使用BE VIVID和BE READY 3期试验的数据,对银屑病症状与影响测量量表(P-SIM)进行心理测量学验证,这是一种用于斑块状银屑病患者的新型患者报告结局工具。
Psychometric Validation of the Psoriasis Symptoms and Impacts Measure (P-SIM), a Novel Patient-Reported Outcome Instrument for Patients with Plaque Psoriasis, Using Data from the BE VIVID and BE READY Phase 3 Trials.
作者信息
Warren Richard B, Gottlieb Alice B, Merola Joseph F, Garcia Llenalia, Cioffi Christopher, Peterson Luke, Pelligra Christopher, Ciaravino Valerie
机构信息
Dermatology Centre, Manchester NIHR Biomedical Research Centre, Salford Royal NHS Foundation Trust, The University of Manchester, Stott Lane, Salford, M6 8HD, Greater Manchester, UK.
Icahn School of Medicine at Mount Sinai, New York, NY, USA.
出版信息
Dermatol Ther (Heidelb). 2021 Oct;11(5):1551-1569. doi: 10.1007/s13555-021-00570-4. Epub 2021 Jul 14.
INTRODUCTION
Plaque psoriasis can significantly impact patients' quality of life. We assessed psychometric properties of the Psoriasis Symptoms and Impacts Measure (P-SIM), developed to capture patients' experiences of signs, symptoms and impacts of psoriasis.
METHODS
Pooled, blinded, 16-week data from 1002 patients in the BE VIVID and BE READY bimekizumab phase 3 trials were analysed. The suitability of the P-SIM missing score rule (weekly scores considered missing if ≥ 4 daily scores were missing) was assessed. Test-retest reliability was evaluated using intraclass correlation coefficients (ICCs). Convergent validity was assessed between P-SIM and relevant patient-reported outcome (PRO) (Dermatology Life Quality Index [DLQI], DLQI item 1 [skin symptoms], Patient Global Assessment of Psoriasis) and clinician-reported outcome (ClinRO) scores (Psoriasis Area and Severity Index [PASI], Investigator's Global Assessment [IGA]) at baseline and week 16. Known-groups validity was assessed, comparing P-SIM scores between patient subgroups predefined using PASI/IGA scores. Sensitivity to change over 16 weeks was evaluated; responder definition (RD) thresholds were explored.
RESULTS
The missing score rule used did not impact P-SIM scores. Test-retest reliability analyses demonstrated excellent score reproducibility (ICC 0.91-0.98). Inter-item correlations at baseline and week 16 were strong (> 0.5), apart from "choice of clothing" with "skin pain" and "burning" at baseline (both 0.49). All P-SIM scores were moderately to strongly correlated with other outcomes, demonstrating convergent validity, apart from ClinROs (PASI, IGA) at baseline that had low variability. P-SIM scores discriminated known groups at week 16, confirming known-groups validity. Changes from baseline to week 16 in P-SIM and other clinically relevant outcomes were strongly correlated (> 0.5; weaker with ClinROs), establishing sensitivity to change. Anchor-based RD analyses determined a four-point P-SIM item score decrease as indicative of marked clinically meaningful improvement.
CONCLUSION
P-SIM scores demonstrated good reliability, validity and sensitivity to change. A four-point RD threshold could be used to assess 16-week treatment effects.
TRIAL REGISTRATION
BE VIVID: NCT03370133; BE READY: NCT03410992.
引言
斑块状银屑病会显著影响患者的生活质量。我们评估了银屑病症状与影响量表(P-SIM)的心理测量特性,该量表旨在了解患者对银屑病体征、症状及影响的体验。
方法
分析了BE VIVID和BE READY两项司库奇尤单抗3期试验中1002例患者汇总的、盲法的16周数据。评估了P-SIM缺失分数规则(如果每周至少4个每日分数缺失,则该周分数视为缺失)的适用性。使用组内相关系数(ICC)评估重测信度。在基线和第16周时,评估P-SIM与相关患者报告结局(PRO)(皮肤病生活质量指数[DLQI]、DLQI第1项[皮肤症状]、患者银屑病整体评估)和临床医生报告结局(ClinRO)评分(银屑病面积和严重程度指数[PASI]、研究者整体评估[IGA])之间的收敛效度。评估已知组效度,比较使用PASI/IGA评分预先定义的患者亚组之间的P-SIM评分。评估16周内对变化的敏感性;探索反应者定义(RD)阈值。
结果
所使用的缺失分数规则不影响P-SIM评分。重测信度分析显示评分具有出色的可重复性(ICC 0.91 - 0.98)。除了基线时“服装选择”与“皮肤疼痛”和“烧灼感”的相关性(均为0.49)外,基线和第16周时各条目之间的相关性很强(>0.5)。除了基线时变异性较低的ClinRO(PASI、IGA)外,所有P-SIM评分与其他结局均呈中度至高度相关,表明具有收敛效度。P-SIM评分在第16周时能够区分已知组,证实了已知组效度。P-SIM和其他临床相关结局从基线到第16周的变化高度相关(>0.5;与ClinRO的相关性较弱),表明具有对变化的敏感性。基于锚定的RD分析确定P-SIM条目评分降低4分表明有显著的临床意义改善。
结论
P-SIM评分显示出良好的信度、效度和对变化的敏感性。四分的RD阈值可用于评估16周的治疗效果。试验注册:BE VIVID:NCT03370133;BE READY:NCT03410992。
Zotero 插件