首页> 外文期刊>Drug safety: An international journal of medical toxicology and drug experience >Domperidone and ventricular arrhythmia or sudden cardiac death: a population-based case-control study in the Netherlands.
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Domperidone and ventricular arrhythmia or sudden cardiac death: a population-based case-control study in the Netherlands.

机译:多潘立酮和室性心律失常或心源性猝死:荷兰一项基于人群的病例对照研究。

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BACKGROUND: Recently, a 4-fold increase in risk of sudden cardiac death (SCD) was reported for domperidone in a study that focused on corrected QT interval (QTc)-prolonging drugs as a class and their association with SCD. OBJECTIVE: To evaluate the association between the use of domperidone and serious non-fatal ventricular arrhythmia (VA) and SCD in the general population. METHODS: We performed a population-based, case-control study during 1996-2007 in the Integrated Primary Care Information (IPCI) database, a longitudinal general practice research database in the Netherlands. We included all patients aged >/=18 years without cancer in the source population. We studied the association between the use of domperidone by recency of use (current, past and none) and daily dose, and the risk of serious non-fatal VA or SCD. Cases were defined as a natural death due to cardiac causes heralded by abrupt loss of consciousness within 1 hour after the onset of acute symptoms or an unwitnessed, unexpected death of someone seen in a stable medical condition <24 hours previously with no evidence of a non-cardiac cause. Controls were randomly drawn from the source population and matched to cases on age, sex, practice and index date. We compared the exposure odds for SCD alone and VA plus SCD by means of conditional logistic regression while adjusting for all available confounders. In addition, we stratified by insurance type. RESULTS: The study population comprised 1366 cases (62 VA and 1304 SCD) and 14114 matched controls. Of all cases, ten patients were current domperidone users at the index date, all with SCD. The matched unadjusted odds ratio of domperidone and SCD was 3.72 (95% CI 1.72, 8.08). Daily doses >30 mg were associated with a significant increased risk of SCD (adjusted odds ratio [OR(adj)] 11.4 [95% CI 1.99, 65.2]). Since there was a near interaction with health insurance (p = 0.050), all analyses were stratified by insurance. In publicly insured patients, seven cases were current users at the index date. Current use was associated with a significant increased risk of SCD (OR(adj) 4.17 [95% CI 1.33, 13.1]). Amongst privately insured patients there was one domperidone-exposed case, and amongst non-insured there were two. CONCLUSIONS: Current use of domperidone, especially high doses, is associated with an increased risk of SCD. We could not demonstrate an effect of domperidone on non-fatal VA due to absence of exposed cases.
机译:背景:最近,一项针对多潘立酮的研究报告称多潘立酮的心脏猝死(SCD)风险增加了4倍,该研究集中在延长QT间期(QTc)的药物作为一类药物及其与SCD的关联上。目的:评估在一般人群中使用多潘立酮与严重非致命性室性心律失常(VA)和SCD的相关性。方法:我们在1996年至2007年间通过综合初级保健信息(IPCI)数据库进行了一项基于人群的病例对照研究,该数据库是荷兰的纵向全科医学研究数据库。我们将所有年龄≥18岁且未患癌症的患者纳入来源人群。我们研究了通过使用新药(当前,过去和无),每日剂量使用多潘立酮与严重非致命性VA或SCD风险之间的关联。病例定义为在急性症状发作后1小时内突然因意识丧失或由于目击者突然丧失意识而预示的心脏原因导致的自然死亡,该患者在稳定的医疗条件下(<24小时前)没有任何证据-心脏原因。从来源人群中随机抽取对照,并与年龄,性别,习俗和索引日期匹配。我们通过条件对数回归比较了单独使用SCD和VA加SCD的暴露几率,同时对所有可用的混杂因素进行了调整。另外,我们按保险类型进行了分层。结果:研究人群包括1366例(62 VA和1304 SCD)和14114例匹配对照。在所有病例中,有十名患者在索引日期为当前的多潘立酮使用者,均患有SCD。多潘立酮和SCD的匹配未调整优势比为3.72(95%CI 1.72,8.08)。每日剂量> 30 mg与SCD的风险显着增加相关(校正比值比[OR(adj)] 11.4 [95%CI 1.99,65.2])。由于与健康保险之间存在密切的互动(p = 0.050),因此所有分析均按保险进行了分层。在公共保险患者中,有7例是在索引日期的当前用户。当前使用与SCD风险显着增加有关(OR(adj)4.17 [95%CI 1.33,13.1])。在私人保险患者中,有1例服用多潘立酮,而在非保险患者中有2例。结论:当前使用多潘立酮,特别是大剂量使用,会增加SCD的风险。由于没有暴露病例,我们无法证明多潘立酮对非致死性VA的作用。

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