Real-world reporting rates of administration-site reactions with on-demand treatment of hereditary angioedema attacks.

IF 2.6 3区医学 Q2 ALLERGY

Allergy and asthma proceedings Pub Date : 2024-01-22 Epub Date: 2023-11-22 DOI:10.2500/aap.2024.45.230073

Raffi Tachdjian, Sinisa Savic, Moshe Fridman, Joao P Frade, Marie Fasehun, Paul K Audhya

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引用次数: 0

Abstract

Background: Hereditary angioedema (HAE) is characterized by recurrent and unpredictable episodes of subcutaneous and/or submucosal swelling. Objective: To characterize the real-world treatment burden associated with existing on-demand therapies, we analyzed administration-site adverse drug reactions (ADR) associated with approved on-demand HAE therapies reported in the U.S. Food and Drug Administration's (FDA) Adverse Event Reporting System (FAERS). Methods: We searched the FAERS database from October 1, 2009, to March 31, 2022, for reports of all FDA-approved on-demand therapies for HAE: plasma-derived C1-inhibitor (pdC1-INH), ecallantide, icatibant, and recombinant C1-inhibitor (rhC1-INH). ADRs in which the drug was listed as the "primary suspect" were recorded for each drug. ADR preferred terms were grouped into 18 ADR domains based on semantic and/or clinical similarity, and the number of reports for each drug was calculated per year from the time of approval through March 2022, and descriptive results were presented. Preferred terms associated with administration-site ADRs identified from clinical trials and denoted on approved HAE drug U.S. package inserts were examined in a complementary analysis. Results: The highest reported rates of administration-site ADRs per year were site pain (17.9 reports per year), site erythema (7.4 per year), and site swelling (6.7 per year). RhC1-INH was the only drug for which access-site complications and/or malfunctions were reported (9.5 per year). PdC1-INH had the highest rate of incorrect route of product administration (3.7 per year). PdC1-INH showed statistically significant elevated reporting rate of injection-site reactions (reporting odds ratio [ROR] 3.59 [2.36-5.46]; empirical Bayesian geometric mean [EBGM] 1.97 [1.39]). Icatibant and rhC1-INH showed a statistical trend toward an increased reporting rate of administration-site reactions. Conclusion: Real-world data from FAERS were generally consistent with adverse events reported in clinical trials and suggest that patients experience substantial treatment burden associated with FDA-approved parenteral on-demand therapies for HAE attacks. It should be noted that ADR rates are not exposure adjusted and are based on spontaneous reporting.

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按需治疗遗传性血管性水肿发作的给药部位反应的真实世界报告率。

背景:遗传性血管性水肿(HAE)以反复发作和不可预测的皮下和/或粘膜下肿胀为特征。目的:为了描述与现有按需治疗相关的现实世界治疗负担，我们分析了美国食品和药物管理局(FDA)不良事件报告系统(FAERS)中报告的与已批准的HAE按需治疗相关的给药部位药物不良反应(ADR)。方法:从2009年10月1日至2022年3月31日，我们检索了FAERS数据库中所有fda批准的HAE按需治疗的报告:血浆源性c1抑制剂(pdC1-INH)、ecallantide、icatibant和重组c1抑制剂(rhC1-INH)。将药物列为“主要嫌疑”的药物的不良反应记录下来。根据语义和/或临床相似性将ADR首选术语分为18个ADR域，从批准之日起至2022年3月，每年计算每种药物的报告数量，并给出描述性结果。在一项补充分析中，研究人员检查了与临床试验中发现的给药部位不良反应相关的首选术语，并在已批准的HAE药物美国说明书上标注。结果:每年报告的给药部位不良反应发生率最高的是部位疼痛(每年17.9例)、部位红斑(每年7.4例)和部位肿胀(每年6.7例)。RhC1-INH是唯一报告通路部位并发症和/或功能障碍的药物(每年9.5例)。PdC1-INH的给药途径错误率最高(3.7 /年)。PdC1-INH组注射部位反应报告率升高有统计学意义(报告优势比[ROR] 3.59 [2.36-5.46];经验贝叶斯几何平均[EBGM] 1.97[1.39])。伊卡替班和rhC1-INH的给药部位反应报告率呈统计学上升趋势。结论:来自FAERS的真实数据与临床试验中报告的不良事件基本一致，表明患者经历了与fda批准的针对HAE发作的静脉外按需治疗相关的巨大治疗负担。值得注意的是，不良反应发生率不是根据暴露情况调整的，而是基于自发报告。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Allergy and asthma proceedings 医学-过敏

CiteScore

5.70

自引率

35.70%

发文量

106

审稿时长

6-12 weeks

期刊介绍： Allergy & Asthma Proceedings is a peer reviewed publication dedicated to distributing timely scientific research regarding advancements in the knowledge and practice of allergy, asthma and immunology. Its primary readership consists of allergists and pulmonologists. The goal of the Proceedings is to publish articles with a predominantly clinical focus which directly impact quality of care for patients with allergic disease and asthma. Featured topics include asthma, rhinitis, sinusitis, food allergies, allergic skin diseases, diagnostic techniques, allergens, and treatment modalities. Published material includes peer-reviewed original research, clinical trials and review articles.