The Headache and Facial Pain Service, Guy's and St Thomas' NHS Foundation Trust, London, UK.
Wolfson CARD, Institute of Psychiatry, Psychology and Neuroscience, King's College London, United Kingdom, London, UK.
Neurotherapeutics. 2023 Sep;20(5):1284-1293. doi: 10.1007/s13311-023-01394-0. Epub 2023 Jul 10.
In migraine patients with a poor response to a calcitonin gene-related peptide monoclonal antibody against the receptor, switching to a calcitonin gene-related peptide monoclonal antibodies against the ligand may be beneficial. This was a long-term real-world prospective analysis conducted in treatment-refractory chronic migraine patients coming from two large tertiary referral headache centres, who did not achieve a meaningful response to erenumab and were switched to fremanezumab. Responders to fremanezumab were considered those who achieved at least 30% reduction in monthly migraine days by month 3, compared to the post-erenumab baseline. Secondary efficacy and disability outcomes were analysed. Thirty-nine patients (female n = 32, 82.1%; median age: 49 years old, IQR = 29.0-56.0) were included. After three months of treatment with fremanezumab, ten out of 39 patients (25.6%) were considered responders. Four of the 11 patients who continued fremanezumab became responders at month 6, increasing the number of responders to 14 patients (35.9%). Responders received a median of 12 injections (IQR = 9.0-18.0) at the time of the analysis. After the last treatment, 13 patients (33.3%) remained responders. The number of mean monthly migraine days significantly decreased from 21.4 at baseline (IQR = 10.7-30.0) to 8.6 (IQR = 3.8-13.9) at the last follow-up. Painkillers intake and HIT-6 score were significantly reduced at the last follow-up. About 1/3 of patients with treatment refractory chronic migraine who have a disappointing response to erenumab and switch to fremanezumab, obtained a meaningful and sustained improvement of their migraine load over time, supporting the appropriateness of this therapeutic approach in clinical practice.
在对降钙素基因相关肽受体单克隆抗体反应不佳的偏头痛患者中,切换为降钙素基因相关肽配体单克隆抗体可能是有益的。这是一项在来自两个大型三级转诊头痛中心的治疗抵抗性慢性偏头痛患者中进行的长期真实世界前瞻性分析,这些患者对依那西普没有明显反应,转而使用了 fremanezumab。对 fremanezumab 的应答者被认为是在第 3 个月与依那西普后基线相比,每月偏头痛天数减少至少 30%的患者。分析了次要疗效和残疾结果。39 例患者(女性 n=32,82.1%;中位数年龄:49 岁,IQR=29.0-56.0)被纳入。在接受 fremanezumab 治疗 3 个月后,39 例患者中有 10 例(25.6%)被认为是应答者。继续接受 fremanezumab 治疗的 11 例患者中有 4 例在第 6 个月成为应答者,使应答者增加到 14 例(35.9%)。应答者在分析时接受了中位数为 12 次注射(IQR=9.0-18.0)。末次治疗后,13 例患者(33.3%)仍为应答者。每月偏头痛天数的平均值从基线时的 21.4 天(IQR=10.7-30.0)显著减少到末次随访时的 8.6 天(IQR=3.8-13.9)。止痛药摄入量和 HIT-6 评分在末次随访时显著降低。大约 1/3 的治疗抵抗性慢性偏头痛患者对依那西普反应不佳,转而使用 fremanezumab,随着时间的推移,他们的偏头痛负担得到了有意义且持续的改善,这支持了这种治疗方法在临床实践中的适当性。
