Predicting response to CGRP-monoclonal antibodies in patients with migraine in Japan: a single-centre retrospective observational study

We conducted a single-centre, retrospective, real-world study on patients with migraine who were treated with CGRPmAbs at Keio University Hospital in Tokyo, Japan. This study was approved by the Institutional Review Board of Keio University School of Medicine (approval number: 20211144). Patients were informed of this observational study via the institute’s website and could opt out of the study. The need for informed consent was waived by the Ethics Committee of the Keio University School of Medicine, in accordance with national regulations (Ethical Guidelines for Medical and Biological Research Involving Human Subjects). All methods were carried out in accordance with relevant guidelines and regulations.

The inclusion criteria for responder analysis were as follows: treatment of ≥ 3 months of galcanezumab (240 mg/120 mg/120 mg), erenumab (70 mg), or fremanezumab (225 mg monthly or 675 mg quarterly starting from 225 mg monthly) as their first CGRPmAb (de novo) from the Headache Group of Keio University Hospital; receipt of the first dose of CGRPmAb between the 12^th of August 2021 (when the drug became available at the hospital) and 31^st of August 2022; fulfilment of the diagnostic criteria for migraine (including probable migraine) according to the International Classification of Headache Disorders, 3^rd edition (ICHD-3); and age ≥ 18 years. The patients were diagnosed with migraine by a headache specialist (TT). Non-Asian patients were excluded (Fig. 1).

We retrospectively collected demographic data (age, sex, height, and weight), medical history (psychiatric, gastrointestinal, vascular, hormonal, cancer, respiratory, and immuno-rheumatologic), and the following headache characteristics: onset age, family history of headache, migraine characteristics (unilateral pain, pulsating pain, or aggravation by routine physical activity), pain intensity (0–10; numerical rating scale [NRS]), associated symptoms (photophobia, phonophobia, and nausea/vomiting; none, mild, moderate, or severe), and the presence of aura. The headache specialist explained the criteria for migraine based on the ICHD-3 to all patients who were asked to track headache and migraine days (including probable migraine days). Patients completed a questionnaire on monthly migraine days (MMD), monthly headache days (MHD), monthly acute medication intake days (AMD) at baseline and MMD after 3 months of treatment. A month was defined as 28 days. The headache specialist verified the accuracy and reliability of the completed questionnaire by interviewing and occasionally reviewing each patient’s headache diary. Patients were classified as having episodic migraine or chronic migraine, according to the ICHD-3. Patients were also diagnosed with MOH based on the ICHD-3. Patients completed the Generalized Anxiety Disorder-7 (GAD-7) questionnaire [27, 28] and Patient Health Questionnaire-9 (PHQ-9) [29] upon CGRPmAb administration to determine the extent of anxiety and depression, respectively. We also collected patient migraine-preventive drug data, including failures of preventative drugs (lomerizine, propranolol, valproate, amitriptyline, or topiramate) before CGRPmAb treatment and response frequency to triptan (0, 1, 2, 3 out of three uses) [10].

We calculated the percentage reduction in MMD from baseline after 3 months of treatment. We assessed the characteristics of patients who responded with ≥ 25%, 50%, and 75% reduction in MMD by comparing the average scores between responders and non-responders for the following items: patient characteristics (age, onset age, sex, and body mass index [BMI]), diagnosis (episodic or chronic, presence of aura), migraine characteristics (unilateral/bilateral, pulsating/non-pulsating, pain intensity on NRS, duration, and aggravation by routine physical activity), MHD, MMD, AMD, whether patients had MOH or not, associated symptoms (photophobia, phonophobia, and nausea/vomiting), treatment (triptan response and total prior failures), other scores (GAD-7 and PHQ-9), medical history (psychiatric, gastrointestinal, vascular, hormonal, cancer, respiratory, or immuno-rheumatologic), and family history of headache. Triptan response was defined as how many times triptan successfully relieved a headache out of three usages.

We compared average scores using the unpaired t-test for continuous variables and chi-square test for categorical variables. All two-sided p-values < 0.05 were considered statistically significant. We also used univariate logistic regression models to determine the baseline characteristics associated with a 50% response to CGRPmAb. The variables significantly associated with the response (p < 0.1) were then tested as independent variables in a multivariate logistic regression model to evaluate potentially independent associations with responder status and to check for collinearity. We reported the odds ratios (ORs) and 95% confidence intervals (CIs) for the risk factors. Missing data were excluded. Statistical analyses were performed using R version 4.0.3 [30].

From the 12th of August 2021 to 31st of August 2022, 125 patients started CGRPmAb treatment at the Keio University Hospital Headache outpatient clinic (galcanezumab: 62 (50%), fremanezumab: 43 (34%), and erenumab: 20 (16%)) (Fig. 1). We excluded one non-Asian patient. In addition, we excluded two patients when analysing the triptan response, as they had not taken the medication multiple times. One patient did not complete PHQ-9 questionnaire and was excluded when analyzing PHQ-9 scores. Twenty-two patients received CGRPmAbs treatment for less than 3 months: 9 discontinued CGRPmAb due to adverse effects (light-headedness, hair loss, eczema, palpitation, throat itching, or constipation) or ineffectiveness, and 13 started CGRPmAbs later than 3 months before the end of the study period. We excluded one patient whose CGRPmAb response could not be assessed due to missing data. No patient was lost to follow-up. One-hundred-and-one patients were considered eligible for the responder analysis (galcanezumab: 57 (56%), fremanezumab: 31 (31%), and erenumab: 13 (13%)). In Japan, one of three CGRPmAbs can be selected after physician–patient discussions. Although erenumab was the first to be placed on the market globally, galcanezumab was launched first in Japan; accordingly, galcanezumab was the most frequently prescribed CGRPmAb in the present study. Additionally, many patients appreciated the convenience of fremanezumab, which can be administered quarterly, not necessarily monthly, making erenumab the least frequently prescribed CGRPmAb during the study period (self-injection of fremanezumab or erenumab was not available during the study period).

After 3 months of treatment, among 101 patients, 71 (70%), 55 (54%), and 31 (31%) patients achieved ≥ 25%, 50%, and 75% reduction in MMDs, respectively. The comparison of ≥ 25%, 50%, and 75% responders and non-responders revealed statistically significant differences in duration, photophobia, total prior treatment failures (p = 0.004, 0.012 and 0.023), age, MHD, and total prior treatment failures (p = 0.003 0.027, and 0.040), and triptan response and total prior treatment failures (p = 0.047 and 0.022), respectively (Table 1). Seven patients had a medical history of immuno-rheumatologic diseases: 1 was a ≥ 50% responder (with a history of Sjogren’s syndrome), and 6 were non-responders with the following histories: rheumatoid arthritis (n = 3), myasthenia gravis (n = 1), Sjogren’s syndrome (n = 1), and peripheral spondyloarthritis (n = 1).

Baseline characteristics were analysed using univariate and multivariate logistic regression models to screen for and identify the prognostic factors of ≥ 50% response to CGRPmAb. Univariate analysis revealed positive associations with age, response to triptans in 2–3 of 3 usages, and moderate photophobia, and negative associations with duration, MHD, prior treatment failures, medical history (immuno-rheumatologic), and family history of headaches (p < 0.1). Multivariate analysis revealed that age was a positive predictor of response, and total prior treatment failures and immuno-rheumatologic medical history were negative predictors of response, with significance (OR = 1.072, 0.512, and 0.027; CI = 1.025–1.121, 0.290–0.904, and 0.002–0.422; p = 0.002, 0.021, and 0.010, respectively) (Table 2).