Real-World Prevalence and Outcomes of Patients with Paroxysmal Nocturnal Hemoglobinuria Treated with C5 Inhibitors in the US: A Retrospective Claims Database Analysis.
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Abstract
Background: Paroxysmal nocturnal hemoglobinuria (PNH) is a rare blood disorder with C5 inhibitors (C5i), eculizumab and ravulizumab, being part of current treatment options.
Objectives: To estimate the 5-year prevalence of PNH and describe the healthcare resource utilization and direct healthcare costs associated with C5i among commercially insured patients with PNH treated with C5i in the US.
Methods: The 5-year prevalence of adults with PNH in IQVIA PharMetrics® Plus was estimated (2018-2022). A retrospective cohort study (2011-2022) was also conducted in adults with PNH treated with C5i and ≥3 months of continuous health plan coverage following the first claim for C5i (index date). PNH-related health resource utilization and direct healthcare costs were assessed from index date until earliest of treatment discontinuation/end of data/end of continuous health plan coverage (follow-up period).
Results: The 5-year prevalence of PNH was 2.4 per 100 000 persons in commercial claims. A total of 371 patients treated with C5i (median age: 40 years; female: 55.3%; eculizumab: 53.9%; ravulizumab: 46.1%) were followed for a mean ± SD [median] of 19.3 ± 16.9 [14.7] months. Annual incidence rates of PNH-related blood transfusion and breakthrough hemolysis (BTH) among patients treated with C5i were 1.2 (eculizumab: 1.3; ravulizumab: 1.0) and 4.5 (eculizumab: 5.2; ravulizumab: 3.3) per person per year (PPPY), respectively. In patients treated with eculizumab and ravulizumab, respectively, PNH-related blood transfusion was required by 46.2% and 11.9% of patients in the first 6 months post-index, and over the follow-up period, transfusion avoidance was observed in 46.2% and 78.2% of patients. The 6- and 12-month rates of PNH-related thrombosis were 8.0% and 10.6% for eculizumab and 6.1% and 11.6% for ravulizumab, respectively. Among patients treated with C5i, estimated annual total PNH-related costs PPPY were 697 459; ravulizumab: 633 984 (eculizumab: 570 832) for subsequent years, with treatment costs accounting for 94.3% to 94.6% of total costs.
Discussion: Despite treatment with C5i, patients with PNH still exhibited BTH, required blood transfusions, and experienced thrombosis.
Conclusion: This study highlights the unmet need for more effective PNH treatments to address the economic and clinical burden associated with PNH and improve disease control among patients.
背景:阵发性夜间血红蛋白尿(PNH)是一种罕见的血液疾病,C5抑制剂(C5i), eculizumab和ravulizumab是目前治疗方案的一部分。目的:估计5年PNH的患病率,并描述在美国商业保险的接受C5i治疗的PNH患者中与C5i相关的医疗资源利用和直接医疗费用。方法:估计IQVIA PharMetrics®Plus中成人PNH的5年患病率(2018-2022)。一项回顾性队列研究(2011-2022)也对接受C5i治疗的PNH成人患者进行了研究,该患者在首次申请C5i(索引日期)后连续健康计划覆盖≥3个月。从索引日期到最早停止治疗/数据终止/连续健康计划覆盖结束(随访期),评估了与pnh相关的卫生资源利用和直接卫生保健费用。结果:商业索赔中PNH的5年患病率为2.4 / 100,000 万人。共371例接受C5i治疗的患者(中位年龄:40岁,女性:55.3%,eculizumab: 53.9%, ravulizumab: 46.1%)被随访,平均±SD[中位数]为19.3±16.9[14.7]个月。在接受C5i治疗的患者中,pnh相关输血和突破性溶血(BTH)的年发生率分别为每人每年1.2 (eculizumab: 1.3; ravulizumab: 1.0)和4.5 (eculizumab: 5.2; ravulizumab: 3.3) (PPPY)。在分别接受eculizumab和ravulizumab治疗的患者中,46.2%和11.9%的患者在指数后的前6个月内需要与pnh相关的输血,在随访期间,46.2%和78.2%的患者观察到输血避免。eculizumab组6个月和12个月pnh相关血栓发生率分别为8.0%和10.6%,ravulizumab组为6.1%和11.6%。C5i患者中,估计每年总PNH-related成本PPPY 660 533 (e c u l z u m b: 697 459;ravulizumab: 612 522)o r t h e f ir s t y e r n d 633 984 (v eculizumab: 691 022;r u l z u m b: 570 832)随后几年,治疗成本占总成本的94.3%到94.6%。讨论:尽管使用C5i治疗,PNH患者仍然表现出BTH,需要输血,并经历血栓形成。结论:本研究强调了对更有效的PNH治疗的需求,以解决与PNH相关的经济和临床负担,并改善患者的疾病控制。
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