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阿片类药物依赖维持性药物治疗的原理。

Rationale for maintenance pharmacotherapy of opiate dependence.

作者信息

Kreek M J

机构信息

Rockefeller University, New York, New York 10021.

出版信息

Res Publ Assoc Res Nerv Ment Dis. 1992;70:205-30.

PMID:1346939
Abstract

At this time, 27 years after the initial studies on development of methadone for the maintenance treatment of opiate addiction were begun, it has been shown that [table; see text] methadone meets most criteria for a pharmacologic agent for chronic treatment of an addiction. It is effective after oral dosing: it has a long biological half-life in humans, it causes minimal side effects when used in chronic treatment, and it has no true toxic effects or serious side effects. Also methadone has been shown to be very effective when appropriately used in programs which combine pharmacotherapy with the best elements of "drug free" treatment, that is, counseling and psychological support. In addition to pharmacological treatment, there should be access to, if not on-site, medical and behavioral care as needed, as well as linkage to resources for various aspects of rehabilitation. At this time many of the actions, as well as the specific sites of action, and mechanisms of actions of methadone as used in chronic treatment of opiate addiction have been defined by scientific experimentation, both at the preclinical and clinical levels. It is known that methadone prevents abstinence symptoms, prevents drug hunger or craving, blocks euphorogenic effects of other opiates, and prevents relapse to illicit use of opiates. It is known that the site of action of methadone is at specific opioid receptors. Research to date suggests that there is no demonstrable down-regulation or up-regulation of opioid receptors during chronic opioid agonist perfusion, although chronic administration of the opioid antagonist naltrexone does appear to up-regulate opioid receptors. Clinical studies show that chronic use of methadone allows normalization of release and peripheral levels of one of the classes of endogenous opioids, beta-endorphin, and the related peptides derived from POMC released and processed from the anterior pituitary in humans. Also levels of beta-endorphin in cerebrospinal fluid become normal during chronic maintenance treatment, reflecting apparently normal processing and release of beta-endorphin at brain or hypothalamic sites of POMC production. Available data from studies of beta-endorphin indicate that there is a [table; see text] normalization, rather than disruption, of the endogenous opioid system in general during steady state administration of methadone, as contrasted with intermittent dosing and then abrupt withdrawal of short-acting opiates such as heroin. Although there is still much to be learned about the neurobiology of opiate addiction, at this time we do know a great deal about the effects of opiates and opioids.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

此时,距离最初开展美沙酮用于阿片类药物成瘾维持治疗的研究已过去27年,研究表明[表格;见正文]美沙酮符合作为一种用于成瘾慢性治疗的药物制剂的大多数标准。口服给药后它是有效的:在人体中它具有较长的生物半衰期,在慢性治疗中使用时产生的副作用极小,并且它没有真正的毒性作用或严重副作用。此外,当美沙酮在将药物治疗与“无毒品”治疗的最佳要素(即咨询和心理支持)相结合的项目中得到适当使用时,已证明它非常有效。除了药物治疗外,如有需要,应能获得医疗和行为护理,即使不是现场提供,也要能联系到康复各方面的资源。此时,美沙酮在阿片类药物成瘾慢性治疗中所起的许多作用、具体作用部位以及作用机制已通过临床前和临床层面的科学实验得以明确。已知美沙酮可预防戒断症状、防止对药物的渴望或渴求、阻断其他阿片类药物的欣快作用,并防止复吸非法使用阿片类药物。已知美沙酮的作用部位是特定的阿片受体。迄今为止的研究表明,在慢性阿片类激动剂灌注期间,阿片受体没有可证明的下调或上调,尽管长期给予阿片拮抗剂纳曲酮似乎确实会使阿片受体上调。临床研究表明,长期使用美沙酮可使内源性阿片类物质之一β-内啡肽以及人类垂体前叶释放和加工的源自阿片促黑皮质素原的相关肽的释放和外周水平恢复正常。在慢性维持治疗期间,脑脊液中β-内啡肽的水平也恢复正常,这显然反映了在阿片促黑皮质素原产生的脑或下丘脑部位β-内啡肽的正常加工和释放。来自β-内啡肽研究的现有数据表明,与间歇性给药然后突然停用海洛因等短效阿片类药物相比,在美沙酮稳态给药期间,内源性阿片系统总体上是恢复正常,而非受到破坏。尽管关于阿片类药物成瘾的神经生物学仍有许多有待了解之处,但此时我们确实对阿片类药物和阿片样物质的作用了解很多。(摘要截选至400字)

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