Department of Internal Medicine, American University of Beirut Medical Center, Beirut, Lebanon
Center for Research on Rare Blood Disorders (CR-RBD), Burjeel Medical City, Abu Dhabi, UAE.
BMJ Open. 2024 Nov 14;14(11):e085234. doi: 10.1136/bmjopen-2024-085234.
To estimate thresholds for defining meaningful within-patient improvement from baseline to weeks 13-24 and interpreting meaningfulness of between-group difference for the non-transfusion-dependent beta-thalassaemia patient-reported outcome (NTDT-PRO) tiredness/weakness (T/W) and shortness of breath (SoB) scores. A secondary objective was to determine the symptom severity threshold for the NTDT-PRO T/W domain to identify patients with symptomatic T/W.
Pooled blinded data from the phase 2, double-blind, placebo-controlled, randomised BEYOND trial in NTDT (NCT03342404) were used. Anchor-based analyses supplemented with distribution-based analyses and empirical cumulative distribution function (eCDF) curves were applied. Distribution-based analyses and receiver operating characteristic curves were used to estimate between-group difference and symptomatic thresholds, respectively.
Greece, Italy, Lebanon, Thailand, the UK and the USA.
Adults (N=145; mean age 39.9 years) with NTDT who were transfusion-free ≥8 weeks before randomisation.
Score changes from baseline to weeks 13-24 in PROs used as anchors (correlation coefficient ≥0.3): NTDT-PRO T/W and SoB scores, Patient Global Impression of Severity, Functional Assessment of Chronic Illness Therapy-Fatigue (Fatigue Subscale, item HI12 and item An2) and Short Form Health Survey version 2.
The eCDF curves support the use of estimates from the improvement by one level group for all anchors to determine the threshold(s) for meaningful within-patient improvement. Mean (median) changes from these groups and estimates from distribution-based analyses suggest that a ≥1-point reduction in the NTDT-PRO T/W or SoB domains represents a clinically meaningful improvement. Meaningful between-group difference threshold ranges were 0.53-1.10 for the T/W domain and 0.65-1.15 for the SoB domain. The optimal symptomatic threshold for the T/W domain (by maximum Youden's index) was ≥3 points.
The thresholds proposed may support the use of NTDT-PRO in assessing and interpreting treatment effects in clinical studies and identifying patients with NTDT in need of symptom relief.
估计从基线到第 13-24 周定义患者个体内有意义改善的阈值,并解释非输血依赖型β地中海贫血患者报告结局(NTDT-PRO)疲乏/无力(T/W)和呼吸短促(SoB)评分的组间差异的有意义程度。次要目的是确定 NTDT-PRO T/W 领域的症状严重程度阈值,以识别有症状 T/W 的患者。
使用来自非输血依赖型β地中海贫血的 2 期、双盲、安慰剂对照、随机 BEYOND 试验的汇总盲法数据(NCT03342404)。应用基于锚点的分析方法,补充基于分布的分析和经验累积分布函数(eCDF)曲线。基于分布的分析和接收者操作特征曲线分别用于估计组间差异和有症状阈值。
希腊、意大利、黎巴嫩、泰国、英国和美国。
年龄≥18 岁的 NTDT 成人(N=145;平均年龄 39.9 岁),在随机分组前 8 周以上无需输血。
使用作为锚点的 PRO 评分的从基线到第 13-24 周的变化(相关系数≥0.3):NTDT-PRO T/W 和 SoB 评分、患者总体印象严重程度、慢性疾病治疗功能评估-疲劳(疲劳分量表、项 HI12 和项 An2)和健康调查简表 2.0。
eCDF 曲线支持使用提高一个等级组的估计值来确定所有锚点的有意义的患者个体内改善的阈值。这些组的平均(中位数)变化和基于分布的分析估计值表明,T/W 或 SoB 领域的评分降低≥1 分代表有临床意义的改善。T/W 领域的有意义的组间差异阈值范围为 0.53-1.10,SoB 领域的阈值范围为 0.65-1.15。T/W 领域最佳的有症状阈值(通过最大 Youden 指数)为≥3 分。
提出的阈值可能支持在临床研究中使用 NTDT-PRO 评估和解释治疗效果,并识别需要缓解症状的 NTDT 患者。
