Hereditary angioedema C1-inhibitor replacement therapy and coexisting autoimmune disorders: findings from a claims database

H. Farkas, M. Fridman, D. Supina, J. Chiao, S. Prusty, M. Berger
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Abstract

Abstract Background: Autoimmune diseases are a leading cause of morbidity and mortality in the US (estimated prevalence: 4.5%) and often associated with dysregulation of the complement system (innate and adaptive immune response). The classic complement pathway is regulated by the C1-inhibitor (C1-INH), which binds to C1 to prevent its activation. Hereditary angioedema with C1-INH deficiency (C1-INH-HAE) may be linked to increased autoimmunity due to secondary deficiency of C1r, C1s, and other components. Aims: It was hypothesized that increased regulation of the complement system via C1-INH replacement therapy may reduce autoimmunity in patients with C1-INH-HAE. The coexisting autoimmune disease claims frequency was compared between C1-INH-HAE patients treated with plasma-derived (pd) C1-INH vs “other (non-C1-INH)” treatments. Methods: C1-INH-HAE patients were identified in the IMS Health PharMetrics Plus claims database between January 2012 and December 2015 by International Classification of Diseases 9/10 diagnosis code, and classified based on the use of pdC1-INH or “other (non-C1-INH)” treatments for HAE. Index date was the first claim for HAE treatment. For patients using pdC1-INH, the first fill was the index date, even if other HAE medications were used previously. Frequency of visit claims for autoimmune conditions was identified by diagnostic codes (primary or secondary). Mean visits per patient per year by treatment group, gender, and age (<50 vs ≥50 years) were summarized for autoimmune conditions. Results: Of 589 patients with HAE identified (69% female, 38% aged ≥50 years), 276 (729 patient-years) received pdC1-INH and 313 (860 patient-years) received “other (non-C1-INH)” treatments. In this cohort, 12.9% of patients had ≥1 visit associated with a coexisting autoimmune disorder – the most common were lupus, alopecia, rheumatoid arthritis, sicca (Sjogren) syndrome, and connective tissue disorders. The mean (95% CI) number of visits for autoimmune diagnoses per patient per year was numerically lower for patients treated with pdC1-INH compared to those receiving “other (non-C1-INH)” treatments (1.37 [0.56–2.19] vs 2.28 [0.83–3.73]). Conclusions: Based on these findings, it is concluded that treatment of C1-INH-HAE with pdC1-INH may have a positive impact on coexisting autoimmune conditions by normalizing complement. Further research is needed on this important issue. There may be implications for healthcare resource utilization among patients with HAE and coexisting autoimmune disorders.
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遗传性血管性水肿C1抑制剂替代疗法与共存的自身免疫性疾病:来自索赔数据库的发现
摘要背景:自身免疫性疾病是美国发病率和死亡率的主要原因(估计患病率:4.5%),通常与补体系统失调(先天和适应性免疫反应)有关。经典的补体途径由C1抑制剂(C1-INH)调节,该抑制剂与C1结合以阻止其激活。遗传性血管性水肿伴C1-INH缺乏(C1-INH-HAE)可能与由于C1r、C1s和其他成分的继发性缺乏而导致的自身免疫增加有关。目的:假设通过C1-INH替代疗法增加补体系统的调节可能会降低C1-INH-HAE患者的自身免疫。比较了接受血浆来源(pd)C1-INH治疗的C1-INH-HAE患者与“其他(非C1-INH)”治疗的患者之间共存的自身免疫性疾病索赔频率。方法:根据国际疾病分类9/10诊断代码,在2012年1月至2015年12月期间,在IMS Health PharMetrics Plus索赔数据库中确定C1-INH-HAE患者,并根据pdC1 INH或“其他(非C1-INH)”HAE治疗的使用情况进行分类。索引日期是HAE治疗的第一个声明。对于使用pdC1 INH的患者,即使之前使用过其他HAE药物,第一次填充也是索引日期。通过诊断代码(原发性或继发性)确定自身免疫性疾病的就诊频率。按治疗组、性别和年龄(<50岁与≥50岁)对每位患者每年的平均访视次数进行了自身免疫性疾病总结。结果:589名HAE患者(69%为女性,38%年龄≥50岁)中,276名(729名患者-年)接受了pdC1 INH治疗,313名(860名患者-岁)接受了“其他(非C1-INH)”治疗。在该队列中,12.9%的患者有≥1次就诊与共存的自身免疫性疾病相关,最常见的是狼疮、脱发、类风湿性关节炎、干燥综合征和结缔组织疾病。与接受“其他(非C1-INH)”治疗的患者相比,接受pdC1 INH治疗的患者每年每名患者的自身免疫诊断平均访视次数(95%CI)较低(1.37[0.56-2.19]vs 2.28[0.83-3.73])。结论:基于这些发现,结论是用pdC1-INH治疗C1-INH-HAE可能通过使补体正常化对共存的自身免疫性疾病具有积极影响。需要对这一重要问题进行进一步研究。这可能对HAE和共存自身免疫性疾病患者的医疗资源利用有影响。
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来源期刊
Journal of Drug Assessment
Journal of Drug Assessment PHARMACOLOGY & PHARMACY-
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