Safety and tolerability of erenumab in individuals with episodic or chronic migraine across age groups: a pooled analysis of placebo-controlled trials

Migraine is a disabling neurological disease affecting all ages [1] and is the second leading cause of years lived with disability worldwide [2]. Studies have shown that migraine has a substantial impact on individuals in terms of quality of life (QoL) and imposes a heavy socioeconomic burden, with the majority of direct costs due to a higher utilization of healthcare resources compared with matched individuals without migraine.

The prevalence of migraine peaks in those aged 30‒39 years and is relatively lower at the end of the lifespan [3, 4], with a one-year prevalence of approximately 10% in older age groups [5]. As life expectancy increases worldwide, it is likely that a larger percentage of patients will be living with migraine as they grow older [5, 6]. Treatment can become more challenging in these individuals due to the need to consider potential age-related changes in medication metabolism and increased medical comorbidities. For example, older individuals are more likely to experience polypharmacy due to comorbid medical conditions such as hypertension, heart disease, and stroke [5]. Age can also lead to physiological changes that may directly impact the pharmacokinetics and pharmacodynamics of drugs [5]. Such age-related factors may affect the effectiveness of migraine medications as well as their tolerability profile.

The preventive treatment of migraine has typically involved the use of oral medications, such as beta-blockers (propranolol), anti-epileptics (topiramate), and tricyclic anti-depressants (amitriptyline), that were originally developed for other conditions and subsequently repurposed for migraine. Medication side effects associated with these treatments, leading to poor patient adherence, [7‐10] may therefore be a another limiting factor when considering treatment options. Thus, the need for migraine specific prophylactic treatment, specifically targeting older individuals, is of growing importance in order to reduce the risk of medication overuse and most importantly, to increase their QoL.

Recent advances in the field of migraine have led to the development of disease-specific preventive medications. Monoclonal antibodies targeting the calcitonin gene-related peptide (CGRP) receptor (erenumab) or CGRP directly (eptinezumab, fremanezumab, and galcanezumab) are new therapeutic agents for the preventive treatment of migraine. They represent an extension of the therapeutic options, which already exist for migraine prevention. Erenumab, a fully human monoclonal antibody, is an approved potent and selective CGRP receptor antagonist specifically designed to prevent migraine [11]. The clinical efficacy and safety of erenumab has been established in several placebo-controlled studies in episodic migraine (EM) and chronic migraine (CM), [12‐17] including a 5-year open-label study in EM [18]. While previous pooled studies of large clinical trials have analyzed the cardiovascular (CV) [19] and non-CV [20] risk associated with erenumab, an age-stratified analysis has never been performed due to a lack of data for the older age group.

Thus, the aim of this pooled analysis was to examine the safety and tolerability of erenumab in adults with EM or CM across different age groups (< 40, 40–49, 50–59, and ≥ 60 years) using pooled data from five large randomized, placebo-controlled trials. This pooled analysis evaluated CV, cerebrovascular and gastrointestinal (GI) adverse events (AEs) as AEs of special interest (AESI) to help physicians make an informed treatment choice of migraine therapy in individuals of older age.

This pooled analysis demonstrated that erenumab treatment (70 mg and 140 mg) showed similar incidence rates of TEAEs versus placebo across the age groups evaluated. Treatment with erenumab in patients with EM and CM also showed favorable CV and cerebrovascular safety in all age groups. Only minimal GI side effects were observed, even in older patients (≥ 60 years), suggesting that erenumab is a suitable preventive treatment option across all evaluated age groups. Importantly, because erenumab is a mAb, it is not expected to have drug-drug interactions, which are often a secondary challenge in older patients [22].

Management of migraine in older individuals can be complex due to the presence of multiple medical comorbidities, such as diabetes, hypertension, heart disease, and other cerebrovascular events, and their associated medications [23]. Additionally, older individuals are often faced with age-related physiological changes, such as slowing of gastric emptying, and an altered drug metabolism rate [24]. The long-term use of medications for chronic conditions like diabetes, hypertension, thyroid, and arthritis may exacerbate migraine symptoms or trigger migraine, thereby stressing the special attention that is needed when developing treatment plans in these individuals [6, 25].

With an increase in the global life expectancy, there is a shift towards finding optimal solutions to manage health problems in an aging population. Migraine already has a significant impact in older individuals and this impact is likely to increase in line with aging population demographics. At the present time, most standard oral preventive treatments should be used with caution in older individuals due to their unfavorable safety and tolerability profile. This pooled analysis shows that erenumab is a suitable, well-tolerated and effective treatment alternative across all age groups studied.

Older individuals receiving medications can be at a higher risk of CV and cerebrovascular AEs, compounded by pre-existing medical conditions. Furthermore, CGRP is a potent vasodilator and plays an important role in regulating vascular resistance and regional organ blood flow [26]; therefore, erenumab, as a CGRP receptor antagonist, could in theory increase the overall cardiovascular risk profile in all age groups. Indeed, development of hypertension and worsening of preexisting hypertension has been reported following the use of erenumab in a post-marketing setting, [27] leading to a recent revision of the USPI for erenumab to include hypertension as a warning and an adverse drug reaction [22]. However, in this pooled analysis, the incidence of TEAEs of hypertension was low, and our findings suggest that erenumab is well tolerated and poses no additional CV and cerebrovascular risk in patients of all age groups, including older individuals. Similarly, the incidence of TEAEs of constipation, another AE that is frequently reported in a post-marketing setting following use of erenumab, [22, 27, 28] was low across all age groups and comparable across treatment arms in this study. Only one patient in the 50- to 59-year age group receiving 140 mg erenumab discontinued treatment due to constipation. Together, these findings add to the growing body of evidence supporting the safety and tolerability of erenumab across age groups and migraine types.

Kudrow et al. have assessed the vascular safety profile of erenumab across four large placebo-controlled trials with similar findings to this pooled analysis [19]. The CV, cerebrovascular, and peripheral vascular safety profile of erenumab was comparable to that of placebo, with no CV risk associated with erenumab use. Another pooled safety analysis of erenumab that included four double-blind, randomized, placebo-controlled trials and their open-label extensions for > 3 years, assessed the longest-term integrated safety data [20]. A favorable safety and tolerability profile was determined for erenumab, supporting its use as a chronic treatment for migraine prevention. However, it should be acknowledged that these randomized-controlled trials had strict inclusion criteria and thus findings cannot be generalized to the general population. We must continue to rely on post-marketing surveillance and real-world observations to provide new insights into the safety of erenumab in a wider patient population [27, 29, 30].

Recently, other pooled analyses of large, placebo-controlled trials have evaluated the comprehensive safety and tolerability profile of two CGRP inhibitors, eptinezumab [31] and fremanezumab [32], across a broad spectrum of participants with EM or CM. Notably, pooled subgroup analysis assessing the safety profile of fremanezumab in participants aged ≥ 60 years reported comparable findings with the overall pooled population [33]. Furthermore, the CONQUER study, which enrolled patients aged 18‒75 years, found no clinically significant safety findings for AEs, laboratory analytes, vital signs, or ECGs in the subgroup of patients aged 65‒75 years treated with galcanezumab, albeit the sample size was low (N = 29) [34]. While this provides preliminary evidence that use of CGRP mAbs may be safe in individuals beyond 65 years, real-life studies in larger populations of older individuals are needed.

A comprehensive understanding of the safety profile of erenumab is of key importance to treatment planning for effective migraine prevention, particularly in individuals aged ≥ 50 years who are at higher risk of incurring medication-related side effects. This pooled analysis established that the overall safety profile of erenumab 70 mg and 140 mg was comparable with placebo across the age groups evaluated in 3345 individuals with EM or CM, with no increase in AEs in those aged ≥ 50 years. That no notable safety events were found in older individuals receiving erenumab when compared with the other age groups is of key importance and suggests that erenumab is a safe and well-tolerated treatment option for older patients.