在产品剂量和适应症(标签外)外接受肌注(IM)奥氮平患者的回顾性(上市后)病例系列:评估安全性和耐受性

Joel Lamoure, A. Rudnick
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引用次数: 1

摘要

肌注奥氮平(IM)已被批准用于治疗继发于精神分裂症、双相情感障碍和痴呆的急性躁动/精神病,每次注射剂量不超过10mg,每天剂量不超过30mg。存在许多其他临床情况,患者急性激动,在这些情况下,IM奥氮平可能需要推荐或更高的剂量。我们系统地回顾了8例此类患者在10例住院期间的数据,以评估该方法的总体安全性和耐受性。方法采用标准化数据记录表,回顾性收集2004年至2007年间10例住院患者的信息,这些患者在产品剂量和/或适应症指南之外给予IM奥氮平。我们单独提供了复合数据和每个案例的详细信息。结果记录8例患者,其中男5例,女3例;平均年龄/年龄范围= 43.9/18-77岁)回顾了10例住院患者,5例精神科,4例外科,1例内科。入院指征为躁狂症(2例)、精神分裂症(1例)、分裂情感性障碍(2例)、脑损伤(2例)、败血症(1例)、败血症伴呼吸衰竭(1例)和癌症(1例)。5例患者醉酒或经历了酒精和/或药物戒断,可能增加了他们的躁动。在合并艰难梭菌性结肠炎的患者中,仅发生了一次直立性低血压的症状发作,在开始使用抗生素并停用奥氮平后,该症状得以缓解;2天后重新使用奥氮平,无意外。没有其他重大不良事件或副作用归因于IM奥氮平。结论在产品剂量和适应症指南之外,肌注奥氮平可能是安全的。随机临床试验有必要进一步研究这种超说明书使用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
A Retrospective (Post-Marketing) Case Series of Patients Receiving Intramuscular (IM) Olanzapine outside of Product Doses and Indications (Off-Label): Assessing Safety and Tolerability
Introduction Intramuscular (IM) olanzapine has been approved for the management of acute agitation/psychosis secondary to schizophrenia, bipolar disorder, and dementia, in a dose not to exceed 10 mg per injection and 30 mg per day. Many other clinical situations exist in which patients are acutely agitated and in whom IM olanzapine might be warranted at recommended or higher doses. We systematically reviewed data on 8 such patients, during 10 inpatient admissions, to assess the overall safety and tolerability of this approach. Methods Using a standardized data recording sheet, we retrospectively collected information on 10 inpatient admissions between 2004 and 2007, in which IM olanzapine was administered outside of product dosing and/or indication guidelines. We present composite data and the details of each case individually. Results Records of eight patients (5 males, 3 females; mean age/age range = 43.9/18–77 years) were reviewed over 10 inpatient admissions, 5 to Psychiatry, 4 to Surgery, and one to Internal Medicine. Indications for admission were mania (2), schizophrenia (1), schizoaffective disorder (2), brain injury (2), sepsis (1), sepsis with respiratory failure (1), and cancer (1). Five patients were intoxicated with or experienced withdrawal from alcohol and/or drugs, likely adding to their agitation. Only one symptomatic episode of orthostatic hypotension occurred, in a patient with comorbid C. difficile colitis, which resolved when antibiotics were initiated and olanzapine discontinued; olanzapine IM was successfully reinstituted 2 days later, without incident. No other significant adverse events or side effects were ascribed to IM olanzapine. Conclusions Intramuscular olanzapine may be safe to use outside of product dosing and indication guidelines. Randomized clinical trials are warranted to study such off-label use further.
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