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阿片类药物引起的呼吸抑制和脑缺氧:吗啡、羟考酮、海洛因和芬太尼。

Respiratory depression and brain hypoxia induced by opioid drugs: Morphine, oxycodone, heroin, and fentanyl.

机构信息

Behavioral Neuroscience Branch, National Institute on Drug Abuse - Intramural Research Program, National Institute of Health, DHHS, 333 Cassell Drive, Baltimore, MD, 21224, USA.

出版信息

Neuropharmacology. 2019 Jun;151:219-226. doi: 10.1016/j.neuropharm.2019.02.008. Epub 2019 Feb 5.

Abstract

Opioid drugs are important tools to alleviate pain of different origins, but they have strong addictive potential and their abuse at higher doses often results in serious health complications. Respiratory depression that leads to brain hypoxia is perhaps the most dangerous symptom of acute intoxication with opioids, and it could result in lethality. The development of substrate-specific sensors coupled with amperometry made it possible to directly evaluate physiological and drug-induced fluctuations in brain oxygen levels in awake, freely-moving rats. The goal of this review paper is to consider changes in brain oxygen levels induced by several opioid drugs (heroin, fentanyl, oxycodone, morphine). While some of these drugs are widely used in clinical practice, they all are abused, often at doses exceeding the clinical range and often resulting in serious health complications. First, we consider some basic knowledge regarding brain oxygen, its physiological fluctuations, and mechanisms involved in regulating its entry into brain tissue. Then, we present and discuss data on brain oxygen changes induced by each opioid drug within a wide range of doses, from low, behaviorally relevant, to high, likely to be self-administered by drug users. These data allowed us to compare the effects of these drugs on brain oxygen in terms of their potency, time-course, and their potential danger when used at high doses via rapid-onset administration routes. While most data discussed in this work were obtained in rats, we believe that these data have clear human relevance in addressing the alarming rise in lethality associated with the opioid abuse.

摘要

阿片类药物是缓解不同来源疼痛的重要工具,但它们具有很强的成瘾潜力,高剂量滥用常常导致严重的健康并发症。呼吸抑制导致脑缺氧可能是阿片类药物急性中毒最危险的症状,可能导致死亡。与安培法相结合的底物特异性传感器的发展使得能够在清醒、自由移动的大鼠中直接评估生理和药物诱导的脑氧水平波动。本文的目的是考虑几种阿片类药物(海洛因、芬太尼、羟考酮、吗啡)引起的脑氧水平变化。虽然这些药物中的一些在临床实践中广泛使用,但它们都被滥用,通常在超过临床剂量的情况下使用,并且经常导致严重的健康并发症。首先,我们考虑一些关于脑氧的基本知识,包括其生理波动以及调节其进入脑组织的机制。然后,我们介绍并讨论了在广泛剂量范围内(从低剂量、行为相关到高剂量,可能由药物使用者自行给药)每种阿片类药物引起的脑氧变化的数据。这些数据使我们能够根据这些药物对脑氧的作用强度、时程以及在高剂量时通过快速起效的给药途径使用时的潜在危险来比较它们的作用。虽然本文讨论的大多数数据是在大鼠中获得的,但我们认为这些数据在解决与阿片类药物滥用相关的致命性上升问题方面具有明确的人类相关性。

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