The Journal of Headache and Pain (Jul 2021)

MAB-MIG: registry of the spanish neurological society of erenumab for migraine prevention

  • Robert Belvís,
  • Pablo Irimia,
  • Patricia Pozo-Rosich,
  • Carmen González-Oria,
  • Antonio Cano,
  • Javier Viguera,
  • Belén Sánchez,
  • Francisco Molina,
  • Isabel Beltrán,
  • Agustín Oterino,
  • Elisa Cuadrado,
  • Angel Gómez-Camello,
  • Miguel Alberte-Woodward,
  • Carmen Jurado,
  • Teresa Oms,
  • David Ezpeleta,
  • Javier Díaz de Terán,
  • Noemí Morollón,
  • Germán Latorre,
  • Marta Torres-Ferrús,
  • Alicia Alpuente,
  • Raquel Lamas,
  • Carlos Toledano,
  • Rogelio Leira,
  • Sonia Santos,
  • Margarita Sánchez del Río

DOI
https://doi.org/10.1186/s10194-021-01267-x
Journal volume & issue
Vol. 22, no. 1
pp. 1 – 8

Abstract

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Abstract Background Erenumab was approved in Europe for migraine prevention in patients with ≥ 4 monthly migraine days (MMDs). In Spain, Novartis started a personalized managed access program, which allowed free access to erenumab before official reimbursement. The Spanish Neurological Society started a prospective registry to evaluate real-world effectiveness and tolerability, and all Spanish headache experts were invited to participate. We present their first results. Methods Patients fulfilled the ICHD-3 criteria for migraine and had ≥ 4 MMDs. Sociodemographic and clinical data were registered as well as MMDs, monthly headache days, MHDs, prior and concomitant preventive treatment, medication overuse headache (MOH), migraine evolution, adverse events, and patient-reported outcomes (PROs): headache impact test (HIT-6), migraine disability assessment questionnaire (MIDAS), and patient global improvement change (PGIC). A > 50% reduction of MMDs after 12 weeks was considered as a response. Results We included 210 patients (female 86.7%, mean age 46.4 years old) from 22 Spanish hospitals from February 2019 to June 2020. Most patients (89.5%) suffered from chronic migraine with a mean evolution of 8.6 years. MOH was present in 70% of patients, and 17.1% had migraine with aura. Patients had failed a mean of 7.8 preventive treatments at baseline (botulinum toxin type A—BoNT/A—had been used by 95.2% of patients). Most patients (67.6%) started with erenumab 70 mg. Sixty-one percent of patients were also simultaneously taking oral preventive drugs and 27.6% were getting simultaneous BoNT/A. Responder rate was 37.1% and the mean reduction of MMDs and MHDs was -6.28 and -8.6, respectively. Changes in PROs were: MIDAS: -35 points, HIT-6: -11.6 points, PIGC: 4.7 points. Predictors of good response were prior HIT-6 score < 80 points (p = 0.01), ≤ 5 prior preventive treatment failures (p = 0.026), absence of MOH (p = 0.039), and simultaneous BoNT/A treatment (p < 0.001). Twenty percent of patients had an adverse event, but only two of them were severe (0.9%), which led to treatment discontinuation. Mild constipation was the most frequent adverse event (8.1%). Conclusions In real-life, in a personalized managed access program, erenumab shows a good effectiveness profile and an excellent tolerability in migraine prevention in our cohort of refractory patients.

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