鼻内注射纳美芬能减少阿片类药物过量致死的人数吗?

IF 1.5 4区 医学 Q3 PHARMACOLOGY & PHARMACY
Edward M. Sellers, Myroslava K. Romach
{"title":"鼻内注射纳美芬能减少阿片类药物过量致死的人数吗?","authors":"Edward M. Sellers,&nbsp;Myroslava K. Romach","doi":"10.1002/cpdd.1381","DOIUrl":null,"url":null,"abstract":"<p>This Journal recently published a paper describing the pharmacokinetics of a recently Food and Drug Administration (FDA) approved device for intranasal administration of the opioid receptor antagonist nalmefene.<span><sup>1</sup></span> Parenteral nalmefene was approved in 1995, but was subsequently withdrawn from the market by the manufacturer because of lack of market success. The new formulation (Trade Name Opvee, Indivior Inc., Richmond, VA) is “indicated for the emergency treatment of known or suspected overdose induced by natural or synthetic opioids in adults and pediatric patients aged 12 years and older, as manifested by respiratory and/or central nervous system depression”. The basis of this approval was nalmefene's high affinity as an antagonist at the mu opioid receptor, the apparent safety of nalmefene in humans, the pharmacokinetic similarity to intramuscular nalmefene, and the demonstration of changes in minute ventilation in an experimental ventilatory model assessed in non-dependent healthy subjects who received an infusion of remifentanil.</p><p>Despite the reportedly favorable pharmacokinetic profile of intranasal nalmefene, the likelihood that this new formulation will play a critical role in preventing opioid overdose deaths in the context of the public health opioid epidemic is questionable given the challenges that have confronted the widely known opioid receptor antagonist naloxone.<span><sup>2</sup></span></p><p>Naloxone, a pure opioid receptor antagonist, has been approved since 1971, is widely available, and can safely reverse the opioid induced respiratory depression and prevent deaths in medical and non-medical settings.<span><sup>3</sup></span> While naloxone is available in intranasal, intravenous, and intramuscular formulations and is effective in preventing opioid overdose death of individuals, the number of opioid overdose deaths continues to rise (about 80,000 per year).<span><sup>4</sup></span> This limited impact is disappointing but not surprising given the many practical obstacles associated with the use of opioid receptor antagonists, including the following: distribution of naloxone to the location of opioid overdose; providing training to first responders; direct and indirect cost of naloxone (in some cases naloxone is more expensive than the street price of opioids and other drugs); bias and prejudice about individuals who have opioid used disorder (OUD); a mismatch of the at-risk population to the available health services for immediate and longer term management of OUD; and a resistance by many opioid users to receive an antagonist and/or enter treatment. These challenges are further exacerbated by pervasive socio-economic factors, wide geographic variation in overdose rates, and uneven access to and cost of healthcare.</p><p>Intranasal nalmefene, like naloxone administered by similar routes, is rapidly absorbed. Theoretically the longer half-life of nalmefene (mean 11.3 hours compared to 30-90 minutes for naloxone) might make the drug useful for preventing and protecting against the toxic effects of longer-acting opioids. However, in emergent overdose situations usually the half-life of the opioid taken is not known. The longer half-life of the antagonist may be associated with a greater frequency of opiate withdrawal, which may need to be managed. The paper published in the Journal documents large variation in C<sub>max</sub> for intranasal nalmefene (typical coefficient of variation 50%-70%) suggesting that the actual clinical response to the intranasal nalmefene is not easily predicted and could be quite variable. However, measures of nalmefene opioid receptor occupancy and reversal of morphine-induced respiratory depression suggest quite prolonged effects, perhaps as long as 4-6 hours.<span><sup>5, 6</sup></span></p><p>Approval of the new intranasal formulation was based on the exposure equivalency of the intranasal to intramuscular route and not based on any actual patient data. Ideally, such data should be gathered as part of a postapproval monitoring, research or safety program. Three other factors may also limit clinical use of the new product: first, cost, which is expected to be greater than generic naloxone; second, the new formulation contains only a single dose, decreasing the flexibility of cost-effective repeat dosing if needed; and finally, lack of familiarity of physicians, first responders, and health facilities with “nalmefene”.</p><p>In our opinion, the new formulation and availability of intranasal nalmefene will save the lives of individuals who receive the drug; it is far less clear whether it will have a significant impact on overall rates of opioid-related overdose deaths and the public health crisis of OUD.</p><p>E.M.S. and M.K.R. have provided psychopharmacology consultant advice to pharmaceutical companies for which they received an hourly consultant fee. Neither E.M.S. nor M.K.R. has any equity or other compensation arrangements with any pharmaceutical company related to product development success or funding. None of the authors received any compensation for preparation of this Letter to the Editor.</p>","PeriodicalId":10495,"journal":{"name":"Clinical Pharmacology in Drug Development","volume":"13 3","pages":"315-316"},"PeriodicalIF":1.5000,"publicationDate":"2024-01-30","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://onlinelibrary.wiley.com/doi/epdf/10.1002/cpdd.1381","citationCount":"0","resultStr":"{\"title\":\"Can Intranasal Nalmefene Reduce the Number of Opioid Overdose Deaths?\",\"authors\":\"Edward M. Sellers,&nbsp;Myroslava K. Romach\",\"doi\":\"10.1002/cpdd.1381\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p>This Journal recently published a paper describing the pharmacokinetics of a recently Food and Drug Administration (FDA) approved device for intranasal administration of the opioid receptor antagonist nalmefene.<span><sup>1</sup></span> Parenteral nalmefene was approved in 1995, but was subsequently withdrawn from the market by the manufacturer because of lack of market success. The new formulation (Trade Name Opvee, Indivior Inc., Richmond, VA) is “indicated for the emergency treatment of known or suspected overdose induced by natural or synthetic opioids in adults and pediatric patients aged 12 years and older, as manifested by respiratory and/or central nervous system depression”. The basis of this approval was nalmefene's high affinity as an antagonist at the mu opioid receptor, the apparent safety of nalmefene in humans, the pharmacokinetic similarity to intramuscular nalmefene, and the demonstration of changes in minute ventilation in an experimental ventilatory model assessed in non-dependent healthy subjects who received an infusion of remifentanil.</p><p>Despite the reportedly favorable pharmacokinetic profile of intranasal nalmefene, the likelihood that this new formulation will play a critical role in preventing opioid overdose deaths in the context of the public health opioid epidemic is questionable given the challenges that have confronted the widely known opioid receptor antagonist naloxone.<span><sup>2</sup></span></p><p>Naloxone, a pure opioid receptor antagonist, has been approved since 1971, is widely available, and can safely reverse the opioid induced respiratory depression and prevent deaths in medical and non-medical settings.<span><sup>3</sup></span> While naloxone is available in intranasal, intravenous, and intramuscular formulations and is effective in preventing opioid overdose death of individuals, the number of opioid overdose deaths continues to rise (about 80,000 per year).<span><sup>4</sup></span> This limited impact is disappointing but not surprising given the many practical obstacles associated with the use of opioid receptor antagonists, including the following: distribution of naloxone to the location of opioid overdose; providing training to first responders; direct and indirect cost of naloxone (in some cases naloxone is more expensive than the street price of opioids and other drugs); bias and prejudice about individuals who have opioid used disorder (OUD); a mismatch of the at-risk population to the available health services for immediate and longer term management of OUD; and a resistance by many opioid users to receive an antagonist and/or enter treatment. These challenges are further exacerbated by pervasive socio-economic factors, wide geographic variation in overdose rates, and uneven access to and cost of healthcare.</p><p>Intranasal nalmefene, like naloxone administered by similar routes, is rapidly absorbed. Theoretically the longer half-life of nalmefene (mean 11.3 hours compared to 30-90 minutes for naloxone) might make the drug useful for preventing and protecting against the toxic effects of longer-acting opioids. However, in emergent overdose situations usually the half-life of the opioid taken is not known. The longer half-life of the antagonist may be associated with a greater frequency of opiate withdrawal, which may need to be managed. The paper published in the Journal documents large variation in C<sub>max</sub> for intranasal nalmefene (typical coefficient of variation 50%-70%) suggesting that the actual clinical response to the intranasal nalmefene is not easily predicted and could be quite variable. However, measures of nalmefene opioid receptor occupancy and reversal of morphine-induced respiratory depression suggest quite prolonged effects, perhaps as long as 4-6 hours.<span><sup>5, 6</sup></span></p><p>Approval of the new intranasal formulation was based on the exposure equivalency of the intranasal to intramuscular route and not based on any actual patient data. Ideally, such data should be gathered as part of a postapproval monitoring, research or safety program. Three other factors may also limit clinical use of the new product: first, cost, which is expected to be greater than generic naloxone; second, the new formulation contains only a single dose, decreasing the flexibility of cost-effective repeat dosing if needed; and finally, lack of familiarity of physicians, first responders, and health facilities with “nalmefene”.</p><p>In our opinion, the new formulation and availability of intranasal nalmefene will save the lives of individuals who receive the drug; it is far less clear whether it will have a significant impact on overall rates of opioid-related overdose deaths and the public health crisis of OUD.</p><p>E.M.S. and M.K.R. have provided psychopharmacology consultant advice to pharmaceutical companies for which they received an hourly consultant fee. Neither E.M.S. nor M.K.R. has any equity or other compensation arrangements with any pharmaceutical company related to product development success or funding. None of the authors received any compensation for preparation of this Letter to the Editor.</p>\",\"PeriodicalId\":10495,\"journal\":{\"name\":\"Clinical Pharmacology in Drug Development\",\"volume\":\"13 3\",\"pages\":\"315-316\"},\"PeriodicalIF\":1.5000,\"publicationDate\":\"2024-01-30\",\"publicationTypes\":\"Journal Article\",\"fieldsOfStudy\":null,\"isOpenAccess\":false,\"openAccessPdf\":\"https://onlinelibrary.wiley.com/doi/epdf/10.1002/cpdd.1381\",\"citationCount\":\"0\",\"resultStr\":null,\"platform\":\"Semanticscholar\",\"paperid\":null,\"PeriodicalName\":\"Clinical Pharmacology in Drug Development\",\"FirstCategoryId\":\"3\",\"ListUrlMain\":\"https://onlinelibrary.wiley.com/doi/10.1002/cpdd.1381\",\"RegionNum\":4,\"RegionCategory\":\"医学\",\"ArticlePicture\":[],\"TitleCN\":null,\"AbstractTextCN\":null,\"PMCID\":null,\"EPubDate\":\"\",\"PubModel\":\"\",\"JCR\":\"Q3\",\"JCRName\":\"PHARMACOLOGY & PHARMACY\",\"Score\":null,\"Total\":0}","platform":"Semanticscholar","paperid":null,"PeriodicalName":"Clinical Pharmacology in Drug Development","FirstCategoryId":"3","ListUrlMain":"https://onlinelibrary.wiley.com/doi/10.1002/cpdd.1381","RegionNum":4,"RegionCategory":"医学","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"Q3","JCRName":"PHARMACOLOGY & PHARMACY","Score":null,"Total":0}
引用次数: 0

摘要

本刊最近发表了一篇论文,介绍了美国食品药品管理局(FDA)最近批准的阿片受体拮抗剂纳美芬鼻内给药装置的药代动力学1。新制剂(商品名 Opvee,Indivior Inc.,弗吉尼亚州里士满)"适用于 12 岁及以上成人和儿童患者由天然或合成阿片类药物引起的已知或疑似用药过量的紧急治疗,表现为呼吸和/或中枢神经系统抑制"。此次批准的依据是纳美芬作为μ阿片受体拮抗剂的高亲和力、纳美芬对人体的明显安全性、与肌肉注射纳美芬相似的药代动力学,以及在非依赖性健康受试者输注瑞芬太尼后,在实验通气模型中评估分钟通气量变化的证明。尽管据报道鼻内注射纳美芬具有良好的药代动力学特征,但鉴于广为人知的阿片受体拮抗剂纳洛酮所面临的挑战,这种新制剂能否在公共卫生阿片类药物流行的背景下在预防阿片类药物过量致死方面发挥关键作用仍是个问题。纳洛酮是一种纯阿片受体拮抗剂,自 1971 年以来就已获得批准,可广泛获得,并能安全地逆转阿片类药物引起的呼吸抑制,防止医疗和非医疗环境中的死亡。3 虽然纳洛酮有鼻内、静脉注射和肌肉注射剂型,并能有效防止阿片类药物过量致死,但阿片类药物过量致死的人数仍在继续上升(每年约 8 万人)。4 这种有限的影响令人失望,但也不足为奇,因为使用阿片受体拮抗剂存在许多实际障碍,包括以下方面:将纳洛酮分发到阿片类药物过量的地点;为急救人员提供培训;纳洛酮的直接和间接成本(在某些情况下,纳洛酮比阿片类药物和其他药物的市价还贵);对阿片类药物滥用症(OUD)患者的偏见和成见;高危人群与现有的即时和长期阿片类药物滥用症管理医疗服务不匹配;以及许多阿片类药物使用者拒绝接受拮抗剂和/或接受治疗。这些挑战因普遍存在的社会经济因素、用药过量率的巨大地域差异以及医疗服务的可及性和成本不均而进一步加剧。理论上,纳美芬的半衰期较长(平均为 11.3 小时,而纳洛酮的半衰期为 30-90 分钟),因此该药物可用于预防和抵御长效阿片类药物的毒性作用。然而,在用药过量的紧急情况下,通常不知道所服用阿片类药物的半衰期。拮抗剂的半衰期越长,阿片类药物戒断的频率就越高,这可能需要加以控制。期刊上发表的论文记录了鼻内注射纳美芬 Cmax 的巨大差异(典型变异系数为 50%-70%),这表明鼻内注射纳美芬的实际临床反应并不容易预测,而且可能变化很大。然而,纳美芬阿片受体占有率和吗啡引起的呼吸抑制逆转的测量结果表明,纳美芬的作用时间相当长,可能长达 4-6 小时。理想情况下,此类数据应作为批准后监测、研究或安全计划的一部分加以收集。其他三个因素也可能限制新产品的临床应用:首先是成本,预计成本高于普通纳洛酮;其次,新配方只含单次剂量,降低了在需要时重复给药的成本效益灵活性;最后,医生、急救人员和医疗机构对 "纳美芬 "不熟悉。我们认为,鼻内注射纳美芬的新配方和可用性将挽救接受这种药物的人的生命;至于它是否会对阿片类药物相关过量死亡的总体比率和 OUD 的公共卫生危机产生重大影响,目前还不太清楚。E.M.S.和 M.K.R. 曾向制药公司提供精神药理学顾问建议,并按小时收取顾问费。E.M.S.和M.K.R.与任何制药公司都没有任何与产品开发成功或资金相关的股权或其他报酬安排。所有作者均未因撰写本致编辑函而获得任何报酬。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Can Intranasal Nalmefene Reduce the Number of Opioid Overdose Deaths?

This Journal recently published a paper describing the pharmacokinetics of a recently Food and Drug Administration (FDA) approved device for intranasal administration of the opioid receptor antagonist nalmefene.1 Parenteral nalmefene was approved in 1995, but was subsequently withdrawn from the market by the manufacturer because of lack of market success. The new formulation (Trade Name Opvee, Indivior Inc., Richmond, VA) is “indicated for the emergency treatment of known or suspected overdose induced by natural or synthetic opioids in adults and pediatric patients aged 12 years and older, as manifested by respiratory and/or central nervous system depression”. The basis of this approval was nalmefene's high affinity as an antagonist at the mu opioid receptor, the apparent safety of nalmefene in humans, the pharmacokinetic similarity to intramuscular nalmefene, and the demonstration of changes in minute ventilation in an experimental ventilatory model assessed in non-dependent healthy subjects who received an infusion of remifentanil.

Despite the reportedly favorable pharmacokinetic profile of intranasal nalmefene, the likelihood that this new formulation will play a critical role in preventing opioid overdose deaths in the context of the public health opioid epidemic is questionable given the challenges that have confronted the widely known opioid receptor antagonist naloxone.2

Naloxone, a pure opioid receptor antagonist, has been approved since 1971, is widely available, and can safely reverse the opioid induced respiratory depression and prevent deaths in medical and non-medical settings.3 While naloxone is available in intranasal, intravenous, and intramuscular formulations and is effective in preventing opioid overdose death of individuals, the number of opioid overdose deaths continues to rise (about 80,000 per year).4 This limited impact is disappointing but not surprising given the many practical obstacles associated with the use of opioid receptor antagonists, including the following: distribution of naloxone to the location of opioid overdose; providing training to first responders; direct and indirect cost of naloxone (in some cases naloxone is more expensive than the street price of opioids and other drugs); bias and prejudice about individuals who have opioid used disorder (OUD); a mismatch of the at-risk population to the available health services for immediate and longer term management of OUD; and a resistance by many opioid users to receive an antagonist and/or enter treatment. These challenges are further exacerbated by pervasive socio-economic factors, wide geographic variation in overdose rates, and uneven access to and cost of healthcare.

Intranasal nalmefene, like naloxone administered by similar routes, is rapidly absorbed. Theoretically the longer half-life of nalmefene (mean 11.3 hours compared to 30-90 minutes for naloxone) might make the drug useful for preventing and protecting against the toxic effects of longer-acting opioids. However, in emergent overdose situations usually the half-life of the opioid taken is not known. The longer half-life of the antagonist may be associated with a greater frequency of opiate withdrawal, which may need to be managed. The paper published in the Journal documents large variation in Cmax for intranasal nalmefene (typical coefficient of variation 50%-70%) suggesting that the actual clinical response to the intranasal nalmefene is not easily predicted and could be quite variable. However, measures of nalmefene opioid receptor occupancy and reversal of morphine-induced respiratory depression suggest quite prolonged effects, perhaps as long as 4-6 hours.5, 6

Approval of the new intranasal formulation was based on the exposure equivalency of the intranasal to intramuscular route and not based on any actual patient data. Ideally, such data should be gathered as part of a postapproval monitoring, research or safety program. Three other factors may also limit clinical use of the new product: first, cost, which is expected to be greater than generic naloxone; second, the new formulation contains only a single dose, decreasing the flexibility of cost-effective repeat dosing if needed; and finally, lack of familiarity of physicians, first responders, and health facilities with “nalmefene”.

In our opinion, the new formulation and availability of intranasal nalmefene will save the lives of individuals who receive the drug; it is far less clear whether it will have a significant impact on overall rates of opioid-related overdose deaths and the public health crisis of OUD.

E.M.S. and M.K.R. have provided psychopharmacology consultant advice to pharmaceutical companies for which they received an hourly consultant fee. Neither E.M.S. nor M.K.R. has any equity or other compensation arrangements with any pharmaceutical company related to product development success or funding. None of the authors received any compensation for preparation of this Letter to the Editor.

求助全文
通过发布文献求助,成功后即可免费获取论文全文。 去求助
来源期刊
CiteScore
3.70
自引率
10.00%
发文量
154
期刊介绍: Clinical Pharmacology in Drug Development is an international, peer-reviewed, online publication focused on publishing high-quality clinical pharmacology studies in drug development which are primarily (but not exclusively) performed in early development phases in healthy subjects.
×
引用
GB/T 7714-2015
复制
MLA
复制
APA
复制
导出至
BibTeX EndNote RefMan NoteFirst NoteExpress
×
提示
您的信息不完整,为了账户安全,请先补充。
现在去补充
×
提示
您因"违规操作"
具体请查看互助需知
我知道了
×
提示
确定
请完成安全验证×
copy
已复制链接
快去分享给好友吧!
我知道了
右上角分享
点击右上角分享
0
联系我们:info@booksci.cn Book学术提供免费学术资源搜索服务,方便国内外学者检索中英文文献。致力于提供最便捷和优质的服务体验。 Copyright © 2023 布克学术 All rights reserved.
京ICP备2023020795号-1
ghs 京公网安备 11010802042870号
Book学术文献互助
Book学术文献互助群
群 号:481959085
Book学术官方微信