Optimization of acute medication use following eptinezumab initiation during a migraine attack: post hoc analysis of the RELIEF study

Cady, Roger; Lipton, Richard B.; Buse, Dawn C.; Lindstén, Annika; Ettrup, Anders

doi:10.1186/s10194-022-01463-3

Cited by 6 publications

(7 citation statements)

References 27 publications

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“…Compared to the placebo group, CGRP antibody therapies resulted in a reduction of monthly migraine days of 1.44–1.55 days (i.e., in patients who on average have 8–14 migraine headache days per month) ( Deen et al, 2017 ; Tso and Goadsby, 2017 ; Tepper, 2018 ; Deng et al, 2020 ; Vandervorst et al, 2021 ). In addition, eptinezumab was shown to increase the proportion of patients with moderate/maximal optimization from 31% at baseline to 58% at week four compared to 40–50% in the placebo group and was associated with improvements in acute medication optimization compared with placebos ( Cady et al, 2022 ). Furthermore, anti-CGRP antibodies were shown to reduce acute migraine-specific medication days of 1.28 days and the use of acute headache medication ( Deng et al, 2020 ; Tepper et al, 2021 ).…”

Section: Discussionmentioning

confidence: 99%

Gel-forming antagonist provides a lasting effect on CGRP-induced vasodilation

Chang

Cai²,

Hsu³

2022

Front. Pharmacol.

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Migraine affects ∼15% of the adult population, and the standard treatment includes the use of triptans, ergotamines, and analgesics. Recently, CGRP and its receptor, the CLR/RAMP1 receptor complex, have been targeted for migraine treatment due to their critical roles in mediating migraine headaches. The effort has led to the approval of several anti-CGRP antibodies for chronic migraine treatment. However, many patients still suffer continuous struggles with migraine, perhaps due to the limited ability of anti-CGRP therapeutics to fully reduce CGRP levels or reach target cells. An alternative anti-CGRP strategy may help address the medical need of patients who do not respond to existing therapeutics. By serendipity, we have recently found that several chimeric adrenomedullin/adrenomedullin 2 peptides are potent CLR/RAMP receptor antagonists and self-assemble to form liquid gels. Among these analogs, the ADE651 analog, which potently inhibits CLR/RAMP1 receptor signaling, forms gels at a 6–20% level. Screening of ADE651 variants indicated that residues at the junctional region of this chimeric peptide are important for gaining the gel-forming capability. Gel-formation significantly slowed the passage of ADE651 molecules through Centricon filters. Consistently, subcutaneous injection of ADE651 gel in rats led to the sustained presence of ADE651 in circulation for >1 week. In addition, analysis of vascular blood flow in rat hindlimbs showed ADE651 significantly reduces CGRP-induced vasodilation. Because gel-forming antagonists could have direct and sustained access to target cells, ADE651 and related antagonists for CLR/RAMP receptors may represent promising candidates for targeting CGRP- and/or adrenomedullin-mediated headaches in migraine patients.

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Section: Discussionmentioning

confidence: 99%

Gel-forming antagonist provides a lasting effect on CGRP-induced vasodilation

Chang

Cai²,

Hsu³

2022

Front. Pharmacol.

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“…This outcome was quantified with the use of the migraine treatment optimization questionnaire-4 (mTOQ-4), which is a validated self-report questionnaire used to assess the optimization of acute treatment in persons with migraine ranging from 0 to 8 and higher scores indicating better acute medication optimization [19]. For the purposes of the current analysis, the acute treatment optimization grouping was merged to "poorly optimized" ("very poor" (score 0) and "poor" (score 1-5) groups), "optimized" ("moderate" (score 6-7) and "maximal" categories (score 8)), as this was previously applied elsewhere [20]; (ii) proportion of individual hypersensitivity symptoms accompanying headache [21], including osmophobia (dislike or aversion to smell or odors), photophobia (sensitivity or aversion to light), phonophobia (sensitivity or aversion to sounds), nausea/vomiting (urge to vomit/forceful ejection of the contents of the stomach through the mouth) and allodynia, i.e., pain generated after applying a non-noxious stimulus. For this cluster of the analysis, patients also provided numerical data concerning the changes in the average days with the specific symptoms between followups; (iii) proportion of individual prodromal symptoms (premonitory symptoms that often precede a migraine attack), including mood changes, yawning, somnolence, drowsiness, food craving, neck stiffness and fatigue [22]; and (iv) presence of triggers followed by headache (endogenous or exogenous stimuli that lower the threshold for the onset of an attack in migraine-predisposed patients), including stress, irregular sleep schedule, specific food consumption, alcohol/caffeine intake, weather changes, dehydration and also luminous and olfactory stimuli [23].…”

Section: Methodsmentioning

confidence: 99%

Nine-Month Continuous Fremanezumab Prophylaxis on the Response to Triptans and Also on the Incidence of Triggers, Hypersensitivity and Prodromal Symptoms of Patients with High-Frequency Episodic Migraine

Dermitzakis,

Vikelis,

Xiromerisiou

et al. 2024

JCM

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Objective: To investigate whether the incidence of triggers, prodromal symptoms, hypersensitivity symptoms accompanying headache and responses to triptans were modified during a continuous 9-month fremanezumab therapy for migraine prophylaxis. Patients and methods: We studied 63 patients with high-frequency episodic migraine (HFEM). Enrolled patients received fremanezumab for nine consecutive months before defining the response rates and being stratified into treatment responders (≥50–74% reduction in monthly headache days (MHDs)), super responders (≥75%), partial non-responders (<50%) and super non-responders (<30%). Through headache diaries, patients provided data in order to document the impact of fremanezumab on the incidence of triggers, associated symptoms followed by headache and response to triptans (the use of the migraine treatment optimization questionnaire-4 (mTOQ-4)) during the 9-month treatment period. Results: Fremanezumab had early (after 3 monthly cycles) beneficial effects on the response to triptans in the majority of responders with relevant increases in mTOQ-4 scoring, but also in half of partial non-responders. A significant reduction in median days with migraine-associated symptoms was seen in responders after 6 months of therapy with fremanezumab, mostly for osmophobia, photophobia, phonophobia and nausea/vomiting, but partial non-responders also benefited. Likewise, the incidence of self-reported prodromal symptoms was significantly reduced in responders and was modestly diminished in partial non-responders. Triggers remained unaffected in both responders and non-responders. Conclusions: Fremanezumab given for at least 6–9 months may exert neuromodulatory effects in the migraine brain. These effects could result both in the inhibition of migraine chronification, but also in the diminishing of the magnitude of migraine-associated symptoms, mostly in responders and in partial non-responders.

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“…Efficacy was maintained up to week 48 (year 1), with a significant reduction in the MMDs after the second (weeks [13][14][15][16][17][18][19][20][21][22][23][24], third (weeks [25][26][27][28][29][30][31][32][33][34][35][36], and fourth (weeks 37-48) infusions (52). Overall, the percentage of patients with a ≥ 50% or ≥ 75% reduction in MMDs up to week 48 was higher with eptinezumab than with placebo.…”

Section: Episodic Migrainementioning

confidence: 99%

“…During recent months, a large number of results from post-hoc analyses of data from eptinezumab pivotal trials (17,18) has been published (19)(20)(21)(22)(23)(24)(25)(26)(27)(28)(29)(30), together with primary and post-hoc results from the DELIVER trial (31)(32)(33)(34). Also, numerous clinical trials on eptinezumab are currently being conducted (35)(36)(37)(38)(39)(40)(41)(42).…”

Section: Introductionmentioning

confidence: 99%

Eptinezumab for the preventive treatment of episodic and chronic migraine: a narrative review

Irimia,

Santos-Lasaosa,

Pozo-Rosich

et al. 2024

Front. Neurol.

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Eptinezumab, a monoclonal antibody that targets calcitonin gene-related peptide (CGRP), was recently approved in Europe for the prophylactic treatment of migraine in adults who have at least four migraine days a month. Eptinezumab is administered by intravenous infusion every 12 weeks. During recent months, a considerable amount of evidence from eptinezumab trials has been published. The aim of this review is to describe the existing evidence on the tolerability, safety and efficacy of eptinezumab in patients with migraine. Data from randomized (PROMISE-1, PROMISE-2, RELIEF and DELIVER) and open-label (PREVAIL) phase 3 clinical trials have demonstrated the favorable effect of eptinezumab in migraine symptoms from first day of treatment. These studies showed that eptinezumab results in an overall reduction in mean monthly migraine days (MMDs), increases in the ≥50% and ≥ 75% migraine responder rates (MRRs) and improvements in patient-reported outcome measures in both patients with episodic migraine (EM) and with chronic migraine (CM), including patients who failed previous preventive treatments. The RELIEF trial also showed that eptinezumab, within 2 h of administration, reduced headache pain, migraine-associated symptoms and acute medication use when administered during a migraine attack. Eptinezumab benefits manifested as early as day 1 after dosing and with the subsequent doses lasted up to at least 2 years. Treatment-emergent adverse events reported by ≥2% of patients included upper respiratory tract infection and fatigue. Current evidence demonstrates that eptinezumab has a potent, fast-acting, sustained migraine preventive effect in patients with EM and CM. Eptinezumab has also shown to be well tolerated, supporting its use in the treatment of patients with migraine and inclusion in the current migraine therapeutic options.

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Optimization of acute medication use following eptinezumab initiation during a migraine attack: post hoc analysis of the RELIEF study

Cited by 6 publications

References 27 publications

Gel-forming antagonist provides a lasting effect on CGRP-induced vasodilation

Gel-forming antagonist provides a lasting effect on CGRP-induced vasodilation

Nine-Month Continuous Fremanezumab Prophylaxis on the Response to Triptans and Also on the Incidence of Triggers, Hypersensitivity and Prodromal Symptoms of Patients with High-Frequency Episodic Migraine

Eptinezumab for the preventive treatment of episodic and chronic migraine: a narrative review

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