Clozapine/administration and dosage

氯氮平 / 给药和剂量
  • 文章类型: Journal Article
    背景:药物警戒研究表明氯氮平病史以药物不良反应(ADR)为特征。
    目标:在一篇2021年的文章中,英国(英国)在VigiBase中超过90%的欧洲氯氮平相关致命结局,世界卫生组织的药物警戒数据库。两个可能相反的假设可以解释这种差异:1)其他西欧国家报告的致命结果较少,主要反映了对VigiBase的报告不足,2)英国报告数量越多,反映出实际相对死亡率越高。
    方法:对2022年12月31日氯氮平介绍的VigiBase报告进行了ADR和致命结局的十大原因研究。英国与其他11个报告最多的西方国家(德国,丹麦,法国,芬兰,爱尔兰,意大利,荷兰,挪威,西班牙,瑞典和瑞士)。在控制人口和氯氮平处方后,对9个国家(爱尔兰和瑞士除外)进行了比较。
    结果:英国占全球氯氮平相关致死结局的29%,德国2%,其他国家都<1%。非特异性标签“死亡”是世界上最大的原因(46%)和英国(33%)。“肺炎”居世界第二(8%),英国(12%),爱尔兰(8%)和芬兰(14%)。假设我们对人口和氯氮平使用的修正是正确的,其他国家仅少报了英国氯氮平致死结局数的1-10%.
    结论:与英国相比,不同的西欧国家始终向VigiBase报告不足,但对于氯氮平相关的ADR/致命性结局有不同的报告/发布方式。三个斯堪的纳维亚登记册表明,随着氯氮平使用量的增加,生命得以挽救,但这不能在药物警戒数据库中进行研究.
    BACKGROUND: Pharmacovigilance studies indicate clozapine history is marked by adverse drug reactions (ADRs).
    OBJECTIVE: In a 2021 article, the United Kingdom (UK) had >90 % of European clozapine-related fatal outcomes in VigiBase, the World Health Organization\'s pharmacovigilance database. Two possibly opposing hypotheses could explain this disparity: 1) fewer reported fatal outcomes in other Western European countries mainly reflect underreporting to VigiBase, and 2) the higher number of UK reports reflects higher real relative mortality.
    METHODS: VigiBase reports from clozapine\'s introduction to December 31, 2022, were studied for ADRs and the top 10 causes of fatal outcomes. The UK was compared with 11 other top reporting Western countries (Germany, Denmark, France, Finland, Ireland, Italy, Netherlands, Norway, Spain, Sweden and Switzerland). Nine countries (except Ireland and Switzerland) were compared after controlling for population and clozapine prescriptions.
    RESULTS: The UK accounted for 29 % of worldwide clozapine-related fatal outcomes, Germany 2 % and <1 % in each of the other countries. The nonspecific label \"death\" was the top cause in the world (46 %) and in the UK (33 %). \"Pneumonia\" was second in the world (8 %), the UK (12 %), Ireland (8 %) and Finland (14 %). Assuming that our corrections for population and clozapine use are correct, other countries underreported only 1-10 % of the UK clozapine fatal outcome number.
    CONCLUSIONS: Different Western European countries consistently underreport to VigiBase compared to the UK, but have different reporting/publishing styles for clozapine-related ADRs/fatal outcomes. Three Scandinavian registries suggest lives are saved as clozapine use increases, but this cannot be studied in pharmacovigilance databases.
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  • 文章类型: Journal Article
    背景:文献很少关注心包炎,儿童和青少年氯氮平治疗期间心包积液和胰腺炎。
    方法:使用以下搜索对儿童氯氮平相关性心包炎和胰腺炎的病例进行了研究:1)PubMed(2023年6月16日),和2)世界卫生组织药物警戒数据库(2022年6月1日),VigiBase。Vigibase使用称为信息分量(IC)的不成比例性的对数度量。
    结果:PubMed搜索产生了3例氯氮平相关心包炎病例,1例胰腺炎病例和1例两者兼有。VigiBase提供了明显的氯氮平相关心包炎IC=3.6,IC025=2.9(预计仅3例,观察到22例)。VigiBase提供了显着的氯氮平相关胰腺炎IC=2.2,IC025=1.4(仅预期3例,而观察到16例)。在VigiBase中,青年时期氯氮平相关的心包炎和心包积液看起来相似,并且与心肌炎的连续性相似,如心肌炎,心包炎和胰腺炎似乎主要发生在氯氮平滴定期间。结合PubMed和VigiBase我们确定:1)29例至少可能的氯氮平相关心包炎/心包积液(6例可能和23例可能),包括7例心肌炎和22例无心肌炎,2)氯氮平相关性胰腺炎17例(明确1例,可能16例)。其中2例胰腺炎发生在用药过量期间。在任何氯氮平相关的心包炎和胰腺炎病例中均未发现致命结局。
    结论:尽管文献中对氯氮平相关性心包炎和胰腺炎缺乏关注,结果表明,它们可能发生在青年时期,特别是在滴定过程中。在剂量滴定期间,心包炎和胰腺炎似乎是氯氮平相关炎症的形式。
    BACKGROUND: The literature has paid very little attention to pericarditis, pericardial effusion and pancreatitis during clozapine treatment in children and adolescents.
    METHODS: Cases of clozapine-associated pericarditis and pancreatitis in children were studied using searches in: 1) PubMed (June 16, 2023), and 2) the World Health Organization\'s pharmacovigilance database (June 1, 2022), VigiBase. VigiBase uses a logarithmic measure of disproportionality called the information component (IC).
    RESULTS: The PubMed search yielded 3 clozapine-associated pericarditis cases, 1 pancreatitis case and 1 with both. VigiBase provided a significant clozapine-associated pericarditis IC = 3.6 with an IC025 = 2.9 (only 3 cases were expected while 22 were observed). VigiBase provided a significant clozapine-associated pancreatitis IC = 2.2 with an IC025 = 1.4 (only 3 cases were expected while 16 were observed). In VigiBase clozapine-associated pericarditis and pericardial effusion in youth looked similar and on a continuum with myocarditis, as myocarditis, pericarditis and pancreatitis appeared to occur mainly during clozapine titration. Combining PubMed and VigiBase we identified: 1) 29 cases of at least possible clozapine-associated pericarditis/pericardial effusion (6 probable and 23 possible) including 7 cases with and 22 without myocarditis, and 2) 17 cases of clozapine-associated pancreatitis (1 definite and 16 possible). Two of the pancreatitis cases occurred during overdoses. No fatal outcomes were found in any clozapine-associated pericarditis and pancreatitis cases.
    CONCLUSIONS: Despite the lack of attention in the literature to clozapine-associated pericarditis and pancreatitis, results demonstrate that they can happen in youth, particularly during titration. Pericarditis and pancreatitis appear to be forms of clozapine-associated inflammation during dose titration.
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  • 文章类型: Journal Article
    目的:比较患病率,法规,以及东欧国家(俄罗斯除外)使用氯氮平的药物警戒措施。
    方法:问卷调查和来自行政数据库的数据(2016年和2021年),来自21个国家的21名共同作者收集了包装说明书和国家指南.从介绍到2022年12月31日,分析了发送到全球药物警戒数据库(VigiBase™)的氯氮平不良反应(ADR)的报告。
    结果:2021年抗精神病药物中的氯氮平处方在各国之间变化了六倍,从捷克共和国的2.8%到黑山的15.8%。2016年和2021年,克罗地亚的抗精神病药物使用率最高,最低的是2016年的塞尔维亚和2021年的黑山,与克罗地亚的数据相比,其定义的每日剂量(DDD)/1000/天的一半。从2016年到2021年,几乎所有国家使用抗精神病药物的患病率都在增加;氯氮平的使用比例基本保持不变。在血液学监测要求和氯氮平批准的适应症方面检测到差异。只有少数国家精神分裂症指南提到氯氮平诱发的心肌炎或单独的滴定方案。VigiBase搜索表明,有关氯氮平及其致命结局的报告严重不足。相比之下,英国的人口不到这些东欧国家的一半,但向VigiBase报告的氯氮平不良反应增加了89倍,氯氮平致死结局增加了近300倍.
    结论:氯氮平在东欧国家应用不足。引入个性化的氯氮平治疗方案可能有助于最大限度地提高氯氮平的益处和安全性。东欧国家在报告氯氮平不良反应和致命结局方面需要重大改进。
    OBJECTIVE: To compare the prevalence, regulations, and pharmacovigilance practices of clozapine use in Eastern European countries (except Russia).
    METHODS: Questionnaires and data from administrative databases (2016 and 2021), package inserts and national guidelines were collected from 21 co-authors from 21 countries. Reports of clozapine adverse drug reactions (ADRs) sent to the global pharmacovigilance database (VigiBase™) were analyzed from introduction to December 31, 2022.
    RESULTS: Clozapine prescription among antipsychotics in 2021 varied six-fold across countries, from 2.8 % in the Czech Republic to 15.8 % in Montenegro. The utilization of antipsychotics in both 2016 and 2021 was highest in Croatia, and lowest in Serbia in 2016, and Montenegro in 2021, which had half the defined daily dose (DDD)/1000/day compared to the Croatian data. From 2016 to 2021, the prevalence of antipsychotic use increased in almost all countries; the proportion of clozapine use mainly remained unchanged. Differences were detected in hematological monitoring requirements and clozapine approved indications. Only a few national schizophrenia guidelines mention clozapine-induced myocarditis or individual titration schemes. The VigiBase search indicated major underreporting regarding clozapine and its fatal outcomes. By comparison, the United Kingdom had less than half the population of these Eastern European countries but reported to VigiBase more clozapine ADRs by 89-fold and clozapine fatal outcomes by almost 300-fold.
    CONCLUSIONS: Clozapine is under-utilized in Eastern European countries. Introducing individualized clozapine treatment schedules may help to maximize clozapine benefits and safety. Major improvement is needed in reporting clozapine ADRs and fatal outcomes in Eastern European countries.
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  • 文章类型: Journal Article
    背景:氯氮平诱导的心肌炎或任何氯氮平诱导的炎症可能是一种超敏反应,因为滴定对患者的氯氮平代谢而言太快。氯氮平的代谢受祖先的影响,性别,吸烟和肥胖等混杂因素的存在,感染,和抑制剂(例如,丙戊酸盐)导致患者表现为氯氮平代谢不良(PM)。土耳其一家医院发表的一项研究确定了1例氯氮平诱发的胰腺炎和肝炎以及9例氯氮平诱发的心肌炎。为了探索10例患者为氯氮平PMs的假设,我们使用浓度剂量比(C/D)调查了他们的血清氯氮平浓度,并仔细审查了他们的滴定法.
    方法:将血清谷浓度除以剂量得出氯氮平C/D比。达到350ng/ml所需的剂量被认为是最小治疗剂量,并用于根据氯氮平PM状态对患者进行分类。评估滴定速度。
    结果:所有10例患者可能是氯氮平PMs(其中3例的最低治疗剂量为72、82或83mg/天)。10名患者中的9名可能由于肥胖和/或在滴定期间丙戊酸盐共同处方而表现为氯氮平PM。一个人也有未诊断的感染。在10个病人中,9至少有3个因素中的1个:在第一周或第二周滴定太快,或最终剂量太高。
    结论:未来使用氯氮平水平并考虑氯氮平PM状态的作用的研究应探索是否所有氯氮平诱导的炎症病例都可以通过缺乏个体化滴定来解释。
    Clozapine-induced myocarditis or any clozapine-induced inflammation may be a hypersensitivity reaction due to titration that was too rapid for the patient\'s clozapine metabolism. Clozapine metabolism is influenced by ancestry, sex, smoking and the presence of confounders including obesity, infections, and inhibitors (e.g., valproate) causing the patient to behave as a clozapine poor metabolizer (PM). A published study in a Turkish hospital identified 1 case of clozapine-induced pancreatitis and hepatitis and 9 cases of clozapine-induced myocarditis. To explore the hypothesis that the 10 patients were clozapine PMs, their serum clozapine concentrations were investigated using concentration-to-dose (C/D) ratios and their titrations carefully reviewed.
    Dividing the trough serum concentration by the dose produces the clozapine C/D ratio. The dose required to reach 350ng/ml was considered the minimum therapeutic dosage and was used to classify patients according to clozapine PM status. Titration speed was assessed.
    All 10 patients were possibly clozapine PMs (3 of them had as minimum therapeutic doses: 72, 82 or 83mg/day). Nine of the 10 patients may have behaved as clozapine PMs due to obesity and/or valproate co-prescription during titration. One also had an undiagnosed infection. Of the 10 patients, 9 had at least 1 of 3 factors: too-rapid titration in the first or second weeks, or a final dosage that was too high.
    Future studies using clozapine levels and considering the role of clozapine PM status should explore whether or not all cases of clozapine-induced inflammation could be explained by lack of individualized titration.
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  • 文章类型: Case Reports
    氯氮平引起的心肌炎知之甚少,罕见,潜在的致命药物不良反应,在澳大利亚,绝对风险为7至34/1000,在其他国家为0.07-0.6/1000。已经推测超敏反应,包括一些可能与快速滴定有关的病例。这个案例描述了一个50岁的非洲裔美国人患有分裂情感障碍,天真的氯氮平,可能死于氯氮平诱发的心肌炎.他开始服用25毫克/天的氯氮平,并在14天内接受1625毫克,在他15天去世之前.尸检发现主要是血管周围软组织和心室心肌的淋巴细胞浸润,偶尔伴有嗜酸性粒细胞。使用利物浦ADR因果关系评估工具,据认为,患者的死亡可能是继发于心肌炎。患者暴发性死亡,生命体征无明显变化。既不测量C反应蛋白也不测量肌钙蛋白,但它是不可能的结果会及时到达,以防止病人的死亡。年龄,快速滴定,同时使用丙戊酸盐导致了这种情况,这可能是与快速滴定相关的特殊不良反应。拉莫三嗪诱导的Stevens-Johnson综合征似乎也是一种与快速滴定相关的特异性药物不良反应。但自拉莫三嗪的推荐起始剂量减少并通过丙戊酸盐等抑制剂的作用得到纠正后,其发病率已显著降低.同样,氯氮平诱导的心肌炎发病率可能可以通过使用慢滴定降低,包括代谢氯氮平能力较低的患者的滴定速度甚至更慢,比如那些服用丙戊酸盐的人。
    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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