查看原文
其他

奥氮平治疗恶心、谵妄、焦虑、失眠和恶病质的证据汇总

2016-06-24 大话精神

奥氮平属于第二代非典型抗精神病药物,临床上常被超说明书用于治疗成人恶心、谵妄、焦虑、失眠和恶病质。因此,姑息治疗的临床医生可以利用它来缓解他们患者的多种症状。本文将审查奥氮平超说明书使用的药理学和可用证据。

药理学:奥氮平具有独特的作用受体,拮抗中枢神经系统多巴胺受体(治疗恶心、谵妄),抑制5-HT2受体(失眠、焦虑、恶病质有关)及抗胆碱能作用[1-3]。达峰时间约为6小时,终末消除半衰期21-54小时[4]

不良反应和注意事项:与其他抗精神病药相比,奥氮平较少引起锥体外系症状[5],对QTc间期的影响小于氟哌啶醇[6],但嗜睡[7]和体重增加[8-10]的不良反应较明显。此外,奥氮平与口干、高血糖症、水肿以及老年痴呆患者的死亡率有关。肾或肝损害的患者无需调整剂量,肝病终末期谨慎使用。

研究数据

恶心:两个病例报告和一项回顾性试验研究了奥氮平对慢性恶心、呕吐的疗效,平均剂量5mg/d[12,13]。在一项开放性标签研究中,晚期癌症患者接受奥氮平2.5mg-10mg,生活质量显著改善,恶心症状缓解[14]。对于化疗引起的恶心和呕吐(CINV),许多有力的证据支持奥氮平的疗效[15]。一项双盲随机对照试验表明,奥氮平对于CINV的治疗要优于胃复安(无呕吐比例70%vs31%a number-needed-to-treat of 2.5[16]

谵妄:奥氮平对谵妄的疗效已被证明与氟哌啶醇相当。剂量范围为2.5mg-10mg/d,最大剂量可达20mg/d[17]。一项针对晚期癌症患者的开放标签初步研究发现,37%的患者对奥氮平(5mg-10mg/d)治疗有响应[18]。在另一项前瞻性开放试验中,79例癌症住院患者服用奥氮平治疗谵妄,结果76%的患者症状完全缓解[19]

焦虑:奥氮平已被研究用于难治性焦虑症(GAD)。在一项随机安慰剂对照试验中,氟西汀单药治疗效果不佳的GAD患者添加奥氮平或安慰剂,结果发现,奥氮平(平均剂量8.7mg/d)疗效优于安慰剂[20]

失眠:奥氮平(初始最小剂量2.5mg)辅助SSRI可以提高抑郁症患者的睡眠效率、改善睡眠质量[21]。此外,还有研究发现,单剂量10mg奥氮平能够增加慢波睡眠及总睡眠时间[3]

恶病质:奥氮平已被研究用于慢性疾病如癌症相关的恶病质治疗。奥氮平5mg/d辅助醋酸甲地孕酮治疗,能显著刺激患者食欲,增加体重[22]。在一项开放标签研究中,奥氮平2.5-20mg单药治疗能够减弱晚期癌症患者的体重减轻现象[23]

总结

证据表明,奥氮平对于化疗所致的恶心和呕吐具有一定的疗效,还对谵妄、焦虑、失眠、恶病质同样有效。然而,由于其治疗成本和长期护理中的潜在障碍,姑息治疗的临床医生要充分权衡,谨慎对待这些超说明书使用。

参考文献


1. JacksonWC, Manning JS, Connor PD et al. Retrospective Study of Olanzapine inDepressive and Anxious States in Primary Care. Prim Care Companion J ClinPsychiatry. 2004; 6(5):199-202.

2. MoY, Yam F. Rational Use of Second-Generation antipsychotic for the Treatment ofICU Delirium: A Neuropharmacological Approach. J Pharm Pract. 2015 Jun 1.pii:0897190015585763 [Epub ahead of print].)

3. LindbergN, Wirkkunen M, Tani P et al. Effect of a single-dose of olanzapine on sleep inhealthy females and males. Int Clin Psychopharmacol. 2002 Jul; 17(4):177-84.

4. CallaghanJT, Bergstrom RF, Ptak LR, Beasley CM. Olanzapine. Pharmacokinetic andpharmacodynamic profile. Clin Pharmacokinet. 1999 Sep;37(3):177-93.

5. MeltzerHY, Fibiger HC. Olanzapine: a new typical antipsychotic drug.Neuropsychopharmacology. 1996 Feb;14(2):83-5.

6. WashingtonNB, Brahm NC, Kissack J. Which psychotropics carry the greatest risk of QTcprolongation? Curr Psychiatry. 2012 Oct;11(10):36-39.

7. MillerDD. Atypical antipsychotics: sleep, sedation, and efficacy. Prim Care CompanionJ Clin Psychiatry. 2004;6(Suppl 2):3-7.

8. NasrallahH. A review of the effect of atypical antipsychotics on weight.Psychoneuroendocrinology. 2003 Jan;28 Suppl 1:83-96.

9. PrommerE. Olanzapine: Palliative Medicine Update. Am J Hosp Palliat Care.2012;30(1):75-82.

10. FremauxT, Reymann JM, Chevreuil C et al. Prescription of olanzapine in children andadolescent psychiatric patients. Encephale. 2007 Mar-Apr;33(2):188-96.

11. ProductInformation: ZYPREXA(R) oral tablets, olanzapine oral tablets. Lilly USA, LLC(per FDA), Indianapolis, IN, 2013.

12. GlareP, Miller J, Nikolova T, Tickoo R. Treating nausea and vomiting in palliativecare: a review. Clin Interv Aging. 2011;6:243-59.

13. KaneishiK, Kawabata M, Morita T. Olanzapine for the relief of nausea in patients withadvanced cancer and incomplete bowel obstruction. J Pain Symptom Manage. 2012Oct;44(4):604-7.

14. PassikSD, Lundberg J, et al. A pilot exploration of the antiemetic activity ofolanzapine for the relief of nausea in patients with advanced cancer and pain.J Pain Symptom Manage. 2002 Jun;23(6):526-32.

15. HockingCM, Kichenadasse G. Olanzapine for chemotherapy-induced nausea and vomiting: asystematic review. Support Care Cancer. 2014 Apr;22(4):1143-51.

16. NavariRM, Nagy CK, Gray SE. The use of olanzapine versus metoclopramide for thetreatment of breakthrough nausea and vomiting in patients receiving highlyemetogenic chemotherapy. Support Care Cancer. 2013 Jun;21(6):1655-63.

17. GrassiL, Caraceni A, Mitchell A et al. Management of Delirium in Palliative Care: aReview. Curr Psychiatry Rep (2015)17:13.).

18. ElsayemA, Bush SH, Munsell MF, Curry 3rd E, Calderon BB, Paraskevopoulos T, et al.Subcutaneous olanzapine for hyperactive or mixed delirium in patients withadvanced cancer: a preliminary study. J Pain Symptom Manag. 2010;40:774–82.

19. BreitbartW, Tremblay A, Gibson C. An open trial of olanzapine for the treatment ofdelirium in hospitalized cancer patients. Psychosomatics. 2002;43(3):175-182.

20. PollackMH, Simon NM, Zalta AK et al. Olanzapine augmentation of fluoxetine forrefractory generalized anxiety disorder: a placebo controlled study. BiolPsychiatry. 2006 Feb 1;59(3):211-5. Epub 2005 Sep 1.

21. SharpleyAL, Attenburrow ME, Hafizi S et al. Olanzapine increases slow wave sleep andsleet continuity in SSRI-resistant depressed patients. J Clin Psychiatry. 2005Apr;66(4):450-4.

22. NavariRM and Brenner MC. Treatment of cancer-related anorexia with olanzapine andmegestrol acetate: a randomized trial. Supp Care Cancer. 2010;18:951-956.

23. NaingA, Dalal S, Abdelrahim et al. Olanzapine for cachexia in patients with advancecancer: an exploratory study of effects on weight and metabolic cytokines. SuppCare Cancer. 2015; 23:2649-2654.


文献索引

Felton M, Weinberg R, Pruskowski J. Olanzapine for Nausea, Delirium, Anxiety, Insomnia, and Cachexia# 315[J]. Journal of palliative medicine, 2016.

姑息医学杂志,双月刊,发表临床、教育、重病和死亡患者护理的法律和伦理等跨学科研究,包括对危及生命的疾病,比如癌症、艾滋病、心脏病、神经系统、呼吸系统疾病等患者的药物和非药物治疗的最新进展。ISSN:1096-62182015年影响因子2.023


大话精神编译,转载请注明出处,原文索取请联系我们。

您可能也对以下帖子感兴趣

文章有问题?点此查看未经处理的缓存