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氯胺酮(
最近有研究发现,氯胺酮这种名声不好的毒品可能是治疗抑郁症的理想药物,而且起效速度超快,并能对抗抑郁症自杀,这一发现可能导致大量精神病医生大量使用这种非标药物治疗抑郁症、也引来一大批医药公司开展这一老药新效的临床研究,更重要的是发现这种药物竟然具有对抗自杀行为的作用,也进一步说明抑郁症自杀行为是独立于其他抑郁行为的表现,给人们研究这种疾病的机理提供了新方向。
经典的抗抑郁药物一般需要持续数周才开始发挥作用,最新研究发现氯胺酮使用后最快2小时就可以发挥作用,这甚至让人联想到用阿司匹林类药物降低体温这样的场景,大汗一出,体温正常。纽约西奈山医院精神病学家James Murrough认为,这一新发现启动了治疗抑郁症新时代。
医院公司将会在此基础上着手开发拥有专利权的药物,科学家将会探索为什么这种药物能产生抗抑郁作用的神经基础。虽然有些医生会担心,在不清楚这种药物的长期作用的情况下,应慎重使用这种药物,肯定有许多临床医生将会给患者服用这一非标药物治疗抑郁症患者。
由于对治疗抑郁症的药物效果失望,过去5年许多药物公司停止了这方面的投入,近10年来几乎没有任何明显能提高治疗效果的药物出现。美国国立精神健康研究所所长Thomas Insel说,由于治疗抑郁症的药物效果一直让大家非常失望,这是为什么大家对发现氯胺酮具有抗抑郁症新作用激动的原因。
目前最常用的抗抑郁药物是针对大脑内的五羟色胺和去甲肾上腺素通路的药物。氯胺酮的作用是阻断谷氨酸的NMDA受体,NMDA受体是脑内重要的兴奋通路,主要参与学习记忆功能的调节。氯胺酮是经过大量研究的麻醉药物,但过去并没有人知道NMDA受体和抑郁症有什么关系。
2013年,Murrough小组发表了关于这种非标药物氯胺酮治疗抑郁症的研究,73名患者参加了这一研究,这些患者都曾经尝试过3-4种抗抑郁药物都没有取得理想效果。研究结果发现,氯胺酮使用后24小时让64%的患者抑郁表现产生效果。对照组使用镇静药咪达唑仑的有效率只有28%。(J. W. Murrough et al. Am. J. Psychiatry 170, 1134–1142; 2013)..Murrough小组现在使用大脑成象技术研究这些患者大脑,以尝试寻找药物作用的基础。
Murrough说,将这种药物作为常规广泛使用前,长期效应研究必须开展。宾夕法尼亚大学生物伦理学家Dominic Sisti担心许多医生可能已经考虑使用这种药物。西奈山医院精神病学家Kyle Lapidus认为,这种药物的使用方法也需要慎重考虑,他已经给部分患者使用了这种药物,猜测有许多医生也已经开始这么干。治疗剂量就能快速产生“分离性幻觉”持续不超过1小时。更高剂量可产生‘K-hole’,这种表现5至20分钟开始产生放松、欣快感及产生性欲,感觉如同喝醉酒,但头脑仍清楚,这也是该药物被滥用的基础。
ntravenous ketamine demonstrated rapid antidepressant effects in an optimized study design, improving depression severity in 64% of treatment-resistant patients 24 hours after a single dose. The double-blind trial provides evidence for the role of the N-methyl-d-aspartate glutamate receptor in depression, a receptor not currently activated by existing antidepressant drugs.
Ketamine, a glutamate N-methyl-d-aspartate (NMDA) receptor antagonist, has shown rapid antidepressant effects, but small study groups and inadequate control conditions in prior studies have precluded a definitive conclusion. The authors evaluated the rapid antidepressant efficacy of ketamine in a large group of patients with treatment-resistant major depression.
This was a two-site, parallel-arm, randomized controlled trial of a single infusion of ketamine compared to an active placebo control condition, the anesthetic midazolam. Patients with treatment-resistant major depression experiencing a major depressive episode were randomly assigned under double-blind conditions to receive a single intravenous infusion of ketamine or midazolam in a 2:1 ratio (N=73). The primary outcome was change in depression severity 24 hours after drug administration, as assessed by the Montgomery-Åsberg Depression Rating Scale (MADRS).
The ketamine group had greater improvement in the MADRS score than the midazolam group 24 hours after treatment. After adjustment for baseline scores and site, the MADRS score was lower in the ketamine group than in the midazolam group by 7.95 points (95% confidence interval [CI], 3.20 to 12.71). The likelihood of response at 24 hours was greater with ketamine than with midazolam (odds ratio, 2.18; 95% CI, 1.21 to 4.14), with response rates of 64% and 28%, respectively.
Ketamine demonstrated rapid antidepressant effects in an optimized study design, further supporting NMDA receptor modulation as a novel mechanism for accelerated improvement in severe and chronic forms of depression. More information on response durability and safety is required before implementation in clinical practice.
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