Onset Time Profiles for Syncope Associated with α 1 -Adrenoceptor Blockers in Males: Analysis of a Spontaneous Adverse Drug Event Database

K. Ohyama, Masaya Furumoto, M. Sugiura
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引用次数: 1

Abstract

Background: α1-Adrenoceptor blockers (α1Bs) are used for the treatment of benign prostatic hyperplasia and hypertension, but they are known to cause hypotension-related adverse events. The objective of the present study was to evaluate the onset time profiles for syncope associated with the use of α1Bs. Methods: We analyzed the data obtained from the Japanese Adverse Drug Event Report (JADER) database for a period from April 2004 until November 2016 and calculated reporting odds ratios (RORs) for eight α1Bs available on the Japanese market, using disproportionality analysis. Moreover, time information recorded in the JADER database was analyzed to evaluate the onset times of adverse events. Results: In total, 186,724 reports for males older than 20 years were analyzed. Significant RORs for syncope, with 95% confidence intervals, were obtained for naftopidil (2.53, 1.81 - 3.53), silodosin (4.24, 2.37 - 5.20), and tamsulosin (2.22, 1.75 - 2.81). The median onset times of syncope for naftopidil, silodosin, and tamsulosin were 37, 26, and 108 days, respectively. The shape parameters obtained by fitting the data for the three α1Bs to the Weibull distribution were all less than 1.0, indicating that all these drugs could be classified as the early failure type. The cumulative incidence rates showed that the onset times of syncope tended to be similar among the three α1Bs. Conclusions: Patients treated with selective α1Bs should be closely monitored for 100 days, especially in the first 20 to 40 days after initiation of silodosin or naftopidil. This information may be useful for patients and healthcare professionals in preventing syncope due to the use of selective α1Bs.
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男性与α 1 -肾上腺素受体阻滞剂相关的晕厥发病时间:自发药物不良事件数据库分析
背景:α1-肾上腺素受体阻滞剂(α 1b)被用于治疗良性前列腺增生和高血压,但已知它们会引起低血压相关的不良事件。本研究的目的是评估与α 1b使用相关的晕厥发病时间概况。方法:分析2004年4月至2016年11月日本不良药物事件报告(JADER)数据库中的数据,采用歧化分析方法计算日本市场上8种α 1b的报告优势比(RORs)。此外,还分析了记录在JADER数据库中的时间信息,以评估不良事件的发生时间。结果:共分析了186,724例20岁以上男性的报告。naftopidil(2.53, 1.81 - 3.53)、silodosin(4.24, 2.37 - 5.20)和tamsulosin(2.22, 1.75 - 2.81)对晕厥有显著的RORs(95%可信区间)。纳托地尔、西洛多辛和坦索罗辛的中位晕厥发作时间分别为37、26和108天。3种α 1b药物的数据拟合Weibull分布得到的形状参数均小于1.0,说明这3种药物均可归为早期失效型。累积发病率显示,3个α 1b组的晕厥发作次数趋于相似。结论:选择性α 1b治疗的患者应密切监测100天,特别是西洛多辛或纳托地尔开始治疗后的前20 ~ 40天。这一信息可能对患者和医疗保健专业人员预防选择性α 1b引起的晕厥有用。
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