Clozapine/adverse effects

氯氮平 / 不良反应
  • 文章类型: Journal Article
    文献将氯氮平与肺炎/吸入性肺炎相关联。
    国际药物警戒数据库(VigiBase™)使用信息成分(IC)作为统计信号。分析了从介绍到2023年5月10日的肺炎/吸入性肺炎的VigiBase氯氮平报告。
    有6392例所有类型的肺炎(5572例肺炎,775例吸入性肺炎,和45合并)。吸入性肺炎的IC为3.52,2003年作为VigiBase标签推出,肺炎为1.91。患者被重新分类为3628,无误吸迹象,1533有迹象。误吸的迹象与一些共同用药密切相关:奥氮平,优势比(OR)=23.8,95%置信区间(CI),14.9-38.0;利培酮OR=18.6,CI,11.4-30.4;丙戊酸,OR=5.5,CI,4.5-6.6;苯二氮卓类药物OR=5.5,CI,4.5-6.6。在2415个数据完整的案例中,致命性结局占45%(误吸迹象没有区别),但是差异很大,从0%(女性<45岁;持续时间≤30天)到76%(男性>64岁;持续时间>1年)。在第一周,肺炎与:1)非常高的滴定剂量有关,2)帕金森氏病的小剂量和3)日本与其他国家。
    在氯氮平治疗的患者中:1)至少30%的肺炎病例可能是吸入性肺炎,2)停止一些联合用药可能会降低吸入性肺炎的风险,3)肺炎的平均致死率为45%,但在长期治疗的老年患者中可能约为75%,和4)更安全的滴定有时可能需要5-mg片剂。
    UNASSIGNED: The literature associates clozapine with pneumonia/aspiration pneumonia.
    UNASSIGNED: The international pharmacovigilance database (VigiBase™) uses the information component (IC) as statistical signal. VigiBase clozapine reports were analyzed for pneumonia/aspiration pneumonia from introduction to 10 May 2023.
    UNASSIGNED: There were 6392 cases of all types of pneumonia (5572 cases of pneumonia, 775 of aspiration pneumonia, and 45 combined). The IC was 3.52 for aspiration pneumonia, introduced as a VigiBase label in 2003, and 1.91 for pneumonia. Patients were reclassified as 3628 with no signs of aspiration and 1533 with signs. Signs of aspiration were strongly associated with some co-medications: olanzapine, odds ratio (OR) = 23.8, 95% confidence interval (CI), 14.9-38.0; risperidone OR = 18.6, CI, 11.4-30.4; valproic acid, OR = 5.5, CI, 4.5-6.6; and benzodiazepines OR = 5.5, CI, 4.5-6.6. In 2415 cases with completed data, fatal outcomes made up 45% (signs of aspiration made no difference), but there was wide variability from 0% (females <45 years of age; duration ≤30 days) to 76% (males >64 years of age; duration >1 year). During the first week, pneumonia was associated with 1) very high titration doses, 2) very small doses in Parkinson\'s disease, and 3) Japan vs other countries.
    UNASSIGNED: In clozapine-treated patients: 1) at least 30% of pneumonia cases may be aspiration pneumonia, 2) stopping some co-medications may decrease the risk of aspiration pneumonia, 3) average lethality in pneumonia was 45% but may be around 75% in geriatric patients with long-term treatment, and 4) safer titrations may sometimes require 5-mg tablets.
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  • 文章类型: Journal Article
    氯氮平于1976年在中国首次生产。氯氮平目前不仅用于治疗难治性精神分裂症(TRS),但也继续用于治疗非TRS和其他精神障碍患者;此外,低剂量氯氮平也用于镇静催眠治疗以及与其他药物联合使用。在中国,有必要使用各种滴定法进行研究,并评估其心肌炎和吸入性肺炎的风险。中国氯氮平包装说明书也将大大受益于这些变化。
    Clozapine was first manufactured in China in 1976. Clozapine is currently used not only for treatment-refractory schizophrenia (TRS), but also continues to be used in the treatment of patients with non-TRS and other mental disorders; moreover, low-dose clozapine is also used in sedative-hypnotic therapy and in combination with other drugs. There is need for studies in China using various titrations and assessing their risk for myocarditis and aspiration pneumonia. The Chinese clozapine package insert will also greatly benefit from these changes.
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  • DOI:
    文章类型: Case Reports
    目标:最近的一项国际指南通过考虑以下因素,为成人住院患者中滴定氯氮平提供了某些个性化的时间表:1)DNA祖先组,2)性吸烟亚组,和3)存在/不存在氯氮平不良代谢(PM)状态。建议在基线和前4周内测量CRP水平。对于特定患者的代谢而言,滴定过快会导致氯氮平诱导的炎症和CRP升高。方法:重新解释3例已发表的病例。使用该指南可能会获得更好的结果。结果:病例1为中国男性非吸烟者,由于潜在的炎症导致的氯氮平PM。病例2是一名土耳其女性非吸烟者,在4个危险因素(未诊断的炎症,肥胖,丙戊酸盐和奥氮平联合处方)。病例3是一名欧洲血统的美国患者,没有已知的危险因素,在常规滴定后发展为心肌炎,并以12.5mg/天的剂量失败。国际氯氮平滴定指南的应用可能已经预防:1)病例1通过建议CRP水平异常的患者不使用氯氮平滴定,2)案例2,通过考虑4个危险因素并使用氯氮平PM的缓慢滴定,和3)案例3通过使用CRP升高早期识别可能的遗传性PM。结论:当基线或之前的CRP正常,然后在氯氮平滴定过程中变得异常时,这表明:1)氯氮平诱导的炎症与该特定患者的滴定过快有关,和/或2)感染的共同发生。前瞻性研究需要验证这一假设。
    Objectives: An international guideline recently provided certain personalized schedules for titrating clozapine in adult inpatients by considering: 1) DNA ancestry group, 2) sexsmoking subgroup, and 3) presence/absence of clozapine poor metabolizer (PM) status. Measuring CRP levels at baseline and during the first 4 weeks is recommended. Titrations too fast for the metabolism of specific patients can lead to clozapine-induced inflammations and CRP elevations. Methods: Three published cases are reinterpreted. Better outcomes might have been obtained by using the guideline. Results: Case 1 was a Chinese male non-smoker, a clozapine PM due to an underlying inflammation. Case 2 was a Turkish female non-smoker who developed clozapine-induced myocarditis in the context of 4 risk factors (undiagnosed infl ammation, obesity, valproate and olanzapine co-prescription). Case 3 was a United States patient of European ancestry with no known risk factors who developed myocarditis after a routine titration and had an unsuccessful rechallenge with 12.5 mg/day. Application of the international clozapine titration guideline may have prevented: 1) Case 1 by recommending against clozapine titration for a patient with an abnormal CRP level, 2) Case 2 by considering 4 risk factors and using a slow titration for clozapine PMs, and 3) Case 3 by using CRP elevations for early identification of a possible genetic PM. Conclusions: When baseline or prior CRPs are normal and then become abnormal during a clozapine titration, this indicates: 1) clozapine-induced inflammation associated with too-rapid titration for that specific patient, and/or 2) co-occurrence of an infection. Prospective studies need to verify this hypothesis.
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  • 文章类型: Systematic Review
    UNASSIGNED:从PubMed搜索(2022年7月18日)(9例)和世界卫生组织的药物警戒数据库中研究了氯氮平诱发的儿童心肌炎(年龄≤18岁)。叫做Vigibase,药物不良反应(ADR)报告(72例非重复病例)。Vigibase使用称为信息分量(IC)的不成比例性的对数度量。建立了VigiBase中严重性存在/不存在(40/32)的逻辑回归模型。
    UNASSIGNED:VigiBase提供了显著的心肌炎IC=4.2,IC025=3.8;预计只有4例氯氮平诱发的心肌炎病例,而观察到72例。PubMed搜索确定了9例,而VigiBase确定了72例(其中67例与已发布的病例不重叠)。这76例合并病例包括35例可疑(大多数在诊断当天缺少信息),19种可能和22种可能,根据ADR量表。在调整了混杂因素后,喹硫平以17.6的比值比(OR)(95%置信区间CI,1.56~198.6)增加严重性风险,而澳大利亚裔以0.13(CI,0.04~0.47)降低严重性风险。
    UASSIGNED:这41例至少可能的氯氮平诱发的心肌炎病例表明,这种ADR可以明确发生在儿童身上,特别是在向上滴定的前30天。儿童和成人病例出现相似。
    UNASSIGNED: Clozapine-induced myocarditis in children (age ≤18 yo) was studied from a PubMed search (18 July 2022) (9 cases) and from the World Health Organization\'s pharmacovigilance database, called Vigibase, of adverse drug reaction (ADR) reports (72 non-duplicated cases). VigiBase uses a logarithmic measure of disproportionality called the information component (IC). A logistic regression model of presence/absence (40/32) of seriousness in VigiBase was developed.
    UNASSIGNED: VigiBase provided a significant myocarditis IC = 4.2 with an IC025 = 3.8; only 4 clozapine-induced myocarditis cases were expected, while 72 were observed. The PubMed search identified 9 cases, while VigiBase identified 72 cases (of which 67 did not overlap with published cases). These 76 combined cases included 35 doubtful (most with missing information on the day of diagnosis), 19 possible and 22 probable, according to the ADR scale. After adjusting for confounders, quetiapine increased the risk of seriousness with an odds ratio (OR) of 17.6 (95% confidence interval CI, 1.56 to 198.6), while Australian origin decreased it with an OR = 0.13 (CI, 0.04 to 0.47).
    UNASSIGNED: These 41 cases of at least possible clozapine-induced myocarditis indicated that this ADR can definitively occur in children, particularly in the first 30 days of up-titration. Children\'s and adult cases appeared similar.
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  • 文章类型: Journal Article
    背景:氯氮平相关性心肌炎的发病率因国家而异。这些变化在VigiBase中进行了探索,世界卫生组织的全球数据库有超过2500万份自发报告的药物不良反应(ADR)来自145个国家药品机构。
    方法:2021年1月15日,自成立以来,对VigiBase的搜索集中在氯氮平患者的心肌炎。使用称为信息分量(IC)的标准VigiBase对数不相称性度量对3572份单独报告进行了研究。IC衡量的是预期利率和报告利率之间的不相称性。消除重复项后,在逻辑回归模型中研究了3274名不同的心肌炎患者。
    结果:第一例发表于1980年,但自1993年以来,VigiBase氯氮平-心肌炎IC已成为重要的病例;此外,目前它非常强(IC=6.0,IC005-IC995=5.9-6.1),与其他抗精神病药物有统计学差异.在3274名不同的心肌炎患者中,43.4%为非严重病例,51.8%为严重但非致命性,4.8%是致命的。超过一半(1621/3274)的报告来自澳大利亚,其中69.2%为非严重,27.7%严重但非致命,3.1%致命。亚洲国家仅提供了41例病例。
    结论:在药物警戒研究中,混杂因素可以解释统计关联,但这些结果的强度和稳健性与心肌炎与早期氯氮平治疗明确相关的假设一致(第1个月和第2个月分别为84%[1309/1560]和5%[82/1560]).来自澳大利亚的心肌炎报告在很大程度上代表过多。亚洲国家可能向其药物机构漏报心肌炎。
    BACKGROUND: The incidence of clozapine-associated myocarditis varies by country. These variations were explored in VigiBase, the World Health Organization\'s global database which has >25 million spontaneously reported adverse drug reaction (ADR) reports from 145 national drug agencies.
    METHODS: On January 15, 2021, a search of VigiBase since inception focused on myocarditis in clozapine patients. The 3572 individual reports were studied using the standard VigiBase logarithmic measure of disproportionality called information component (IC). The IC measures the disproportionality between the expected and the reported rates. After duplicates were eliminated there were 3274 different patients with myocarditis studied in logistic regression models.
    RESULTS: The first case was published in 1980 but since 1993 the VigiBase clozapine-myocarditis IC has been significant; moreover, currently it is very strong (IC=6.0, IC005-IC995=5.9-6.1) and statistically significantly different from other antipsychotics. Of the 3274 different patients with myocarditis, 43.4% were non-serious cases, 51.8% were serious but non-fatal, and 4.8% were fatal. More than half (1621/3274) of the reports came from Australia, of which 69.2% were non-serious, 27.7% serious but non-fatal, and 3.1% fatal. Asian countries contributed only 41 cases.
    CONCLUSIONS: In pharmacovigilance studies, confounding factors may explain statistical associations, but the strength and robustness of these results are compatible with the hypothesis that myocarditis is definitively associated with early clozapine treatment (84% [1309/1560] and 5% [82/1560] in the first and second months). Myocarditis reports from Australia are over-represented to a major degree. Asian countries may be underreporting myocarditis to their drug agencies.
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  • 文章类型: Journal Article
    背景:氯氮平相关性心肌炎的发病率因国家而异。这些变化在VigiBase中进行了探索,世界卫生组织的全球数据库有超过2500万份自发报告的药物不良反应(ADR)来自145个国家药品机构。
    方法:2021年1月15日,自成立以来,对VigiBase的搜索集中在氯氮平患者的心肌炎。使用称为信息分量(IC)的标准VigiBase对数不相称性度量对3572份单独报告进行了研究。IC衡量的是预期利率和报告利率之间的不相称性。消除重复项后,在逻辑回归模型中研究了3274名不同的心肌炎患者。
    结果:第一例发表于1980年,但自1993年以来,VigiBase氯氮平-心肌炎IC已成为重要的病例;此外,目前它非常强(IC=6.0,IC005-IC995=5.9-6.1),与其他抗精神病药物有统计学差异.在3274名不同的心肌炎患者中,43.4%为非严重病例,51.8%为严重但非致命性,4.8%是致命的。超过一半(1621/3274)的报告来自澳大利亚,其中69.2%为非严重,27.7%严重但非致命,3.1%致命。亚洲国家仅提供了41例病例。
    结论:在药物警戒研究中,混杂因素可以解释统计关联,但这些结果的强度和稳健性与心肌炎与早期氯氮平治疗明确相关的假设一致(第1个月和第2个月分别为84%[1309/1560]和5%[82/1560]).来自澳大利亚的心肌炎报告在很大程度上代表过多。亚洲国家可能向其药物机构漏报心肌炎。
    BACKGROUND: The incidence of clozapine-associated myocarditis varies by country. These variations were explored in VigiBase, the World Health Organization\'s global database which has >25 million spontaneously reported adverse drug reaction (ADR) reports from 145 national drug agencies.
    METHODS: On January 15, 2021, a search of VigiBase since inception focused on myocarditis in clozapine patients. The 3572 individual reports were studied using the standard VigiBase logarithmic measure of disproportionality called information component (IC). The IC measures the disproportionality between the expected and the reported rates. After duplicates were eliminated there were 3274 different patients with myocarditis studied in logistic regression models.
    RESULTS: The first case was published in 1980 but since 1993 the VigiBase clozapine-myocarditis IC has been significant; moreover, currently it is very strong (IC=6.0, IC005-IC995=5.9-6.1) and statistically significantly different from other antipsychotics. Of the 3274 different patients with myocarditis, 43.4% were non-serious cases, 51.8% were serious but non-fatal, and 4.8% were fatal. More than half (1621/3274) of the reports came from Australia, of which 69.2% were non-serious, 27.7% serious but non-fatal, and 3.1% fatal. Asian countries contributed only 41 cases.
    CONCLUSIONS: In pharmacovigilance studies, confounding factors may explain statistical associations, but the strength and robustness of these results are compatible with the hypothesis that myocarditis is definitively associated with early clozapine treatment (84% [1309/1560] and 5% [82/1560] in the first and second months). Myocarditis reports from Australia are over-represented to a major degree. Asian countries may be underreporting myocarditis to their drug agencies.
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  • 文章类型: Editorial
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  • 文章类型: Journal Article
    利用理查森和戴维森的模型以及药代动力学和临床药物心理学科学,本文综述了:(1)与难治性精神分裂症(TRS)相关的预期寿命差,坚持使用氯氮平的患者可能会有所改善;(2)发现氯氮平是TRS的最佳治疗方法(根据疗效,有效性和幸福感);和(3)氯氮平可能导致漏洞,包括可能致命的药物不良反应,如粒细胞缺乏症,肺炎,和心肌炎.合理使用要求:(1)在全球范围内修改氯氮平包装说明书,以减少亚洲人的剂量,并避免与肺炎相关的致死性,(2)使用氯氮平水平进行个性化给药,(3)使用缓慢和个性化滴定。这可能使氯氮平尽可能安全,并有助于增加预期寿命和福祉。在氯氮平患者缺乏COVID-19数据的情况下,氯氮平可能损害免疫机制,并可能增加感染患者的肺炎风险。精神科医生应该打电话给他们的氯氮平患者和家属,并向他们解释,如果患者出现发烧或流感样症状,应该召集精神科医生,并考虑将氯氮平剂量减半。如果病人因肺炎住院,治疗医师需要评估氯氮平中毒的症状,因为对所有患者来说,将剂量减半可能是不够的;考虑将其减少至1/3,甚至停用.一旦炎症和发烧的迹象消失,氯氮平剂量可以缓慢增加到之前的剂量水平。
    Using Richardson and Davidson\'s model and the sciences of pharmacokinetics and clinical pharmacopsychology, this article reviewed the: (1) poor life expectancy associated with treatment-resistant schizophrenia (TRS), which may be improved in patients who adhere to clozapine; (2) findings that clozapine is the best treatment for TRS (according to efficacy, effectiveness and well-being); and (3) potential for clozapine to cause vulnerabilities, including potentially lethal adverse drug reactions such as agranulocytosis, pneumonia, and myocarditis. Rational use requires: (1) modification of the clozapine package insert worldwide to include lower doses for Asians and to avoid the lethality associated with pneumonia, (2) the use of clozapine levels for personalizing dosing, and (3) the use of slow and personalized titration. This may make clozapine as safe as possible and contribute to increased life expectancy and well-being. In the absence of data on COVID-19 in clozapine patients, clozapine possibly impairs immunological mechanisms and may increase pneumonia risk in infected patients. Psychiatrists should call their clozapine patients and families and explain to them that if the patient develops fever or flu-like symptoms, the psychiatrist should be called and should consider halving the clozapine dose. If the patient is hospitalized with pneumonia, the treating physician needs to assess for symptoms of clozapine intoxication since halving the dose may not be enough for all patients; consider decreasing it to one-third or even stopping it. Once the signs of inflammation and fever have disappeared, the clozapine dose can be slowly increased to the prior dosage level.
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