Comparison of the μ-Opioid Receptor Antagonists Methocinnamox and Naloxone to Reverse and Prevent the Ventilatory Depressant Effects of Fentanyl, Carfentanil, 3-Methylfentanyl, and Heroin in Male Rats.

IF 3.1 3区医学 Q2 PHARMACOLOGY & PHARMACY

Journal of Pharmacology and Experimental Therapeutics Pub Date : 2024-09-18 DOI:10.1124/jpet.123.002032

Takato Hiranita, Nicholas P Ho, Charles P France

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引用次数: 0

Abstract

The number of opioid overdose deaths has increased significantly over the past decade. The life-threatening effect of opioids is hypoventilation, which can be reversed by the μ-opioid receptor (MOR) antagonist naloxone; however, because of the very short duration of action of naloxone, reemergence of MOR agonist-induced hypoventilation can occur, requiring additional doses of naloxone. The MOR antagonist methocinnamox (MCAM) antagonizes hypoventilation by the nonmorphinan fentanyl and the morphinan heroin in laboratory animals with an unusually long duration of action. Whole-body plethysmography was used to compare the potency and effectiveness of MCAM and naloxone for preventing and reversing hypoventilation by fentanyl, heroin, and the ultrapotent and longer-acting fentanyl analogs carfentanil and 3-methylfentanyl in male rats breathing normal air. Sessions comprised a 45-minute habituation period followed by intravenous administration of saline or an acute dose of MOR agonist. The rank order of potency to decrease ventilation was 3-methylfentanyl > carfentanil > fentanyl > heroin. MCAM (0.0001-0.1 mg/kg) and naloxone (0.0001-0.01 mg/kg) dose dependently reversed hypoventilation by 3-methylfentanyl (0.01 mg/kg), carfentanil (0.01 mg/kg), fentanyl (0.1 mg/kg), or heroin (3.2 mg/kg). For prevention studies, MCAM, naloxone, or vehicle was administered intravenously 22, 46, or 70 hours prior to a MOR agonist. When administered 22 hours earlier, MCAM (0.1-1.0 mg/kg) but not naloxone (1.0 mg/kg) prevented hypoventilation by each MOR agonist. This study demonstrates the effectiveness of MCAM at reversing and preventing hypoventilation by MOR agonists including ultrapotent fentanyl analogs that have a long duration of action. SIGNIFICANCE STATEMENT: The number of opioid overdose deaths increased over the past decade despite the availability of antagonists that can prevent and reverse the effects of opioids. This study demonstrates the effectiveness and long duration of action of the μ-opioid receptor (MOR) antagonist methocinnamox (MCAM) for reversing and preventing hypoventilation by MOR agonists including ultrapotent fentanyl analogs. These results provide support for the notion that MCAM has the potential to positively impact the ongoing opioid crisis by reversing and preventing opioid overdose.

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比较μ-阿片受体拮抗剂甲氧肉桂酸（MCAM）和纳洛酮在雄性大鼠体内逆转和预防芬太尼、卡芬太尼、3-甲基芬太尼和海洛因的通气抑制作用。

在过去十年中，阿片类药物过量致死的人数大幅增加。阿片类药物危及生命的影响是低通气，μ-阿片受体（MOR）拮抗剂纳洛酮可以逆转这种影响；但是，由于纳洛酮的作用时间很短，MOR激动剂引起的低通气可能再次出现，因此需要额外剂量的纳洛酮。MOR 拮抗剂甲氧肉桂醇（MCAM）可以拮抗非吗啡类芬太尼和吗啡类海洛因在实验室动物中造成的换气不足，而且作用时间异常长。在雄性大鼠呼吸正常空气的情况下，使用全身胸透法比较 MCAM 和纳洛酮在预防和逆转芬太尼、海洛因以及超强长效芬太尼类似物卡芬太尼和 3-甲基芬太尼造成的换气不足方面的效力和效果。实验过程包括 45 分钟的适应期，然后静脉注射生理盐水或急性剂量的 MOR 激动剂。降低通气量的效力排序为 3-甲基芬太尼 > 卡芬太尼 > 芬太尼 > 海洛因。MCAM（0.0001-0.1 毫克/千克）和纳洛酮（0.0001-0.01 毫克/千克）剂量依赖性地逆转了3-甲基芬太尼（0.01 毫克/千克）、卡芬太尼（0.01 毫克/千克）、芬太尼（0.1 毫克/千克）或海洛因（3.2 毫克/千克）造成的通气不足。在预防研究中，在使用 MOR 激动剂前 22、46 或 70 小时静脉注射 MCAM、纳洛酮或载体。如果提前 22 小时给药，MCAM（0.1-1.0 毫克/千克）而不是纳洛酮（1.0 毫克/千克）可防止每种 MOR 激动剂造成的通气不足。这项研究表明，MCAM 能够有效逆转和预防 MOR 激动剂（包括作用时间较长的超强芬太尼类似物）引起的换气不足。意义声明尽管拮抗剂可以预防和逆转阿片类药物的作用，但在过去十年中，阿片类药物过量致死的人数仍在增加。本研究证明了μ-阿片受体（MOR）拮抗剂甲氧肉桂酸（MCAM）在逆转和预防MOR激动剂（包括超强芬太尼类似物）引起的通气不足方面的有效性和长效性。这些结果为 MCAM 有可能通过逆转和预防阿片类药物过量对当前的阿片类药物危机产生积极影响这一观点提供了支持。

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来源期刊

Journal of Pharmacology and Experimental Therapeutics 医学-药学

CiteScore

6.90

自引率

0.00%

发文量

115

审稿时长

1 months

期刊介绍： A leading research journal in the field of pharmacology published since 1909, JPET provides broad coverage of all aspects of the interactions of chemicals with biological systems, including autonomic, behavioral, cardiovascular, cellular, clinical, developmental, gastrointestinal, immuno-, neuro-, pulmonary, and renal pharmacology, as well as analgesics, drug abuse, metabolism and disposition, chemotherapy, and toxicology.