抗肿瘤坏死因子生物类似药治疗小儿和老年人群银屑病的有效性和安全性:一项为期72周的现实研究

IF 5.2 Q1 DERMATOLOGY Psoriasis (Auckland, N.Z.) Pub Date : 2022-07-09 eCollection Date: 2022-01-01 DOI:10.2147/PTT.S365493
Matteo Megna, Luigi Fornaro, Luca Potestio, Maria Antonietta Luciano, Mariateresa Nocerino, Mario Delfino, Maria Guarino, Gabriella Fabbrocini, Elisa Camela
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引用次数: 8

摘要

目的:确定阿达木单抗(ADA)和依那西普(ETA)生物类似药治疗老年和儿童牛皮癣的疗效和安全性。方法:采用现实生活中的回顾性观察研究方法,对小儿牛皮癣患者进行研究。结果:共纳入11例儿童和23例老年牛皮癣患者。在儿童中,6例(54.5%)使用ADA生物仿制药,5例(45.5%)使用ETA生物仿制药。ETA和ADA生物仿制药在长达72周的时间内同样有效和安全(平均PASI和BSA < 3)。没有明显的ae报告,也没有人停止治疗。老年患者中,ADA生物类似药15例(65.2%),ETA生物类似药8例(34.8%)。ETA和ADA生物仿制药在72周内同样有效(平均PASI < 4,平均BSA < 5%)。9例(39.1%)出现不良反应(以轻度为主)。此外,4名(17.4%)患者因继发性疗效不足(3.75%)或不良反应(1.25%)而停用生物制剂。结论:我们的研究发现ADA和ETA生物仿制药治疗儿童和老年人中重度牛皮癣是有效和安全的。在儿童和老年人中,ADA和ETA生物类似药的疗效和安全性没有统计学上的显著差异。即使没有接近统计学意义,老年患者的停药率和副作用也比儿科患者高。
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Efficacy and Safety of Anti-TNF Biosimilars for Psoriasis in Pediatric and Geriatric Populations: A 72-Week Real-Life Study.

Purpose: To determine the efficacy and safety of adalimumab (ADA) and etanercept (ETA) biosimilars in elderly and children with psoriasis.

Methods: A real-life retrospective observational study was conducted on pediatric (<18 years) and geriatric (≥65 years) psoriasis patients treated with anti-TNF biosimilar agents referring to the Psoriasis Unit of the University of Naples Federico II, Italy, from January 2018 to January 2022. At baseline, demographic characteristics (age and sex), data on psoriasis duration and severity (measured by Psoriasis Area Severity Index [PASI] and body surface area [BSA]), presence of psoriatic arthritis if applicable, comorbidities, and previous psoriasis treatments were recorded. Patients were monitored by regular follow-ups (week 12, 24, 48 and 72) through clinical and haematological assessments and adverse events (AEs) were registered.

Results: A total of 11 children and 23 elderly psoriasis patients were enrolled. Concerning children, 6 (54.5%) were under ADA biosimilar and 5 (45.5%) under ETA biosimilar. ETA and ADA biosimilars were equally effective and safe for up to 72 weeks (mean PASI and BSA < 3). No significant AEs were reported, and none discontinued treatment. In the elderly, 15 (65.2%) were treated with ADA biosimilar and 8 (34.8%) with ETA biosimilar. ETA and ADA biosimilars were equally effective up to 72 weeks (mean PASI < 4 and mean BSA < 5%). AEs (mainly mild) were registered in 9 subjects (39.1%). Also, 4 (17.4%) patients discontinued biologicals for secondary lack of efficacy (3, 75%) or AEs (1, 25%).

Conclusion: Our study found that ADA and ETA biosimilars are effective and safe for the treatment of moderate-to-severe psoriasis in children and the elderly. No statistically significant efficacy and safety differences were found between ADA and ETA biosimilars in both children and the elderly. Geriatric patients displayed a higher discontinuation rate and side effects than the pediatric counterpart even if without approaching statistical significance.

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