DuMouchel William, Smith Eric T, Beasley Richard, Nelson Harold, Yang Xionghu, Fram David, Almenoff June S
AT&T Labs-Research, Florham Park, New Jersey, USA.
Clin Ther. 2004 Jul;26(7):1092-1104. doi: 10.1016/s0149-2918(04)90181-6.
Churg-Strauss syndrome (CSS), also known as allergic granulomatous angiitis (AGA), is a rare vasculitis that occurs in patients with bronchial asthma. The nature of the association of CSS with various asthma therapies is unclear.
This study investigated the associations of different multidrug asthma therapy regimens and the reporting of AGA (the preferred code for CSS in the coding dictionary for the Adverse Event Reporting System [AERS]) by applying an iterative method of disproportionally analysis to th AERS database maintained by the US Food and Drug Administration.
The public-release version of the AERS database was used to identify reports of AGA in patients receiving asthma therapy. Reporting of AGA was examined using iterative disproportionality methods in patients receiving > or =1 of the following drug classes: inhaled corticosteroid (ICS), leukotriene receptor antagonist (LTRA), short-acting beta(2)-agonist (SABA), or long-acting beta(2)-agonist (LABA). The Bayesian data-mining algorithm known as the multi-item gamma poisson shrinker was used to determine the relative reporting rates by calculation of the empirical Bayes geometric mean (EBGM) and its 90% CI (EB05 = lower limit and EB95 = upper limit) for each drug. Subset analyses were performed for each drug with different medication combinations to differentiate the relative reporting of AGA for each.
A strong association was found between LTRA use and AGA (EBGM = 104.0, EB05 = 95.0, EB95 = 113.8) that persisted with all combinations of therapy studied. AGA was also associated with the ICS, SABA and LABA classes (EBGM values of 27.8, 14.6 and 40.4, respectively). However, the latter associations were mostly dependent on the presence of concurrent LTRA and, to a lesser extemt, oral corticosteroid therapy and became negligible (ie, EB05 < 2) for patients who were not receiving these concurrent treatments.
Differences based on relative reporting were observed in the patterns of association of AGA with LTRA, ICS, and beta(2)-agonist therapies. A strong association between LTRA use and AGA was present regardless of the use of other asthma drugs.
变应性肉芽肿性血管炎(CSS),又称过敏性肉芽肿性血管炎(AGA),是一种发生于支气管哮喘患者的罕见血管炎。CSS与各种哮喘治疗方法之间关联的性质尚不清楚。
本研究通过对美国食品药品监督管理局维护的不良事件报告系统(AERS)数据库应用迭代不成比例分析方法,调查不同的多药哮喘治疗方案与AGA报告(AERS编码字典中CSS的首选编码)之间的关联。
使用AERS数据库的公开发布版本来识别接受哮喘治疗患者的AGA报告。在接受以下至少一种药物治疗的患者中,使用迭代不成比例方法检查AGA报告情况:吸入性糖皮质激素(ICS)、白三烯受体拮抗剂(LTRA)、短效β₂受体激动剂(SABA)或长效β₂受体激动剂(LABA)。使用称为多项目伽马泊松收缩器的贝叶斯数据挖掘算法,通过计算每种药物的经验贝叶斯几何均值(EBGM)及其90%可信区间(EB05 =下限,EB95 =上限)来确定相对报告率。对每种药物进行不同药物组合的亚组分析,以区分每种药物的AGA相对报告情况。
发现使用LTRA与AGA之间存在强关联(EBGM = 104.0,EB05 = 95.0,EB95 = 113.8),在所研究的所有治疗组合中均持续存在。AGA也与ICS、SABA和LABA类别相关(EBGM值分别为27.8、14.6和40.4)。然而,后一种关联大多取决于同时使用LTRA,在较小程度上还取决于口服糖皮质激素治疗,对于未接受这些同时治疗的患者,这种关联可忽略不计(即EB05 < 2)。
观察到AGA与LTRA、ICS和β₂受体激动剂治疗之间的关联模式存在基于相对报告的差异。无论是否使用其他哮喘药物,使用LTRA与AGA之间均存在强关联。
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