采用潜在类别轨迹模型揭示了活动期 SLE 患者随时间推移的疾病活动的不同模式。
Distinct patterns of disease activity over time in patients with active SLE revealed using latent class trajectory models.
机构信息
Rheumatology Research Group, Institute of Inflammation and Ageing, College of Medical and Dental Sciences, University of Birmingham, Birmingham, UK.
Rheumatology Department, Sandwell and West Birmingham NHS Trust, Birmingham, UK.
出版信息
Arthritis Res Ther. 2021 Jul 29;23(1):203. doi: 10.1186/s13075-021-02584-x.
BACKGROUND
Systemic lupus erythematosus (SLE) is a heterogeneous systemic autoimmune condition for which there are limited licensed therapies. Clinical trial design is challenging in SLE due at least in part to imperfect outcome measures. Improved understanding of how disease activity changes over time could inform future trial design. The aim of this study was to determine whether distinct trajectories of disease activity over time occur in patients with active SLE within a clinical trial setting and to identify factors associated with these trajectories.
METHODS
Latent class trajectory models were fitted to a clinical trial dataset of a monoclonal antibody targeting CD22 (Epratuzumab) in patients with active SLE using the numerical BILAG-2004 score (nBILAG). The baseline characteristics of patients in each class and changes in prednisolone over time were identified. Exploratory PK-PD modelling was used to examine cumulative drug exposure in relation to latent class membership.
RESULTS
Five trajectories of disease activity were identified, with 3 principal classes: non-responders (NR), slow responders (SR) and rapid-responders (RR). In both the SR and RR groups, significant changes in disease activity were evident within the first 90 days of the trial. The SR and RR patients had significantly higher baseline disease activity, exposure to epratuzumab and activity in specific BILAG domains, whilst NR had lower steroid use at baseline and less change in steroid dose early in the trial.
CONCLUSIONS
Longitudinal nBILAG scores reveal different trajectories of disease activity and may offer advantages over fixed endpoints. Corticosteroid use however remains an important confounder in lupus trials and can influence early response. Changes in disease activity and steroid dose early in the trial were associated with the overall disease activity trajectory, supporting the feasibility of performing adaptive trial designs in SLE.
背景
系统性红斑狼疮(SLE)是一种异质性全身性自身免疫性疾病,其治疗方法有限。由于临床试验中存在不完善的结局评估,因此 SLE 的临床试验设计极具挑战性。对疾病活动随时间变化的深入理解可能为未来的临床试验设计提供信息。本研究旨在确定在临床试验环境中,患有活动性 SLE 的患者是否存在疾病活动随时间变化的不同轨迹,并确定与这些轨迹相关的因素。
方法
使用数值 BILAG-2004 评分(nBILAG)对靶向 CD22 的单克隆抗体(Epratuzumab)治疗活动性 SLE 的临床试验数据集进行潜在类别轨迹模型拟合。确定每个类别的患者的基线特征和随时间推移的泼尼松变化情况。探索性 PK-PD 模型用于检查累积药物暴露与潜在类别成员的关系。
结果
确定了 5 种疾病活动轨迹,其中有 3 个主要类别:无应答者(NR)、缓慢应答者(SR)和快速应答者(RR)。在 SR 和 RR 组中,在试验的前 90 天内,疾病活动的显著变化。SR 和 RR 患者的基线疾病活动、暴露于 Epratuzumab 和特定 BILAG 域的活性明显更高,而 NR 患者在基线时使用的皮质类固醇激素较低,且在试验早期皮质类固醇激素剂量变化较少。
结论
纵向 nBILAG 评分揭示了不同的疾病活动轨迹,并且可能优于固定终点。然而,皮质类固醇激素的使用仍然是狼疮试验中的一个重要混杂因素,并可能影响早期反应。试验早期疾病活动和皮质类固醇剂量的变化与整体疾病活动轨迹相关,支持在 SLE 中进行适应性试验设计的可行性。
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