Does MIDAS reduction at 3 months predict the outcome of erenumab treatment? A real-world, open-label trial.

The Journal of Headache and Pain Pub Date : 2022-09-17 DOI:10.1186/s10194-022-01480-2

Roberto De Icco, Gloria Vaghi, Marta Allena, Natascia Ghiotto, Elena Guaschino, Daniele Martinelli, Lara Ahmad, Michele Corrado, Federico Bighiani, Federica Tanganelli, Sara Bottiroli, Francescantonio Cammarota, Grazia Sances, Cristina Tassorelli

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引用次数: 7

Abstract

Background: In Italy, monoclonal antibodies targeting the CGRP pathway are subsidized for the preventive treatment of high frequency and chronic migraine (CM) in patients with a MIgraine Disability ASsessment (MIDAS) score ≥ 11. Eligibility to treatment continuation requires a ≥ 50% MIDAS score reduction at three months (T3). In this study, we evaluate whether a ≥ 50% MIDAS score reduction at T3 is a reliable predictor of response to one-year erenumab treatment.

Methods: In this prospective, open-label, real-world study, 77 CM patients were treated with erenumab 70-140 mg s.c. every 28 days for one year (T13). We collected the following variables: monthly migraine days (MMDs), monthly headache days (MHDs), days of acute medication intake, MIDAS, HIT-6, anxiety, depression, quality of life and allodynia. Response to erenumab was evaluated as: i) average reduction in MMDs during the 1-year treatment period; and ii) percentage of patients with ≥ 50% reduction in MMDs during the last 4 weeks after the 13^th injection (Responders^T13).

Results: Erenumab induced a sustained reduction in MMDs, MHDs and intake of acute medications across the 12-month treatment period, with 64.9% of patients qualifying as Responders^T13. At T3, 55.8% of patients reported a ≥ 50% reduction in MIDAS score (MIDAS^Res) and 55.4% of patients reported a ≥ 50% reduction in MMDs (MMD^Res). MIDAS^Res and MMD^Res patients showed a more pronounced reduction in MMDs during the 1-year treatment as compared to NON-MIDAS^Res (MIDAS^Res: T0: 23.5 ± 4.9 vs. T13: 7.7 ± 6.2; NON- MIDAS^Res: T0: 21.6 ± 5.4 vs. T13: 11.3 ± 8.8, p = 0.045) and NON-MMD^Res (MMD^Res: T0: 23.0 ± 4.5 vs. T13: 6.6 ± 4.8; NON-MMD^Res: T0: 22.3 ± 6.0 vs. T13: 12.7 ± 9.2, p < 0.001) groups. The percentage of Responders^T13 did not differ between MIDAS^Res (74.4%) and NON-MIDAS^Res (52.9%) patients (p = 0.058), while the percentage of Responders^T13 was higher in the MMD^Res group (83.3%) when compared to NON-MMD^Res (42.9%) (p = 0.001). MMD^Res predicted the long-term outcome according to a multivariate analysis (Exp(B) = 7.128; p = 0.001), while MIDAS^Res did not. Treatment discontinuation based on MIDAS^Res would have early excluded 36.0% of Responders^T13. Discontinuation based on "either MIDAS^Res or MMD^Res" would have excluded a lower percentage (16%) of Responders^T13.

Conclusion: MIDAS^Res only partly reflects the 12-month outcome of erenumab treatment in CM, as it excludes more than one third of responders. A criterion based on the alternative consideration of ≥ 50% reduction in MIDAS score or MMDs in the first three months of treatment represents a more precise and inclusive option.

Trial registration: The trial was retrospectively registered at www.

Clinicaltrials: gov (NCT05442008). CGRP: Calcitonin Gene Related Peptide.

Midas: MIgraine Disability Assessment. MMDs: monthly migraine days. MIDAS^Res: Patients with a MIDAS score reduction of at least 50% at T3. MMD^Res: Patients with a MMDs reduction of at least 50% at T3. Responder^T13: Patients with a MMDs reduction from baseline of at least 50% in the last 4 weeks of observation period (after 13 erenumab administrations). T0: First erenumab administration. T3, T6, T9, T12: Follow-up visits at three, six, nine, and twelve months after first erenumab administration. T13: Last visit of the protocol.

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3个月时MIDAS降低是否预示着伊瑞那单抗治疗的结果?一个真实的、开放标签的试验。

背景:在意大利，针对CGRP通路的单克隆抗体被资助用于偏头痛残疾评估(MIDAS)评分≥11的高频和慢性偏头痛(CM)患者的预防性治疗。有资格继续治疗需要在3个月(T3)时MIDAS评分降低≥50%。在这项研究中，我们评估T3时MIDAS评分降低≥50%是否是对一年erenumab治疗反应的可靠预测因子。方法:在这项前瞻性、开放标签、真实世界的研究中，77例CM患者每28天服用erenumab 70-140 mg s.c.，持续一年(T13)。我们收集了以下变量:每月偏头痛天数(MMDs)、每月头痛天数(MHDs)、急性药物摄入天数、MIDAS、HIT-6、焦虑、抑郁、生活质量和异常性疼痛。对erenumab的反应评估为:i) 1年治疗期间MMDs的平均减少;ii)在第13次注射后的最后4周内MMDs减少≥50%的患者百分比(RespondersT13)。结果:在12个月的治疗期间，Erenumab诱导MMDs、mhd和急性药物摄入持续减少，64.9%的患者符合RespondersT13标准。在T3时，55.8%的患者报告MIDAS评分(MIDASRes)降低≥50%，55.4%的患者报告MMDs (MMDRes)降低≥50%。与非MIDASRes相比，MIDASRes和MMDRes患者在1年治疗期间MMDs的降低更为明显(MIDASRes: T0: 23.5±4.9 vs. T13: 7.7±6.2;非MIDASRes: T0: 21.6±5.4 vs T13: 11.3±8.8,p = 0.045)和NON-MMDRes (MMDRes: T0: 23.0±4.5 vs T13: 6.6±4.8;非MMDRes: T0: 22.3±6.0 vs. T13: 12.7±9.2,T13在MIDASRes(74.4%)和NON-MIDASRes(52.9%)患者之间没有差异(p = 0.058)，而MMDRes组的RespondersT13百分比(83.3%)高于NON-MMDRes (42.9%) (p = 0.001)。MMDRes通过多变量分析预测远期预后(Exp(B) = 7.128;p = 0.001)，而MIDASRes则没有。基于MIDASRes的治疗终止将早期排除36.0%的应答者13。基于“MIDASRes或MMDRes”的停药将排除较低百分比(16%)的RespondersT13。结论:MIDASRes仅部分反映了CM患者伊莫那单抗治疗12个月的结果，因为它排除了超过三分之一的应答者。在治疗的前三个月，基于MIDAS评分或MMDs降低≥50%的替代考虑的标准代表了一个更精确和包容的选择。试验注册:该试验在www.Clinicaltrials: gov (NCT05442008)上回顾性注册。CGRP:降钙素基因相关肽。Midas:偏头痛残疾评估。MMDs:每月偏头痛天数。MIDASRes:在T3时MIDAS评分降低至少50%的患者。MMDRes:在T3时MMDs降低至少50%的患者。ResponderT13:在最后4周的观察期内(在13次erenumab给药后)MMDs从基线降低至少50%的患者。T0:第一次给药。T3、T6、T9、T12:首次给药后3、6、9、12个月随访。T13:议定书的最后一次访问。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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The Journal of Headache and Pain

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