Safety findings from Phase 3 lasmiditan studies for acute treatment of migraine: Results from SAMURAI and SPARTAN

John H Krege, Paul B Rizzoli, Emily Liffick, Erin G Doty, Sherie A Dowsett, Jianing Wang, Andrew S Buchanan, John H Krege, Paul B Rizzoli, Emily Liffick, Erin G Doty, Sherie A Dowsett, Jianing Wang, Andrew S Buchanan

Abstract

Background: We assessed the safety profile of lasmiditan, a selective 5-HT1F receptor agonist without vasoconstrictive activity being developed as an acute therapy for migraine.

Methods: SAMURAI and SPARTAN were Phase 3 double-blind studies of patients with migraine, randomized to oral lasmiditan 50 mg (SPARTAN only), 100 mg, 200 mg, or placebo to be taken within 4 hours of onset of migraine pain. Safety data from the studies were integrated. Treatment-emergent adverse events (occurring within 48 hours of first dose) were considered in the analyses.

Results: The safety population comprised 1262 patients assigned placebo, and 654, 1265, and 1258 assigned lasmiditan 50 mg, 100 mg, and 200 mg, respectively. There were no deaths; serious adverse events were reported for seven patients (placebo, n = 2 [0.2%]; lasmiditan 50 mg, n = 1 [0.2%]; lasmiditan 100 mg, n = 1 [0.2%]; lasmiditan 200 mg, n = 3 [0.2%]). Patients reporting ≥ 1 treatment-emergent adverse events were: Placebo, n = 174 (13.5%); lasmiditan 50 mg, n = 166 (25.4%); lasmiditan 100 mg, n = 458 (36.2%); and lasmiditan 200 mg, n = 510 (40.6%). Treatment-emergent adverse events were generally mild or moderate in severity. The most common treatment-emergent adverse events with lasmiditan were dizziness, paresthesia, somnolence, fatigue, nausea, muscular weakness and hypoesthesia. There were no ischemic events.

Conclusions: As a centrally-penetrant drug, lasmiditan use was associated with neurologic treatment-emergent adverse events; most were mild or moderate in severity and self-limiting.

Trial registration at clinicaltrials.gov: SAMURAI (NCT02439320) and SPARTAN (NCT02605174).

Keywords: Lasmiditan; phase 3; safety.

Figures

Figure 1.
Figure 1.
Association between the presence/absence of common TEAEs and outcomes at 2 hours in patients who took lasmiditan. For five most common TEAEs (common TEAES with >100 events in total). Note: Yes/No on Figure refers to presence/absence of the common TEAE. MBS: most bothersome symptom; PGIC: Patient Global Impression of Change.

References

    1. Vila-Pueyo M. Targeted 5-HT1F therapies for migraine. Neurotherapeutics 2018; 15: 291–303.
    1. Kuca B, Silberstein SD, Wietecha L, et al. Lasmiditan is an effective acute treatment for migraine: A phase 3 randomized study. Neurology 2018; 91: e2222–e2232.
    1. Goadsby PJ LL, Dennehy EB, Kuca B, et al. Phase 3 randomized, placebo-controlled, double-blind study of lasmiditan for acute treatment of migraine. Brain. Epub ahead of print 27 May 2019. DOI: 10.1093/brain/awz134.
    1. Guy W. Clinical global impression. In: ECDEU assessment manual for psychopharmacology – revised. Rockville, MD: US Department of Health, Education and Welfare, pp.218–222. (1976, accessed 28 May 2019).
    1. Goff DC, Lloyd-Jones DM, Bennett G, et al. 2013 ACC/AHA guideline on the assessment of cardiovascular risk: A report of the American College of Cardiology/American Heart Association Task Force on Practice Guidelines. Circulation 2014; 129: S49–S73.
    1. American Heart Association resource page. Understanding blood pressure readings: Know your numbers, (2017, accessed 1 May 2019).
    1. Dunkley E, Isbister G, Sibbritt D, et al. The Hunter Serotonin Toxicity Criteria: Simple and accurate diagnostic decision rules for serotonin toxicity. QJM 2003; 96: 635–642.
    1. Tepper SK, Krege J, Lombard L, et al. Characterization of dizziness after lasmiditan: Findings from the SAMURAI and SPARTAN acute migraine treatment randomized trials. Headache. (in press).
    1. Pilgrim A, Dussault B, Rupniak NM, et al. col-144, an orally bioavailable selective 5-HT1F receptor agonist for acute migraine therapy: Po34. Cephalalgia 2009; 29: 24–25.
    1. Nilsson T, Longmore J, Shaw D, et al. Contractile 5-HT1B receptors in human cerebral arteries: Pharmacological characterization and localization with immunocytochemistry. Brit J Pharmacol 1999; 128: 1133–1140.
    1. Neeb L, Meents J, Reuter U. 5-HT 1F receptor agonists: A new treatment option for migraine attacks? Neurotherapeutics 2010; 7: 176–182.
    1. Rubio-Beltrán E, Labastida-Ramírez A, Villalon CM, et al. Is selective 5-HT1F receptor agonism an entity apart from that of the triptans in antimigraine therapy? Pharmacol Ther 2018; 186: 88–97.
    1. Hippisley-Cox J, Coupland C, Brindle P. Development and validation of QRISK3 risk prediction algorithms to estimate future risk of cardiovascular disease: Prospective cohort study. BMJ 2017; 357: j2099.
    1. Mahmoud AN, Mentias A, Elgendy AY, et al. Migraine and the risk of cardiovascular and cerebrovascular events: A meta-analysis of 16 cohort studies including 1 152 407 subjects. BMJ Open 2018; 8: e020498.
    1. Humphrey P, Feniuk W, Perren MJ, et al. Serotonin and migraine. Ann NY Acad Sci 1990; 600: 587–598.
    1. Mitsikostas D, Tfelt-Hansen P. Targeting to 5-HT1F receptor subtype for migraine treatment: Lessons from the past, implications for the future. Cent Nerv Syst Agents Med Chem 2012; 12: 241–249.
    1. Valeant Pharmaceuticals North America. D.H.E. 45® (dihydroergotamine mesylate) injection, USP, (2008, accessed 1 May 2019).
    1. GlaxoSmithKline. IMITREX (sumatriptan succinate) tablets, for oral use. Highlights of prescribing information, (2017, accessed 1 May 2019).
    1. Depomed Inc. CAMBIA® (diclofenac potassium), for oral solution. Highlights of prescribing information, (2017, accessed 1 May 2019).
    1. GlaxoSmithKline. AMERGE® (naratriptan hydrochloride) tablets, for oral use, (2016, accessed 1 May 2019).
    1. Merck & Co, Inc. MAXALT (rizatriptan benzoate) tablets, for oral use, (2011, accessed 1 May 2019).
    1. Ferrari MD, Roon KI, Lipton RB, et al. Oral triptans (serotonin 5-HT(1B/1D) agonists) in acute migraine treatment: A meta-analysis of 53 trials. Lancet 2001; 358: 1668–1675.

Source: PubMed

Sponsors et collaborateurs

Les conditions médicales

Interventions en matière de drogue

3
S'abonner