, and pharmacodynamics. Additionally, JCP publishes review articles, commentaries and educational manuscripts. The Journal also serves as an instrument to disseminate Public Policy statements from the American College of Clinical Pharmacology.