Center for Compulsive Behavior and Addiction, Rush University Medical Center, Chicago, IL, USA.
Pharmacol Ther. 2012 Dec;136(3):343-53. doi: 10.1016/j.pharmthera.2012.08.013. Epub 2012 Aug 29.
Understanding substance use disorders (SUDs) and the problems associated with abstinence has grown in recent years. Nonetheless, highly efficacious treatment targeting relapse prevention has remained elusive, and there remains no FDA-approved pharmacotherapy for psychostimulant dependence. Preclinical and clinical investigations assessing the utility of classical antidepressants, which block monoamine reuptake, show mixed and often contradictory results. Mirtazapine (Remeron®) is a unique FDA-approved antidepressant, with negligible affinity for reuptake proteins, indirectly augments monoamine transmission presumably through antagonist activity at multiple receptors including the norepinephrine (NE)(α2), and serotonin (5-HT)(2A/C) receptors. Historically, mirtazapine was also considered to be a 5-HT(2C) antagonist, but recent evidence indicates that mirtazapine is an inverse agonist at this receptor subtype. Suggesting a promising role for mixed-action serotonergic drugs for addiction pharmacotherapy, mirtazapine attenuates psychostimulant-induced behaviors in several rodent models of substance abuse, and antagonizes methamphetamine-induced biochemical and electrophysiological alterations in rats. Preclinical findings are confirmed through published case studies documenting successful outcomes with mirtazapine therapy across a number of SUDs. To date, a large scale clinical trial assessing the utility of mirtazapine in substance abuse pharmacotherapy has yet to be conducted. However, as reviewed here, accumulating preclinical and clinical evidence argues that mirtazapine, or compounds that emulate aspects of its pharmacological profile, may prove useful in helping treat addictions.
近年来,人们对物质使用障碍(SUD)及其与戒断相关的问题的理解有了深入的认识。尽管如此,针对复发预防的高效治疗方法仍然难以实现,并且仍然没有 FDA 批准的治疗精神兴奋剂依赖的药物治疗方法。评估经典抗抑郁药(阻断单胺再摄取)效用的临床前和临床研究结果喜忧参半,且往往相互矛盾。米氮平(Remeron®)是一种独特的 FDA 批准的抗抑郁药,对再摄取蛋白的亲和力可忽略不计,通过在包括去甲肾上腺素(NE)(α2)和 5-羟色胺(5-HT)(2A/C)受体在内的多种受体上的拮抗作用,间接增强单胺传递。历史上,米氮平也被认为是 5-HT(2C)拮抗剂,但最近的证据表明,米氮平是该受体亚型的反向激动剂。这表明混合作用的 5-羟色胺能药物在成瘾药物治疗方面有很好的应用前景,米氮平可减弱几种物质滥用的啮齿动物模型中的精神兴奋剂诱导行为,并拮抗安非他命引起的大鼠生化和电生理改变。通过记录米氮平治疗多种物质使用障碍的成功案例研究,证实了临床前发现。迄今为止,尚未进行评估米氮平在物质滥用药物治疗中的效用的大规模临床试验。然而,如本文所述,越来越多的临床前和临床证据表明,米氮平或模仿其药理学特征的化合物可能有助于治疗成瘾。