氯氮平引起的心肌炎可能与快速滴定有关

N. Chopra, J. de Leon
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引用次数: 36

摘要

氯氮平引起的心肌炎是一种鲜为人知的、罕见的、潜在致命的药物不良反应,其绝对风险在澳大利亚为7 - 34 / 1000,在其他国家为0.07-0.6 / 1000。已假定过敏反应,包括一些可能与快速滴定有关的病例。这个病例描述了一个50岁的非洲裔美国人患有分裂情感性障碍,naïve氯氮平,他可能死于氯氮平引起的心肌炎。他开始服用25毫克/天的氯氮平,并在14天内服用1625毫克,直到他在第15天死亡。尸检发现血管周围软组织和心室心肌主要有淋巴细胞浸润,偶有嗜酸性粒细胞。使用利物浦不良反应因果关系评估工具,认为患者的死亡可能继发于心肌炎。患者暴发性死亡,生命体征无明显变化。c反应蛋白和肌钙蛋白都没有检测到,但结果不太可能及时到达以防止患者死亡。年龄、快速滴定和同时使用丙戊酸钠是导致本病例的原因,这可能是与快速滴定相关的特殊药物不良反应。拉莫三嗪诱导的史蒂文斯-约翰逊综合征似乎也是一种与快速滴定相关的特殊药物不良反应,但由于推荐的拉莫三嗪起始剂量减少并通过丙戊酸盐等抑制剂的作用得到纠正,其发生率已显著降低。同样,氯氮平引起的心肌炎发生率可能可以通过使用缓慢的滴定来降低,包括对氯氮平代谢能力较低的患者,如服用丙戊酸盐的患者,使用更慢的滴定。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Clozapine-induced myocarditis may be associated with rapid titration
Clozapine-induced myocarditis is a poorly understood, rare, potentially fatal adverse drug reaction with absolute risks ranging from 7 to 34 per 1000 in Australia and 0.07–0.6 per 1000 in other countries. Hypersensitivity reactions have been postulated including some cases probably associated with rapid titrations. This case describes a 50-year-old African-American man with schizoaffective disorder, naïve to clozapine, who probably died from clozapine-induced myocarditis. He was started on 25 mg/day of clozapine and received 1625 mg over 14 days, prior to his death on day 15. The autopsy found predominantly lymphocytic infiltrate of the perivascular soft tissue and myocardium of the ventricles, with occasional eosinophils. Using the Liverpool ADR Causality Assessment Tool, it was deemed probable that the patient’s death was secondary to myocarditis. The patient had fulminant death with no obvious changes in vital signs. Neither C-reactive protein nor troponin was measured, but it is unlikely that the results would have arrived in time to prevent the patient’s death. Age, rapid titration, and concomitant use of valproate contributed to this case, which was probably an idiosyncratic adverse drug reaction associated with rapid titration. Lamotrigine-induced Stevens-Johnson syndrome also appears to be an idiosyncratic adverse drug reaction associated with rapid titration, but its incidence has been remarkably reduced since the recommended starting lamotrigine dose was reduced and corrected by the effect of inhibitors such as valproate. Similarly, clozapine-induced myocarditis incidence probably can be reduced with the use of slow titrations, including even slower titrations for patients with lower ability to metabolize clozapine, such as those taking valproate.
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