Gowing L, Ali R, White J
University of Adelaide, Department of Clinical and Experimental Pharmacology, DASC Evidence-Bsed Practice Unit, Adelaide, Australia, 5005.
Cochrane Database Syst Rev. 2006 Apr 19(2):CD002022. doi: 10.1002/14651858.CD002022.pub2.
Withdrawal (detoxification) is necessary prior to drug-free treatment. It may also represent the end point of long-term opioid replacement treatment such as methadone maintenance. The availability of managed withdrawal is essential to an effective treatment system.
To assess the effectiveness of interventions involving the administration of opioid antagonists to induce opioid withdrawal with concomitant heavy sedation or anaesthesia, in terms of withdrawal signs and symptoms, completion of treatment and adverse effects.
We searched the Drugs and Alcohol Group register (October 2003), Cochrane Central Register of Controlled Trials (The Cochrane Library, Issue 4, 2004), Medline (January 1966 to January 2005), Embase (January 1985 to January 2005), PsycINFO (1967 to January 2005), and Cinahl (1982 to December 2004) and reference lists of studies.
Controlled trials comparing antagonist-induced withdrawal under heavy sedation or anaesthesia with another form of treatment, or a different regime of anaesthesia-based antagonist-induced withdrawal.
One reviewer assessed studies for inclusion and undertook data extraction and assessed quality. Inclusion decisions and the overall process were confirmed by consultation between all three reviewers.
Six studies (five randomised controlled trials) involving 834 participants met the inclusion criteria for the review.Antagonist-induced withdrawal is more intense but less prolonged than withdrawal managed with reducing doses of methadone, and doses of naltrexone sufficient for blockade of opioid effects can be established significantly more quickly with antagonist-induced withdrawal than withdrawal managed with clonidine and symptomatic medications. The level of sedation does not affect the intensity and duration of withdrawal, although the duration of anaesthesia may influence withdrawal severity. There is a significantly greater risk of adverse events with heavy, compared to light, sedation (RR 3.21, 95% CI 1.13 to 9.12, P = 0.03) and probably also other forms of detoxification.
AUTHORS' CONCLUSIONS: Heavy sedation compared to light sedation does not confer additional benefits in terms of less severe withdrawal or increased rates of commencement on naltrexone maintenance treatment. Given that the adverse events are potentially life-threatening, the value of antagonist-induced withdrawal under heavy sedation or anaesthesia is not supported. The high cost of anaesthesia-based approaches, both in monetary terms and use of scarce intensive care resources, suggest that this form of treatment should not be pursued.
在进行无毒品治疗之前,脱毒(戒毒)是必要的。它也可能代表长期阿片类药物替代治疗(如美沙酮维持治疗)的终点。可管理的脱毒对有效的治疗系统至关重要。
评估使用阿片类拮抗剂诱导阿片类药物脱毒并伴有深度镇静或麻醉的干预措施在脱毒体征和症状、治疗完成情况及不良反应方面的有效性。
我们检索了药物与酒精研究组登记册(2003年10月)、Cochrane对照试验中心注册库(Cochrane图书馆,2004年第4期)、Medline(1966年1月至2005年1月)、Embase(1985年1月至2005年1月)、PsycINFO(1967年至2005年1月)以及Cinahl(1982年至2004年12月),并查阅了研究的参考文献列表。
比较在深度镇静或麻醉下拮抗剂诱导脱毒与另一种治疗形式,或不同的基于麻醉的拮抗剂诱导脱毒方案的对照试验。
一名评价者评估纳入研究,进行数据提取并评估质量。纳入决策和整个过程经所有三名评价者协商确认。
六项研究(五项随机对照试验)涉及834名参与者,符合本综述的纳入标准。与用逐渐减少剂量的美沙酮进行的脱毒相比,拮抗剂诱导的脱毒更强烈但持续时间更短,并且与用可乐定和对症药物进行的脱毒相比,使用拮抗剂诱导脱毒能显著更快地确定足以阻断阿片类药物作用的纳曲酮剂量。镇静水平不影响脱毒的强度和持续时间,尽管麻醉持续时间可能影响脱毒严重程度。与轻度镇静相比,深度镇静时不良事件的风险显著更高(相对危险度3.21,95%可信区间1.13至9.12,P = 0.03),可能其他形式的戒毒也是如此。
与轻度镇静相比,深度镇静在减轻脱毒严重程度或提高纳曲酮维持治疗开始率方面并无额外益处。鉴于不良事件可能危及生命,不支持在深度镇静或麻醉下进行拮抗剂诱导脱毒。基于麻醉的方法成本高昂,无论是在金钱方面还是在稀缺的重症监护资源使用方面,这表明不应采用这种治疗形式。
