Real-World Experience of Bimekizumab in a Cohort of 109 Patients Over 48 Weeks and Identification of Predictive Factors for an Early Super Response and Risk of Adverse Events.

IF 5.2 Q1 DERMATOLOGY

Psoriasis (Auckland, N.Z.) Pub Date : 2025-04-11 eCollection Date: 2025-01-01 DOI:10.2147/PTT.S514249

Zeno Fratton, Stefano Bighetti, Luca Bettolini, Vincenzo Maione, Mariachiara Arisi, Cinzia Buligan, Giuseppe Stinco, Enzo Errichetti

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Abstract

Introduction: Psoriasis is a chronic inflammatory skin disease significantly impairing quality of life. The introduction of biologic therapies, such as bimekizumab-a monoclonal antibody targeting IL-17A and IL-17F-has revolutionized treatment outcomes. This study investigates the effectiveness of bimekizumab in a real-world setting, focusing on the predictors of Early Super Response (ESR), defined as achieving PASI 100 by week 4, and evaluates the safety profile over a 48-week follow-up period.

Methods: A retrospective study was conducted on 109 psoriasis patients treated with bimekizumab at two Italian dermatology centers. Of these, 61 patients completed a 48-weeks follow-up. Baseline clinical and demographic data, PASI scores at multiple time points, and adverse events were collected. ESR predictors were analyzed using univariate and multivariate logistic regression models. Safety was assessed using Cox proportional hazards models to find predictive factors associated with the risk of adverse events (AEs).

Results: At week 4, 28.4% of patients achieved PASI 100. Baseline PASI (OR: 0.93, p = 0.029), absence of nail involvement (OR: 0.12, p = 0.003), and fewer biologic failures (OR: 0.14, p = 0.038) were independently associated with ESR status. Safety analysis revealed that 15.6% of patients experienced adverse events, with asthma/allergic rhinitis significantly associated with a higher risk (HR: 6.43, p = 0.012). Candidiasis (7.3%) and eczema (4.6%) were the most common adverse events.

Conclusion: Bimekizumab demonstrated significant effectiveness and an acceptable safety profile in a real-world setting. Baseline PASI, nail involvement, and prior biologic failures influenced early treatment response. Identifying predictors of ESR and adverse events can guide personalized therapeutic approaches, optimizing outcomes for psoriasis patients.

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比美珠单抗在109例患者48周以上的队列中的实际应用经验，以及早期超反应和不良事件风险的预测因素的确定。

简介：银屑病是一种慢性炎症性皮肤病，严重影响生活质量。生物疗法的引入，如bimekizumab（一种靶向IL-17A和il - 17f的单克隆抗体）已经彻底改变了治疗结果。本研究调查了比美珠单抗在现实世界中的有效性，重点关注早期超级反应（ESR）的预测因素，定义为在第4周达到PASI 100，并在48周的随访期间评估安全性。方法：对意大利两家皮肤病中心接受比美珠单抗治疗的109例银屑病患者进行回顾性研究。其中，61名患者完成了48周的随访。收集基线临床和人口统计数据、多个时间点的PASI评分和不良事件。采用单因素和多因素logistic回归模型分析ESR预测因子。使用Cox比例风险模型评估安全性，以寻找与不良事件（ae）风险相关的预测因素。结果：第4周，28.4%的患者达到PASI 100。基线PASI （OR: 0.93, p = 0.029）、没有指甲受累（OR: 0.12, p = 0.003）和较少的生物失败（OR: 0.14, p = 0.038）与ESR状态独立相关。安全性分析显示，15.6%的患者出现不良事件，其中哮喘/变应性鼻炎的风险较高（HR: 6.43, p = 0.012）。念珠菌病（7.3%）和湿疹（4.6%）是最常见的不良事件。结论：Bimekizumab在现实世界中显示出显著的有效性和可接受的安全性。基线PASI，指甲受累和先前的生物学失败影响早期治疗反应。确定ESR和不良事件的预测因子可以指导个体化治疗方法，优化银屑病患者的预后。

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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Psoriasis (Auckland, N.Z.)

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审稿时长

16 weeks