Comparison of Drug-Free Remission after the End of Phase III Trials of Three Different Anti-IL-23 Inhibitors in Psoriasis.

IF 3.5 3区 医学 Q1 DERMATOLOGY
Dermatology and Therapy Pub Date : 2024-09-01 Epub Date: 2024-07-29 DOI:10.1007/s13555-024-01229-6
Chang-Yu Hsieh, Francis Li-Tien Hsu, Tsen-Fang Tsai
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引用次数: 0

Abstract

Introduction: Knowing the remission duration after biologics discontinuation in patients with psoriasis is important, especially when disease relapse is defined as the restart of systemic agents, because it also reflects the real-world clinical practice when topical treatment alone is not adequate for disease control, and a systemic treatment, including biologic, is needed. Biologics are currently indicated for patients with psoriasis who are candidates for systemic treatments.

Methods: We included 42 patients who were followed up with regularly after the end of risankizumab, guselkumab and mirikizumab trials and investigated the drug-free remission (DFR). A Kaplan-Meier survival analysis and Cox regression model were employed to identify the possible risk factors for relapse.

Results: Overall, 38/42 (90.5%) patients experienced relapses after discontinuing trial biologics during the follow-up period of at least 96 weeks and up to 227 weeks. In all patients with relapse, the median DFR was 104 days. Kaplan-Meier survival analysis revealed a significant 1-year drug-free survival (DFS) difference between risankizumab (Z) and guselkumab (T) + mirikizumab (M) (p = 0.0462). A difference in DFS curves was noted when patients were categorized by disease duration > or ≤ 2 years (p = 0.1577) and maintenance of a psoriasis area and severity index score (PASI) of 90 at the end of trials (p = 0.1177). Univariate Cox regression model identified that age [hazard ratio (HR) = 1.030 (1.000-1.060), p = 0.0467] and disease duration [HR = 1.046(1.009-1.084), p = 0.0134] were significantly associated with relapse risk. A risk model was established on the basis of multivariable Cox regression results. Risk value = 0.021038 * Age + 0.515628 * Biologic_type (Z = 0,T/M = 1) + 0.025048 * Disease_Duration. The validated patients were divided into two groups by median risk value (1.5). The high-risk group (risk value > 1.5) had a non-significant higher relapse risk than the low-risk group (risk value < 1.5), with a hazard ratio of 1.62 [95% confidence interval (CI) = 0.82-3.23, p = 0.1809].

Conclusion: Types of biologics used, disease duration > or ≤ 2 years, and PASI 90 improvement at the end of trial affect the 1-year DFS after biologics discontinuation. Further studies consisting of a larger patient number and longer follow-up period are needed to verify our findings.

Trial registration: ClinicalTrials.gov identifiers NCT02694523, NCT03047395, NCT02207224, NCT02576431, NCT03482011, and NCT03556202.

Abstract Image

三种不同的银屑病抗IL-23抑制剂III期试验结束后的无药缓解率比较。
简介:了解银屑病患者停用生物制剂后的缓解持续时间非常重要,尤其是当疾病复发被定义为重新开始使用系统药物时,因为这也反映了现实世界中的临床实践,即当单纯的局部治疗不足以控制疾病,而需要包括生物制剂在内的系统治疗时。生物制剂目前适用于可接受系统治疗的银屑病患者:方法:我们纳入了在利桑珠单抗、古谢库单抗和米利珠单抗试验结束后定期随访的42名患者,并对无药缓解率(DFR)进行了调查。采用卡普兰-梅耶生存分析和考克斯回归模型确定复发的可能风险因素:总的来说,38/42(90.5%)名患者在至少 96 周至 227 周的随访期间停用试验生物制剂后复发。所有复发患者的中位DFR为104天。Kaplan-Meier生存分析显示,利桑珠单抗(Z)与古谢库单抗(T)+米利珠单抗(M)的1年无药生存期(DFS)差异显著(p = 0.0462)。如果按病程大于或小于 2 年(p = 0.1577)和试验结束时银屑病面积和严重程度指数(PASI)维持在 90 分(p = 0.1177)对患者进行分类,则 DFS 曲线存在差异。单变量 Cox 回归模型发现,年龄[危险比 (HR) = 1.030 (1.000-1.060),p = 0.0467]和病程[HR = 1.046(1.009-1.084),p = 0.0134]与复发风险显著相关。根据多变量考克斯回归结果建立了一个风险模型。风险值 = 0.021038 * 年龄 + 0.515628 * 生物类型(Z = 0,T/M = 1) + 0.025048 * 病程。根据中位风险值(1.5)将验证患者分为两组。高风险组(风险值大于 1.5)的复发风险明显高于低风险组(风险值等于 1.5):使用的生物制剂类型、病程大于或小于 2 年以及试验结束时 PASI 90 的改善程度都会影响停用生物制剂后的 1 年 DFS。要验证我们的研究结果,还需要更多患者和更长随访时间的进一步研究:试验注册:ClinicalTrials.gov标识符NCT02694523、NCT03047395、NCT02207224、NCT02576431、NCT03482011和NCT03556202。
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来源期刊
Dermatology and Therapy
Dermatology and Therapy Medicine-Dermatology
CiteScore
6.00
自引率
8.80%
发文量
187
审稿时长
6 weeks
期刊介绍: Dermatology and Therapy is an international, open access, peer-reviewed, rapid publication journal (peer review in 2 weeks, published 3–4 weeks from acceptance). The journal is dedicated to the publication of high-quality clinical (all phases), observational, real-world, and health outcomes research around the discovery, development, and use of dermatological therapies. Studies relating to diagnosis, pharmacoeconomics, public health and epidemiology, quality of life, and patient care, management, and education are also encouraged. Areas of focus include, but are not limited to all clinical aspects of dermatology, such as skin pharmacology; skin development and aging; prevention, diagnosis, and management of skin disorders and melanomas; research into dermal structures and pathology; and all areas of aesthetic dermatology, including skin maintenance, dermatological surgery, and lasers. The journal is of interest to a broad audience of pharmaceutical and healthcare professionals and publishes original research, reviews, case reports/case series, trial protocols, and short communications. Dermatology and Therapy will consider all scientifically sound research be it positive, confirmatory or negative data. Submissions are welcomed whether they relate to an International and/or a country-specific audience, something that is crucially important when researchers are trying to target more specific patient populations. This inclusive approach allows the journal to assist in the dissemination of quality research, which may be considered of insufficient interest by other journals. The journal appeals to a global audience and receives submissions from all over the world.
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