肌肉注射纳洛酮 1600μg 联合滴定静脉注射纳洛酮 100μg 治疗阿片类药物中毒的疗效：一项随机对照试验。

Effectiveness of intramuscular naloxone 1,600 μg in addition to titrated intravenous naloxone 100 μg for opioid poisoning: a randomised controlled trial.

机构信息

Clinical Toxicology Unit, Princess Alexandra Hospital, Brisbane, Australia.

Faculty of Medicine, University of Queensland, Brisbane, Australia.

出版信息

Clin Toxicol (Phila). 2024 Oct;62(10):643-650. doi: 10.1080/15563650.2024.2396447. Epub 2024 Sep 5.

DOI:10.1080/15563650.2024.2396447

PMID:39235169

Abstract

INTRODUCTION

Naloxone is an effective antidote, but its short half-life means repeated doses, and infusions are often required. We investigated the effectiveness of adding intramuscular naloxone to titrated intravenous naloxone in opioid overdose in preventing recurrence of respiratory depression.

METHODS

This double-blinded randomised placebo-controlled trial was conducted in patients with suspected opioid poisoning and respiratory depression (respiratory rate <10 breaths/min or oxygen saturation <93%). Patients were randomised to receive either intramuscular naloxone 1,600 µg or saline placebo. All patients received titrated intravenous naloxone 100 µg and were managed on an opioid poisoning care pathway. The primary outcome was recurrence of respiratory depression within 4 h. Secondary outcomes were the proportion receiving naloxone infusions, number of naloxone boluses administered, reversal of respiratory depression at 10 min, and precipitation of opioid withdrawal (any symptom).

RESULTS

Recurrence of respiratory depression within 4 h was less common in 28/69 (41%) patients receiving intramuscular naloxone versus 48/67 (72%) patients receiving placebo (difference 31%, 95% CI: 13-46%; < 0.001). Fewer naloxone infusions (5/69; 7% versus 25/67; 37%, difference 30%, 95% CI: 15 to 55%; < 0.001) and fewer naloxone doses were administered (median 2, IQR: 1 to 5, versus median 5, IQR: 2 to 8; = 0.001) in the intramuscular group. Reversal of respiratory depression at 10 min was similar between groups (51/69; 74% intramuscular naloxone versus 47/67; 70% placebo; = 0.703). Opioid withdrawal occurred in 35/69 (51%) given intramuscular naloxone compared to 28/67 (42%) in the placebo group (difference 9%; 95% CI: -8 to 27%; = 0.308).

DISCUSSION

The favourable pharmacokinetics of intramuscular naloxone, particularly its longer duration of activity, likely explains the improved effectiveness with lower recurrence of respiratory depression.

CONCLUSION

The addition of intramuscular naloxone 1,600 µg to titrated intravenous naloxone prolonged effective reversal of respiratory depression, with fewer naloxone doses and infusions given, and no significant difference in patients developing withdrawal.

摘要

简介

纳洛酮是一种有效的解毒剂，但由于其半衰期短，需要重复给药，通常还需要静脉输注。我们研究了在阿片类药物过量中，在滴定静脉用纳洛酮的基础上加入肌肉注射纳洛酮，是否能预防呼吸抑制的复发。

方法

这是一项双盲、随机、安慰剂对照试验，在疑似阿片类药物中毒和呼吸抑制（呼吸频率<10 次/分或血氧饱和度<93%）的患者中进行。患者被随机分配接受肌肉注射纳洛酮 1600µg 或生理盐水安慰剂。所有患者均接受滴定静脉用纳洛酮 100µg，并按照阿片类药物中毒护理途径进行管理。主要结局是 4 小时内呼吸抑制的复发。次要结局是接受纳洛酮输注的比例、给予的纳洛酮冲击剂量、10 分钟时呼吸抑制的逆转以及阿片类药物戒断的发生（任何症状）。

结果

在接受肌肉注射纳洛酮的 69 例患者中，有 28 例（41%）在 4 小时内出现呼吸抑制的复发，而在接受安慰剂的 67 例患者中，有 48 例（72%）出现呼吸抑制的复发（差异 31%，95%CI：13-46%； <0.001）。接受肌肉注射纳洛酮的患者接受纳洛酮输注的次数较少（5/69；7%比 25/67；37%，差异 30%，95%CI：15 至 55%； <0.001），给予的纳洛酮剂量也较少（中位数 2，IQR：1 至 5，比中位数 5，IQR：2 至 8； = 0.001）。两组在 10 分钟时呼吸抑制的逆转情况相似（肌肉注射纳洛酮组 51/69；74%，安慰剂组 47/67；70%； = 0.703）。接受肌肉注射纳洛酮的患者中有 35 例（51%）发生阿片类药物戒断，而接受安慰剂的患者中有 28 例（42%）发生阿片类药物戒断（差异 9%，95%CI：-8 至 27%； = 0.308）。