夜间脊柱疼痛的改善及其对影像学轴向脊柱关节炎长期结局的影响:依奇珠单抗 COAST-V 随机试验结果。
Improvement in spinal pain at night and its impact on long-term outcomes in radiographic axial spondyloarthritis: Results from Ixekizumab COAST-V randomised trial.
机构信息
Department of Rheumatology, Leiden University Medical Center, Leiden, the Netherlands; Department of Rheumatology, Zuyderland Medical Center, Heerlen, the Netherlands.
Department of Rheumatology, University Hospital Centre of Montpellier, Montpellier, France.
出版信息
Semin Arthritis Rheum. 2024 Dec;69:152571. doi: 10.1016/j.semarthrit.2024.152571. Epub 2024 Oct 23.
INTRODUCTION
Spinal pain at night is a major contributor to the patient burden of radiographic axial spondyloarthritis (r-axSpA), resulting in substantial functional limitations and impairment of health-related quality of life (QoL). Ixekizumab (IXE), an interleukin-17A inhibitor, has shown efficacy in patients with r-axSpA.
OBJECTIVE
To assess spinal pain at night improvement up to week (W) 52 in COAST-V and to determine if clinically important improvement in spinal pain at night at W16 is associated with improvement in disease activity and other patient-reported outcomes (PROs) at W16 and W52.
METHODS
The 52 W phase 3 COAST-V trial investigated the efficacy of IXE in patients with r-axSpA that were naïve to biological disease-modifying anti-rheumatic drug (bDMARD). Patients were randomised to IXE every two weeks (Q2W), IXE every four weeks (Q4W), adalimumab (ADA) Q2W, or placebo up to W16. Patients were categorised as achieving or not achieving a ≥3-point improvement, considered a clinically important improvement (CII), in spinal pain at night at W16. Associations between achieving CII in spinal pain at night at W16 and change from baseline in disease activity (ASDAS, ASAS40), Fatigue severity NRS, JSEQ, WPAI and the SF-36 survey, were tested using analysis of covariance (continuous variables) and logistic regression (binary variables).
RESULTS
At W16, 63.0 % (n=51), 46.7 % (n=42), and 32.2 % (n=28) of patients treated with IXE Q4W, ADA Q2W, and placebo, respectively, had reached a CII in spinal pain at night. Of those who were treated with IXE Q4W and achieved a CII in spinal pain at night at W16, 58.8 % and 66.7 % achieved an ASDAS <2.1 at W16 and W52 while 25.5 % and 29.4 % of patients also achieved ASDAS <1.3 at W16 and W52, respectively. Results at W16 and W52 show an improvement in disease activity, functioning, and health related QoL for patients who achieved a CII in spinal pain at night at W16.
CONCLUSION
A larger proportion of patients treated with IXE Q4W achieved rapid and clinically meaningful improvement in spinal pain at night versus placebo, with improvements maintained up to W52. Achieving a CII in spinal pain at night at W16 was associated with improved disease activity, functioning, PROs, and QoL at W16 and W52.
TRIAL REGISTRATION
ClinicalTrials.gov NCT02696785.
简介
夜间脊柱疼痛是放射学轴向脊柱关节炎(r-axSpA)患者负担的主要原因,导致严重的功能受限和健康相关生活质量(QoL)受损。白细胞介素-17A 抑制剂依奇珠单抗(IXE)已在 r-axSpA 患者中显示出疗效。
目的
评估 COAST-V 中夜间脊柱疼痛在第 52 周(W)的改善情况,并确定第 16 周时夜间脊柱疼痛的临床显著改善是否与疾病活动度和其他患者报告结局(PROs)的改善相关在第 16 周和第 52 周。
方法
为期 52 周的 3 期 COAST-V 试验研究了 IXE 在生物疾病修饰抗风湿药物(bDMARD)治疗初治的 r-axSpA 患者中的疗效。患者被随机分配至 IXE 每两周(Q2W)、IXE 每四周(Q4W)、阿达木单抗(ADA)Q2W 或安慰剂,直至第 16 周。患者被分类为在第 16 周时达到或未达到夜间脊柱疼痛改善≥3 分,被认为是临床显著改善(CII)。使用协方差分析(连续变量)和逻辑回归(二分类变量)来测试第 16 周时夜间脊柱疼痛 CII 与疾病活动度(ASDAS、ASAS40)、疲劳严重程度 NRS、JSEQ、WPAI 和 SF-36 调查从基线的变化之间的关联。
结果
在第 16 周时,分别有 63.0%(n=51)、46.7%(n=42)和 32.2%(n=28)接受 IXE Q4W、ADA Q2W 和安慰剂治疗的患者夜间脊柱疼痛达到 CII。在第 16 周时接受 IXE Q4W 治疗并达到夜间脊柱疼痛 CII 的患者中,分别有 58.8%和 66.7%在第 16 周和第 52 周时达到 ASDAS<2.1,而分别有 25.5%和 29.4%的患者在第 16 周和第 52 周时也达到 ASDAS<1.3。第 16 周和第 52 周的结果显示,在第 16 周夜间脊柱疼痛达到 CII 的患者中,疾病活动度、功能和健康相关 QoL 得到改善。
结论
与安慰剂相比,更多接受 IXE Q4W 治疗的患者夜间脊柱疼痛快速且具有临床意义的改善,这种改善一直持续到第 52 周。在第 16 周时达到夜间脊柱疼痛的 CII 与第 16 周和第 52 周时的疾病活动度、功能、PROs 和 QoL 的改善相关。
试验注册
ClinicalTrials.gov NCT02696785。
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