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View and ReviewArq. Neuro-Psiquiatr. 81 (12) Dec 2023https://doi.org/10.1055/s-0043-1777723   copy

The history and rationale of the development of new drugs for migraine treatment

A história e os fundamentos do desenvolvimento de novos medicamentos para o tratamento da migrânea

Authorship SCIMAGO INSTITUTIONS RANKINGS

Abstract

Migraine is one of the most prevalent and disabling diseases in the world. Migraine attack treatments and prophylactic treatments of this disease are essential to lessen its individual, social, and economic impact. This is a narrative review of the main drugs used for treating migraine, as well as the experimental models and the theoretical frameworks that led to their development. Ergot derivatives, triptans, non-steroid anti-inflammatory drugs, tricyclic antidepressants, beta-blockers, flunarizine, valproic acid, topiramate, onabotulinumtoxin A, ditans, monoclonal antibodies against CGRP and its receptor, and gepants are discussed. Possible therapeutic targets for the development of new drugs that are under development are also addressed. Many of the drugs currently in use for treating migraine were developed for the treatment of other diseases, but have proven effective for the treatment of migraine, expanding knowledge about the disease. With a better understanding of the pathophysiology of migraine, new drugs have been and continue to be developed specifically for the treatment of this disease.

Keywords
Headache; Migraine Disorders; Drug Development; Therapeutics; Pathophysiology

Resumo

A migrânea é uma das doenças mais prevalentes e incapacitantes do mundo. O tratamento da crise de migrânea e o tratamento profilático da doença são essenciais para diminuir o seu impacto individual, social e econômico. Este é um artigo de revisão narrativa. Revisamos as principais drogas usadas para a migrânea e os modelos experimentais e referenciais teóricos que levaram ao seu desenvolvimento. Foram abordados os derivados do ergot, triptanas, anti-inflamatórios não hormonais, antidepressivos tricíclicos, betabloqueadores, flunarizina, ácido valproico, topiramato, toxina onabotulínica do tipo A, os ditans, anticorpos monoclonais contra o CGRP e seu receptor e os gepants. Também foram abordados possíveis alvos terapêuticos para o desenvolvimento de novas drogas e drogas que estão em desenvolvimento para o tratamento da migrânea. Muitas das drogas usadas atualmente foram desenvolvidas para o tratamento de outras doenças e se mostraram efetivas para o tratamento da migrânea. Essas ajudaram a ampliar o conhecimento sobre a doença. Com o melhor entendimento da fisiopatologia da migrânea, novas drogas foram e estão sendo desenvolvidas especificamente para o tratamento dessa doença.

Palavras-chave
Cefaleia; Transtornos de Enxaqueca; Desenvolvimento de Medicamentos; Terapêutica; Fisiopatologia

INTRODUCTION

In addition to being one of the most prevalent human diseases, affecting 14% of the world's population,11 Stovner LJ, Hagen K, Linde M, Steiner TJ. The global prevalence of headache: an update, with analysis of the influences of methodological factors on prevalence estimates. J Headache Pain 2022;23(01):34 migraine is considered the second most disabling disease in the world.22 Steiner TJ, Stovner LJ, Jensen R, Uluduz D, Katsarava ZLifting The Burden: the Global Campaign against Headache. Migraine remains second among the world's causes of disability, and first among young women: findings from GBD2019. J Headache Pain 2020;21(01):137 Indeed, migraine is the leading cause of disability among non-communicable chronic diseases in Brazil as well as most other countries of the world.33 Peres MFP, Queiroz LP, Rocha-Filho PS, Sarmento EM, Katsarava Z, Steiner TJ. Migraine: a major debilitating chronic non-communicable disease in Brazil, evidence from two national surveys. J Headache Pain 2019;20(01):85 Its high prevalence, coupled with the disability it causes, results in a great individual, social, and economic impact. Improving its treatment is therefore a key aspect to reduce this burden.22 Steiner TJ, Stovner LJ, Jensen R, Uluduz D, Katsarava ZLifting The Burden: the Global Campaign against Headache. Migraine remains second among the world's causes of disability, and first among young women: findings from GBD2019. J Headache Pain 2020;21(01):137,33 Peres MFP, Queiroz LP, Rocha-Filho PS, Sarmento EM, Katsarava Z, Steiner TJ. Migraine: a major debilitating chronic non-communicable disease in Brazil, evidence from two national surveys. J Headache Pain 2019;20(01):85

Information on medieval-era treatments of migraine is scarce. Most remedies prescribed for migraine attacks at that time were herbal medicines, such as nettles, laurel, rue, and mustard. The rationale for prescribing these agents was speculative rather than rational.44 Foxhall K. The “Beating of Hammers”: Classical and medieval approaches to hemicrania. In: Foxhall K, ed. Migraine: a history.. Baltimore: Johns Hopkins University Press; 2019 Post-medieval eras did not differ much regarding therapeutic approaches, which sometimes kept far from scientific or observational bases.44 Foxhall K. The “Beating of Hammers”: Classical and medieval approaches to hemicrania. In: Foxhall K, ed. Migraine: a history.. Baltimore: Johns Hopkins University Press; 2019

Despite being a disease known since antiquity, we can consider that the “scientific” phase of migraine treatment began in the twentieth century. Some of the drugs we use today were discovered by chance, being developed for the treatment of other diseases, and later proved effective for the treatment of migraine. Many of these early drugs were important in advancing our knowledge of disease mechanisms. From the end of the 20th century to the beginning of the 21st century, a better understanding of the pathophysiology of migraine allowed the development of drugs that were specifically designed for the treatment of migraine.

This article aims to review the discoveries of the main drugs used for the treatment of migraine and the pathophysiological models that led to their development. It also addresses possible therapeutic targets for the development of new drugs. Greater emphasis is placed on drugs that represented advances in treatment when they were incorporated into the therapeutic arsenal for migraine, as well as on drugs that have helped to better understand the pathophysiology of the disease. Treatments restricted to emergency rooms are out of the scope of this paper.

MIGRAINE PATHOPHYSIOLOGY

Experimental methods in migraine began when Harold Wolff and colleagues measured the pulsations of the temporal artery during a migraine attack and recorded the effects of ergotamine on temporal artery diameter.55 Graham JR, Wolff HG. Mechanism of migraine headache and action of ergotamine tartrate. Arch Neur Psych 1938;39: 737–763 A consequence of their report was the consolidation of the concept of migraine as a vascular rather than a neurogenic disease. This model was coined the “vascular model” which has been dominant in explaining the pathophysiology of migraine during most of the second half of the twentieth century.

The discovery of cortical spreading depression (CSD) was an important milestone in demonstrating the involvement of the cerebral cortex in the pathophysiology of migraine. Aristides Leão, a Brazilian researcher, first described CSD while in Harvard,66 Leao AAP. Spreading depression of activity in the cerebral cortex. J Neurophysiol 1944;7:359–390 and Lashley, while describing his own aura, found it to share temporal features with CSD.77 Lashley KS. Patterns of cerebral integration indicated by the scotomas of migraine. Arch NeurPsych 1941;46:331–339 After that, Martin Lauritzen studied the changes of blood flow in the brain during a migraine attack and linked its changes to the CSD phenomenon.88 Lauritzen M, Jørgensen MB, Diemer NH, Gjedde A, Hansen AJ. Persistent oligemia of rat cerebral cortex in the wake of spreading depression. Ann Neurol 1982;12(05):469–474 Jes Olesen also examined blood flow during a migraine attack, and the effects of nitric oxide and calcitonin gene-related peptide (CGRP) pathways. It was proven that during CSD, the brain hypoperfusion phase was followed by a hyperperfusion phase before its flow returned to normality.99 Olesen J, Larsen B, Lauritzen M. Focal hyperemia followed by spreading oligemia and impaired activation of rCBF in classic migraine. Ann Neurol 1981;9(04):344–352 Thus, CSD is recognized as the pathophysiological substrate of migraine aura.

Moscowitz further advanced our understanding of migraine by disclosing the complex relationships between the cortex, the trigeminal nuclei, and the cranial vasculature.1010 Bolay H, Reuter U, Dunn AK, Huang Z, Boas DA, Moskowitz MA. Intrinsic brain activity triggers trigeminal meningeal afferents in a migraine model. Nat Med 2002;8(02):136–142 Conversely and later on, Weiller et al. suggested migraine attacks to start in the brainstem.1111 Weiller C, May A, Limmroth V, et al. Brain stem activation in spontaneous human migraine attacks. Nat Med 1995;1(07): 658–660 These views are now challenged by Arne May,1212 Mehnert J, Fischer-Schulte L, May A. Aura phenomena do not initiate migraine attacks-Findings from neuroimaging. Headache 2023;63(08):1040–1044; Epub ahead of print. Doi: 10.1111/head.14597
https://doi.org/10.1111/head.14597... who revealed hypothalamic activation to occur two days before a migraine attack. He proposed migraine aura to be an epiphenomenon unrelated to headache. Andrew Charles further discussed this and was in support.1313 Charles A. Aura is a symptom of a migraine attack, not its cause. Headache 2023;63(08):1029–1030; Epub ahead of print. Doi: 10.1111/HEAD.14623
https://doi.org/10.1111/HEAD.14623...

Lars Edvinsson was the first to show CGRP to colocalize with substance P in the CNS and in the trigeminovascular system (at the neurovascular junctions) and propose the role of CGRP in migraine as well as having an important role for CGRP in intracranial arteries and pial arteriolar vasodilation. Later, Edvinsson and Goadsby identified CGRP as the neuropeptide released in the jugular vein in both cat and human models of migraine. Their efforts helped to place on the spotlight the evidence of a neural generation of migraine.1414 Edvinsson L, Haanes KA, Warfvinge K, Krause DN. CGRP as the target of new migraine therapies - successful translation from bench to clinic. Nat Rev Neurol 2018;14(06):338–350

A migraine attack can have at most four phases: prodrome, aura, headache phase, and postdrome. Not all individuals have all phases and they do not always occur in all attacks.1515 Sampaio Rocha-Filho PA, Gherpelli JLD. Premonitory and Accompanying Symptoms in Childhood Migraine. Curr Pain Headache Rep 2022;26(02):151–163 Although much progress has been made in knowledge about the pathophysiology of migraine with the recognition of the participation of the trigeminovascular system, the hypothalamus, the cerebral cortex, and the brain stem, it is still not known which mechanism is responsible for initiating the attack. It is possible that more than a single pathway is operative in different individuals or even in the same subject in attacks with different phenotypes.

EXPERIMENTAL MODELS OF MIGRAINE: INSIGHTS INTO PATHOPHYSIOLOGY AND THERAPEUTICS

The chemical-induced models of migraine involve the administration of compounds that trigger migraine-like symptoms, such as nitric oxide donors (e.g., nitroglycerin) and CGRP.1616 Greco R, Demartini C, De Icco R, Martinelli D, Putortì A, Tassorelli C. Migraine neuroscience: from experimental models to target therapy. Neurol Sci 2020;41(Suppl 2):351–361 Both models can induce headaches and migraine-like symptoms not only in animals but also in humans.1616 Greco R, Demartini C, De Icco R, Martinelli D, Putortì A, Tassorelli C. Migraine neuroscience: from experimental models to target therapy. Neurol Sci 2020;41(Suppl 2):351–361,1717 Tardiolo G, Bramanti P, Mazzon E. Migraine: Experimental models and novel therapeutic approaches. Int J Mol Sci 2019; 20(12):2932 Additionally, electrophysiological testing in humans can also be used to study the effects of antimigraine drugs in the evoked responses of migraine subjects.1616 Greco R, Demartini C, De Icco R, Martinelli D, Putortì A, Tassorelli C. Migraine neuroscience: from experimental models to target therapy. Neurol Sci 2020;41(Suppl 2):351–361,1717 Tardiolo G, Bramanti P, Mazzon E. Migraine: Experimental models and novel therapeutic approaches. Int J Mol Sci 2019; 20(12):2932

Animal models of CSD provide an opportunity to test the effects of antimigraine drugs on the mechanisms of migraine aura.1616 Greco R, Demartini C, De Icco R, Martinelli D, Putortì A, Tassorelli C. Migraine neuroscience: from experimental models to target therapy. Neurol Sci 2020;41(Suppl 2):351–361,1717 Tardiolo G, Bramanti P, Mazzon E. Migraine: Experimental models and novel therapeutic approaches. Int J Mol Sci 2019; 20(12):2932

Electrical stimulation of the superior sagittal sinus1818 Buzzi MG, Carter WB, Shimizu T, Heath H III, Moskowitz MA. Dihydroergotamine and sumatriptan attenuate levels of CGRP in plasma in rat superior sagittal sinus during electrical stimulation of the trigeminal ganglion. Neuropharmacology 1991;30(11): 1193–1200 may be used to study the effect of antimigraine drugs on neuropeptide levels in the jugular vein,1919 Goadsby PJ, Edvinsson L, Ekman R. Release of vasoactive peptides in the extracerebral circulation of humans and the cat during activation of the trigeminovascular system. Ann Neurol 1988;23 (02):193–196 as well as to study not only the activation of neurons at the nucleus trigeminalis caudalis but also the effect of antimigraine drugs and in the neuronal activity through electrophysiological records and c-fos expression.2020 Hoskin KL, Kaube H, Goadsby PJ. Central activation of the trigeminovascular pathway in the cat is inhibited by dihydroergotamine. A c-Fos and electrophysiological study. Brain 1996; 119(Pt 1):249–256

Genetically modified animal models, such as knockout or transgenic mice or rats, targeting genes associated with migraine susceptibility, have provided insights into the role of specific genes in migraine pathophysiology, and may lead to the identification of novel therapeutic targets.1616 Greco R, Demartini C, De Icco R, Martinelli D, Putortì A, Tassorelli C. Migraine neuroscience: from experimental models to target therapy. Neurol Sci 2020;41(Suppl 2):351–361

In vitro models include cortical slices, cell cultures, and trigeminal system models. These models, if kept in a controlled environment, allow researchers to expose them to different migraine triggers, and to study the impact of antimigraine drugs/candidates.1212 Mehnert J, Fischer-Schulte L, May A. Aura phenomena do not initiate migraine attacks-Findings from neuroimaging. Headache 2023;63(08):1040–1044; Epub ahead of print. Doi: 10.1111/head.14597
https://doi.org/10.1111/head.14597... ,1616 Greco R, Demartini C, De Icco R, Martinelli D, Putortì A, Tassorelli C. Migraine neuroscience: from experimental models to target therapy. Neurol Sci 2020;41(Suppl 2):351–361

Though models are imperfect, they represent our best attempts at approximating human migraine to seek relief for our patients' suffering.

Migraine mechanisms involve multipoint complex pathways rather than a single circuitry. There is significant interindividual variability, even among those presenting similar phenotypes.

Figure 1 presents a simplified diagram illustrating the neurochemical systems upon which antimigraine drugs exert their therapeutic effect.

Figure 1
Neuropharmacology of antimigraine treatments. Abbreviatitons: GABA, gamma-aminobutyric acid; 5-HT 1D, 5-HT1F, 5-HT1A, serotonin neuronal receptors; 5-HT1B, serotonin neurovascular receptors; NSAID, non-steroidal antiinflammatory drugs; α2, alpha-2 adrenergic receptors; β2, beta-2 adrenergic receptors. Modified from: Sarrouilhe et al.119119 Sarrouilhe D, Dejean C, Mesnil M. Involvement of gap junction channels in the pathophysiology of migraine with aura. Front Physiol 2014;5:78

THE ANTIMIGRAINE DRUGS

Drugs for the treatment of migraine attacks

Ergot alkaloids

Modern treatment of migraine, although empirical, used to involve the use of ergot alkaloids, initially described by Eulenburg in 1808,2121 Eulenburg A. Lehrbuch der Funktionellen Nervenkrankheiten.. Berlin: August Hirschwald; 1871 but only in 1928 two case series were reported independently by Tzanck and by Trautmann.2222 Tzanck MAp. Bull Soc Méd Hosp Paris 1928;52:513 In 1948, caffeine was added to oral ergots, enhancing their action.2323 Friedman AP, Brenner C. Treatment of the migraine attack. Am Pract Dig Treat 1948;2(07):467–470

Ten years later, Doepfner and Cerletti postulated that ergot alkaloids act through an anti-serotonin effect,2424 Doepfner W, Cerletti A. Comparison of lysergic acid derivatives and antihistamines as inhibitors of the edema provoked in the rat's paw by serotonin. Int Arch Allergy Appl Immunol 1958;12 (1-2):89–97 a view shared by Sicuteri, who tested the efficacy of methysergide in the prophylaxis of migraine and cluster headaches.2525 Sicuteri F. Prophylactic and therapeutic properties of 1-methyllysergic acid butanolamide in migraine. Int Arch Allergy Appl Immunol 1959;15:300–307 It was only in 1992 that Müller-Schweinitzer postulated that ergot alkaloids' effects in migraine were related to their agonistic 5-HT1B receptor and 5-HT1D effect rather than their 5-HT7 receptor antagonism.2626 Müller-Schweinitzer E. Ergot alkaloids in migraine: Is the effect via 5-HT receptors? In: Olesen J, Saxena PR, eds. 5-Hydroxytryptamine Mechanisms in Primary Headaches.. New York: Raven; 1992:297–304

Methysergide was banned worldwide, due to the risk of retroperitoneal fibrosis, an effect that nowadays could be easily screened with periodic point-of-care retroperitoneal ultrasounds. Ergotamine is still available in a few countries, parenteral dihydroergotamine is available in North America, and oral dihydroergotamine is no longer available in Europe, with its consumption seeming to decline worldwide.

Non-steroid anti-inflammatory drugs (NSAIDs), isometheptene mucate, metamizole and over-the-counter (OTC) analgesics

Tolfenamic acid, in 1979 was the first NSAIDs to be tested for treating migraine.2727 Hakkarainen H, Vapaatalo H, Gothoni G, Parantainen J. Tolfenamic acid is as effective as ergotamine during migraine attacks. Lancet 1979;2(8138):326–328 From the following years to the first decade of the 21st century, several NSAIDs were tried for migraine, the larger trials involving aspirin, diclofenac, and ibuprofen.2828 Migraine AM. N Engl J Med 2020;383:1866–1876 All of them proved effective in treating migraine attacks. For choosing one of the several NSAIDs available, it is advisable to take into account their time to peak (Tmax), half-life (T1/2), absorption, and tolerability. Isometheptene mucate underwent a few trials, always combined with other drugs.2929 Yuill GM, Swinburn WR, Liversedge LA. A double-blind crossover trial of isometheptene mucate compound and ergotamine in migraine. Br J Clin Pract 1972;26(02):76–79 Metamizole, a quite popular drug in some Latin American and European countries at the end of the former century, had its efficacy against migraine attacks proven only in 2001.3030 Tulunay FC, Ergün H, Gülmez SE, et al. The efficacy and safety of dipyrone (Novalgin) tablets in the treatment of acute migraine attacks: a double-blind, cross-over, randomized, placebo-controlled, multi-center study. Funct Neurol 2004;19(03): 197–202 OTC were proven to control migraine attacks in a timely manner with the former drugs. Their use, however, while still popular, remains limited to milder migraine attacks.3131 Goldstein J, Silberstein SD, Saper JR, Ryan RE Jr, Lipton RB. Acetaminophen, aspirin, and caffeine in combination versus ibuprofen for acute migraine: results from a multicenter, double-blind, randomized, parallel-group, single-dose, placebo-controlled study. Headache 2006;46(03):444–453 Of the abovementioned medications, only isometheptene mucate was primarily used for treating migraine attacks.

Humphrey, the triptans and their rationale

The first study on the 5-HT receptors co-authored by Patrick Humphrey was published in 1974.3232 Humphrey PPA, Feniuk W, Perren MJ, et al. GR43175, a selective agonist for the 5-HT1-like receptor in dog isolated saphenous vein. Br J Pharmacol 1988;94(04):1123–1132 Fourteen years later, he described the discovery of a selective 5-HT1B1D receptor agonist, that would dramatically change migraine treatment protocols.3333 Edvinsson L, Villalón CM, MaassenVanDenBrink A. Basic mechanisms of migraine and its acute treatment. Pharmacol Ther 2012;136(03):319–333 Triptans pharmacological effect is exerted through activation of vascular smooth muscle 5-HT 1B receptor (vasoconstriction) and presynaptic 5-HT 1D receptors (lessening trigeminovascular neuron firing of CGRP).3333 Edvinsson L, Villalón CM, MaassenVanDenBrink A. Basic mechanisms of migraine and its acute treatment. Pharmacol Ther 2012;136(03):319–333,3434 González-Hernández A, Marichal-Cancino BA, MaassenVanDen-Brink A, Villalón CM. Serotonergic modulation of neurovascular transmission: A focus on prejunctional 5-HT receptors/mechanisms. Biomedicines 2023;11(07):1864

Shortly thereafter, three triptans were launched in the market: sumatriptan, referential triptan, zolmitriptan, and naratriptan. While zolmitriptan's pharmacological profile resembled that of sumatriptan, naratriptan differed due to its slower onset of action, and lower potency but longer half-life.3535 Cameron C, Kelly S, Hsieh SC, et al. Triptans in the acute treatment of migraine: A systematic review and network meta-analysis. Headache 2015;55(Suppl 4):221–235

It did not take a long time for the development of a new generation of triptans, namely rizatriptan, eletriptan, frovatriptan, and almotriptan.3535 Cameron C, Kelly S, Hsieh SC, et al. Triptans in the acute treatment of migraine: A systematic review and network meta-analysis. Headache 2015;55(Suppl 4):221–235 Of these, rizatriptan is the one with the shorter Tmax, and eletriptan the one who bears the best results.3535 Cameron C, Kelly S, Hsieh SC, et al. Triptans in the acute treatment of migraine: A systematic review and network meta-analysis. Headache 2015;55(Suppl 4):221–235 Triptans may be administered as oral tablets, as dispersive wafers, or atomized intranasally, and sumatriptan is still the only triptan to have a subcutaneous presentation.3535 Cameron C, Kelly S, Hsieh SC, et al. Triptans in the acute treatment of migraine: A systematic review and network meta-analysis. Headache 2015;55(Suppl 4):221–235 A transdermic product reached the market3636 Vikelis M, Mitsikostas DD, Rapoport AM. Sumatriptan iontophoretic transdermal system for the acute treatment of migraine. Pain Manag (Lond) 2014;4(02):123–128 but was discontinued due to safety issues.3737 Loder EW, Rayhill M, Burch RC. Safety problems with a transdermal patch for migraine: lessons from the development, approval, and marketing process. Headache 2018;58(10):1639–1657

Since 5-HT1B receptors are located mainly on meningeal vessels, triptans have a tolerability profile far better than ergot alkaloids but are still contraindicated in patients with uncontrolled hypertension, and cardiac and/or peripheral artery disease. Triptans are well tolerated, and their relative risk for an adverse event ranges from 0.81 a 1.23.3535 Cameron C, Kelly S, Hsieh SC, et al. Triptans in the acute treatment of migraine: A systematic review and network meta-analysis. Headache 2015;55(Suppl 4):221–235,3838 Tfelt-Hansen P, De Vries P, Saxena PR. Triptans in migraine: a comparative review of pharmacology, pharmacokinetics and efficacy. Drugs 2000;60(06):1259–1287 A short-lasting cluster of symptoms such as throat and chest tightness and tingling, also known as “triptan sensation” may occur, and, in spite of its benign nature, it may be misinterpreted as heart-related and frighten patients,3535 Cameron C, Kelly S, Hsieh SC, et al. Triptans in the acute treatment of migraine: A systematic review and network meta-analysis. Headache 2015;55(Suppl 4):221–235,3838 Tfelt-Hansen P, De Vries P, Saxena PR. Triptans in migraine: a comparative review of pharmacology, pharmacokinetics and efficacy. Drugs 2000;60(06):1259–1287 who should be warned about the possibility of its occurrence. Triptans are associated with less need for rescue medication, earlier return to usual activities, lower expenses with additional medications, and reduction of direct and indirect costs. Table 1 summarizes the pharmacological features of the triptans.3535 Cameron C, Kelly S, Hsieh SC, et al. Triptans in the acute treatment of migraine: A systematic review and network meta-analysis. Headache 2015;55(Suppl 4):221–235,3838 Tfelt-Hansen P, De Vries P, Saxena PR. Triptans in migraine: a comparative review of pharmacology, pharmacokinetics and efficacy. Drugs 2000;60(06):1259–1287

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Table 1
Pharmacological and efficacy data of the triptans in the treatment of migraine attacks.2323 Friedman AP, Brenner C. Treatment of the migraine attack. Am Pract Dig Treat 1948;2(07):467–470,4444 Kuca B, Silberstein SD, Wietecha L, Berg PH, Dozier G, Lipton RBCOL MIG-301 Study Group. Lasmiditan is an effective acute treatment for migraine: A phase 3 randomized study. Neurology 2018;91(24):e2222–e2232,4747 Edvinsson L. Novel migraine therapy with calcitonin gene-regulated peptide receptor antagonists. Expert Opin Ther Targets 2007;11(09):1179–1188

Ditans and the central mechanisms of migraine: circumventing the vasoconstrictor action of triptans

Despite a favorable tolerability profile of the triptans, there were concerns regarding their vasoconstrictive action. The growing evidence on the fact that migraine was primarily a neurological disease raised the question of whether a drug with a “pure” neuronal effect could be used to treat migraine. This hypothesis led to the creation of a new class of drugs, the ditans, of which lasmiditan was the only one that reached the market.

Lasmiditan is a 5-HTF agonist. Since 5-HTF receptors are expressed mostly in neuronal membranes, lasmiditan is devoid of significant vasoconstrictive effects.3939 Nelson DL, Phebus LA, Johnson KW, et al. Preclinical pharmacological profile of the selective 5-HT1F receptor agonist lasmiditan. Cephalalgia 2010;30(10):1159–1169 Recently, a study carried out with rats showed that lasmiditan possibly also has a partial agonist at 5-HT1B/1D receptors.4040 Edvinsson JCA, Maddahi A, Christiansen IM, et al. Lasmiditan and 5-Hydroxytryptamine in the rat trigeminal system; expression, release and interactions with 5-HT1 receptors. J Headache Pain 2022;23(01):26

Its efficacy in controlling migraine attacks was proved in several pivotal trials.4141 Färkkilä M, Diener HC, Géraud G, et al; COL MIG-202 study group. Efficacy and tolerability of lasmiditan, an oral 5-HT(1F) receptor agonist, for the acute treatment of migraine: a phase 2 randomised, placebo-controlled, parallel-group, dose-ranging study. Lancet Neurol 2012;11(05):405–4134444 Kuca B, Silberstein SD, Wietecha L, Berg PH, Dozier G, Lipton RBCOL MIG-301 Study Group. Lasmiditan is an effective acute treatment for migraine: A phase 3 randomized study. Neurology 2018;91(24):e2222–e2232 Lasmiditan was better than placebo in pain freedom at 2 and 24 hours, in resolution of the most bothersome symptom and of photophobia, and in returning to normal functioning. Post-hoc analysis of subsets of participants with cardiovascular risk factors and elders proved it to be safe.4545 Martin VT, Ahmed Z, Hochstetler HM, et al. Tolerability and safety of lasmiditan treatment in elderly patients with migraine: Post hoc analyses from randomized studies. Clin Ther 2021;43 (06):1066–1078,4646 Shapiro RE, Hochstetler HM, Dennehy EB, et al. Lasmiditan for acute treatment of migraine in patients with cardiovascular risk factors: post-hoc analysis of pooled results from 2 randomized, double-blind, placebo-controlled, phase 3 trials. J Headache Pain 2019;20(01):90

Its CNS treatment-emergent side effects attributed to its lipophilicity may be a problem. Patients need warning about lasmiditan's potential to impair driving abilities.4545 Martin VT, Ahmed Z, Hochstetler HM, et al. Tolerability and safety of lasmiditan treatment in elderly patients with migraine: Post hoc analyses from randomized studies. Clin Ther 2021;43 (06):1066–1078, Table 2 summarizes the pharmacological features of lasmiditan.

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Table 2
Pharmacological and efficacy data of lasmiditan in the treatment of migraine attacks.2323 Friedman AP, Brenner C. Treatment of the migraine attack. Am Pract Dig Treat 1948;2(07):467–470,4848 González-Hernández A, Marichal-Cancino BA, MaassenVanDen-Brink A, Villalón CM. Side effects associated with current and prospective antimigraine pharmacotherapies. Expert Opin Drug Metab Toxicol 2018;14(01):25–415454 Couch JR, Hassanein RS. Amitriptyline in migraine prophylaxis. Arch Neurol 1979;36(11):695–699

Monoclonal antibodies – beyond migraine prophylaxis

In spite of initially aimed for migraine prophylaxis, CGRP-driven monoclonal antibodies development gave way to the only intravenously administered anti-CGRP monoclonal antibody, eptinezumab, tested against migraine attacks.1414 Edvinsson L, Haanes KA, Warfvinge K, Krause DN. CGRP as the target of new migraine therapies - successful translation from bench to clinic. Nat Rev Neurol 2018;14(06):338–350 Eptinezumab cost may limit its use in this indication to refractory attacks and to wealthy markets. Eptinezumab's clinical pharmacologic features can be appreciated in Table 3.

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Table 3
Pharmacological and efficacy data of the monoclonal antibodies in the prevention of migraine attacks2323 Friedman AP, Brenner C. Treatment of the migraine attack. Am Pract Dig Treat 1948;2(07):467–470,5656 https://go.drugbank.com/drugs/
https://go.drugbank.com/drugs/... 7979 Goadsby PJ, Reuter U, Hallström Y, et al. A controlled trial of erenumab for episodic migraine. N Engl J Med 2017;377(22): 2123–2132

Gepants – the new anti-CGRP small molecules to fight migraine.

Shortly after the description of the role of CGRP in migraine and far before the antimigraine mAbs, a first generation of a category of “small molecules” called gepants4747 Edvinsson L. Novel migraine therapy with calcitonin gene-regulated peptide receptor antagonists. Expert Opin Ther Targets 2007;11(09):1179–1188 - namely, telcagepant, olcegepant, MK-3207, and BI 44370 - underwent phase I and II studies, without meeting acceptable safety levels due to hepatotoxicity.4848 González-Hernández A, Marichal-Cancino BA, MaassenVanDen-Brink A, Villalón CM. Side effects associated with current and prospective antimigraine pharmacotherapies. Expert Opin Drug Metab Toxicol 2018;14(01):25–41,4949 Edvinsson L, Linde M. New drugs in migraine treatment and prophylaxis: telcagepant and topiramate. Lancet 2010;376 (9741):645–655 Almost twenty years later, a second generation of gepants reached the market. These new molecules also represented a victory in drug design and have been proven not only to be efficacious but also versatile. Of the currently available gepants, ubrogepant, rimegepant, and zavegepant were tested for aborting migraine attacks.5050 Croop R, Madonia J, Stock DA, et al. Zavegepant nasal spray for the acute treatment of migraine: A Phase 2/3 double-blind, randomized, placebo-controlled, dose-ranging trial. Headache 2022;62(09):1153–11635252 Dodick DW, Lipton RB, Ailani J, et al. Ubrogepant for the treatment of migraine. N Engl J Med 2019;381(23):2230–2241 While ubrogepant and rimegepant tabs are suited for oral intake, zavegepant was developed for intranasal administration.5050 Croop R, Madonia J, Stock DA, et al. Zavegepant nasal spray for the acute treatment of migraine: A Phase 2/3 double-blind, randomized, placebo-controlled, dose-ranging trial. Headache 2022;62(09):1153–1163,5151 Lipton RB, Croop R, Stock DA, et al. Safety, tolerability, and efficacy of zavegepant 10 mg nasal spray for the acute treatment of migraine in the USA: a phase 3, double-blind, randomised, placebo-controlled multicentre trial. Lancet Neurol 2023;22 (03):209–217 In general, their therapeutic gain for acute treatment is lower than that of the triptans, but their tolerability seems to be better, in spite of causing mild nausea. Since symptoms and disease of the central nervous system involve several biochemical and neuronal pathways, perhaps soon an anti-CGRP responsive population will become identifiable. Gepants characteristics can be appreciated in Table 4.

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Table 4
Pharmacological and efficacy data of the gepants in the treatment of migraine2323 Friedman AP, Brenner C. Treatment of the migraine attack. Am Pract Dig Treat 1948;2(07):467–470,8383 Mulleners WM, Kim BK, Láinez MJA, et al. Safety and efficacy of galcanezumab in patients for whom previous migraine preventive medication from two to four categories had failed (CONQUER): a multicentre, randomised, double-blind, placebo-controlled, phase 3b trial. Lancet Neurol 2020;19(10):814–8259494 Ashina M, Lanteri-Minet M, Pozo-Rosich P, et al. Safety and efficacy of eptinezumab for migraine prevention in patients with two-to-four previous preventive treatment failures (DE-LIVER): a multi-arm, randomised, double-blind, placebo-controlled, phase 3b trial. Lancet Neurol 2022;21(07):597–607

Figure 2 shows the timeline of studies of acute medications for migraine.

Figure 2
Timeline of the migraine acute treatment trials (1928 and ahead).

Prophylactic medications for migraine

Tricyclic antidepressants

Friedman, in 1968, linked the empirical recommendation of amitriptyline for migraine prophylaxis to the presence of depression.5353 Friedman AP. The migraine syndrome. Bull N Y Acad Med 1968; 44(01):45–62 This view was challenged by Couch and Hassanein, who in 1972 conducted the first placebo-controlled trial of this drug. Its efficacy was confirmed but its anti-migraine effect appeared to be independent of its antidepressant effect.5454 Couch JR, Hassanein RS. Amitriptyline in migraine prophylaxis. Arch Neurol 1979;36(11):695–699 Its indication however preceded any kind of preclinical study. Amitriptyline, the leading tricyclic prophylactic main features are summarized in Table 5.5555 Lampl C, Huber G, Adl J, et al. Two different doses of amitriptyline ER in the prophylaxis of migraine: long-term results and predictive factors. Eur J Neurol 2009;16(08):943–948,5656 https://go.drugbank.com/drugs/
https://go.drugbank.com/drugs/...

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Table 5
Pharmacological and efficacy data of some oral migraine prophylactic drugs2121 Eulenburg A. Lehrbuch der Funktionellen Nervenkrankheiten.. Berlin: August Hirschwald; 18713535 Cameron C, Kelly S, Hsieh SC, et al. Triptans in the acute treatment of migraine: A systematic review and network meta-analysis. Headache 2015;55(Suppl 4):221–235

Beta-adrenoceptor blockers

The first mention of propranolol as a migraine prophylactic drug pertains to Rabkin et al. who in 1966, studying its effects in subjects with angina pectoris, described a patient in whom there was a “relief of vascular headaches which relapsed on placebo”, subsiding again after reintroduction of propranolol.5757 Rabkin R, Stables DP, Levin NW, Suzman MM. The prophylactic value of propranolol in angina pectoris. Am J Cardiol 1966;18 (03):370–383

In 1971, Weber and Reinmuth published the first placebo-controlled trial on the prophylactic treatment of migraine with propranolol,5858 Weber RB, Reinmuth OM. The treatment of migraine with propranolol. Neurology 1972;22(04):366–369 and the efficacy of beta-adrenoceptor blockers in the prevention of migraine was further confirmed in other trials not only with propranolol but also with other beta-blockers lacking intrinsic sympathomimetic activity. In spite of a larger experience with propranolol, metoprolol is more selective for peripheral beta-adrenergic receptors and results in lesser platelet agregability.5959 Hedman C, Winther K, Knudsen JB. The difference between non-selective and beta 1-selective beta-blockers in their effect on platelet function in migraine patients. Acta Neurol Scand 1986; 74(06):475–478

For further pharmacological information on propranolol features in migraine refer to Table 5.5656 https://go.drugbank.com/drugs/
https://go.drugbank.com/drugs/... ,6060 Kaniecki RG. A comparison of divalproex with propranolol and placebo for the prophylaxis of migraine without aura. Arch Neurol 1997;54(09):1141–1145

Flunarizine

In 1980, Drillisch and Girke published a trial on the effects of flunarizine and cinnarizine in migraine.6161 Drillisch C, Girke W. [Results of treatment of migraine patients with cinnarizine and flunarizine]. Med Welt 1980;31(51-52): 1870–1872 After that, a double-blind trial was published a year later.6262 Louis P. A double-blind placebo-controlled prophylactic study of flunarizine (Sibelium) in migraine. Headache 1981;21(06): 235–239 Of those drugs, flunarizine became quite popular in Europe and in South America as a migraine prophylactic, but its use has been declining in the last years due to concerns regarding side effects such as somnolence, slowness, weight gain, depression, and Parkinsonism, the last mainly in post-menopausal women. Its mechanism in controlling migraine has never been fully clarified. However, it remains a useful medicine to be remembered. Its main clinical pharmacological features are displayed in Table 5.5656 https://go.drugbank.com/drugs/
https://go.drugbank.com/drugs/... ,6262 Louis P. A double-blind placebo-controlled prophylactic study of flunarizine (Sibelium) in migraine. Headache 1981;21(06): 235–239

Valproic acid

Valproic acid, a drug previously used as an inert solvent, and later found to have antiepileptic properties, was found to also have antimigraine effects. Sorensen in 1991 conducted an open-label trial that proved valproic acid to be effective in migraine prevention, after the previous unreported response of two previously refractory migraine subjects.6363 Sørensen KV. Valproate: a new drug in migraine prophylaxis. Acta Neurol Scand 1988;78(04):346–348 One year later Hering and Kuritzky published the first placebo-controlled trial,6464 Hering R, Kuritzky A. Sodium valproate in the prophylactic treatment of migraine: a double-blind study versus placebo. Cephalalgia 1992;12(02):81–84 and, later on, not only valproic acid but also its prodrugs such as sodium valproate and divalproate were proved to be effective and better tolerated than valproic acid (Table 5).5656 https://go.drugbank.com/drugs/
https://go.drugbank.com/drugs/... ,6060 Kaniecki RG. A comparison of divalproex with propranolol and placebo for the prophylaxis of migraine without aura. Arch Neurol 1997;54(09):1141–1145

A word must be said about the trials involving older migraine prophylactic drugs. Most of them were low-powered, with small numbers of subjects, and conducted in single centers, sometimes with hardly reproducible results in real life. Thus, these results should be interpreted with caution. Real-life studies may show results that differ from those of multicenter, randomized, placebo-controlled trials, the gold standard of clinical pharmacology, and reflect a combination of the intrinsic therapeutic effect with post-marketing physician- and patient-dependent placebo effects.

Topiramate

After years without novelties in migraine prophylaxis, topiramate, a drug planned for treating diabetes and launched for treating epilepsy, was found to be a migraine-preventative medication, a quality not present in every membrane-stabilizing drug. Clinical evidence led to large trials that confirmed topiramate efficacy not only for preventing lower frequency and frequent migraine but also for chronic migraine.6565 Silberstein SD, Lipton RB, Dodick DW, et al; Topiramate Chronic Migraine Study Group. Efficacy and safety of topiramate for the treatment of chronic migraine: a randomized, double-blind, placebo-controlled trial. Headache 2007;47(02):170–180,6666 Diener HC, Bussone G, Van Oene JC, Lahaye M, Schwalen S, Goadsby PJTOPMAT-MIG-201(TOP-CHROME) Study Group. Topiramate reduces headache days in chronic migraine: a randomized, double-blind, placebo-controlled study. Cephalalgia 2007; 27(07):814–823

Its efficacy usually increases in parallel to its dose, but the opposite occurs regarding its tolerability. Indeed, topiramate trials have had high drop-out rates due to side effects.6565 Silberstein SD, Lipton RB, Dodick DW, et al; Topiramate Chronic Migraine Study Group. Efficacy and safety of topiramate for the treatment of chronic migraine: a randomized, double-blind, placebo-controlled trial. Headache 2007;47(02):170–1806767 Diener H-C, Tfelt-Hansen P, Dahlöf C, et al; MIGR-003 Study Group. Topiramate in migraine prophylaxis–results from a placebo-controlled trial with propranolol as an active control. J Neurol 2004;251(08):943–950 However, when taken by subjects with episodic migraine with a high frequency of attacks it may prevent its progression to chronic migraine.6868 Lipton RB, Silberstein S, Dodick D, et al. Topiramate intervention to prevent transformation of episodic migraine: the topiramate INTREPID study. Cephalalgia 2011;31(01):18–30 Patients should be warned about the possibility of memory problems, weight loss, temporary tingling of extremities, and to discontinue treatment in case of irritability or visual symptoms.

Topiramate pharmacodynamics of migraine control are not fully understood, but they may involve its actions on multiple receptors.5656 https://go.drugbank.com/drugs/
https://go.drugbank.com/drugs/... Despite its low tolerability, topiramate remains one of the most versatile and efficient migraine prophylactic medications.Table 5 summarizes topiramate's pharmacological and efficacy features.5656 https://go.drugbank.com/drugs/
https://go.drugbank.com/drugs/... ,6969 Hu C, Zhang Y, Tan G. Advances in topiramate as prophylactic treatment for migraine. Brain Behav 2021;11(10):e2290

Onabotulinumtoxin A

Because onabotulinumtoxin A resolved pain before dystonia in cervical torticollis,7070 Jankovic J, Schwartz K. Botulinum toxin injections for cervical dystonia. Neurology 1990;40(02):277–280 the question of whether it could treat or prevent other pains such as migraine attacks arose.

Initial trials of onabotulinumtoxin A in the prevention of migraine failed to meet primary and secondary outcomes. However, a post-hoc analysis of the database disclosed an impact on the high-frequency migraine subjects.7171 Aurora S. Botulinum toxin type A for the treatment of migraine. Expert Opin Pharmacother 2006;7(08):1085–1095 This finding prompted the two pivotal trials of onabotulinumtoxin A as a preventative medication for chronic migraine, which proved onabotulinumtoxin A to be significantly better than placebo in nearly all primary and secondary outcomes. Thus, to date, onabotulinumtoxin A stands to be prescribed only for chronic migraine and according to the technique described in the PREEMPT protocols.7272 Dodick DW, Turkel CC, DeGryse RE, et al; PREEMPT Chronic Migraine Study Group. OnabotulinumtoxinA for treatment of chronic migraine: pooled results from the double-blind, randomized, placebo-controlled phases of the PREEMPT clinical program. Headache 2010;50(06):921–936

Onabotulinumtoxin A injections must be done after appropriate training in a skillful manner, to not harm the patient physically or aesthetically. Its administration should be done strictly following the PREEMPT protocol, with a 5 UI intramuscular dose per injection site, with a total dose range of 155 to 195 UI. At least three quarterly onabotulinumtoxin A administrations must be carried out before treatment can be called a failure.

Onabotulinumtoxin A efficacy in chronic migraine control was attained in parallel with the understanding of its antinociceptive effect which is secondary to its binding to nerve terminals, internalization, and lysis or cleavage of a protein (SNAP-25: synaptosome associated protein−25 kDa) that is part of the SNARE (Soluble NSF Attachment protein Receptor) complex needed for synaptic vesicle docking and fusion. Thus, it permanently impairs normal synaptic functioning, and further synaptic sprouting is needed for the synapse to recover.

Migraine prevention with onabotulinumtoxin A is believed to be reached through several mechanisms, mainly by interfering with C fibers transmission by disrupting protein kinase C-mediated membrane normal cycling of TRPV1, TRPA1, and ATP-gated P2 × 3 receptors, among other pathways.5656 https://go.drugbank.com/drugs/
https://go.drugbank.com/drugs/... ,7373 Aoki KR, Francis J. Updates on the antinociceptive mechanism hypothesis of botulinum toxin A. Parkinsonism Relat Disord 2011;17(Suppl 1):S28–S33 Therapeutic gain for chronic migraine is 11%, and the NNT for chronic migraine is nine. The predominant adverse effects associated with Onabotulinumtoxin A primarily include eyelid ptosis, facial asymmetry, facial palsy, head drop, and shoulder drop, with the primary causative factor being inadequate training.

Miscellaneous drugs in migraine prevention

Several other drugs that were tested for migraine prevention failed to reach a large market share. Of these are worth mentioning some phytotherapeutic drugs such as Thanacetum parthenum and Petasites hybridus; minerals such as magnesium, vitamins such as coenzyme Q10 and riboflavin; the circadian-related hormone melatonin; antihypertensive drugs such as verapamil, enalapril, Olmesartan, and candesartan; antiseizure drugs such as lamotrigine and levetiracetam and NMDA-blockers such as memantine.7474 Melhado EM, Santos PSF, Kaup AO, et al. Consensus of the Brazilian Headache Society (SBCe) for the prophylactic treatment of episodic migraine: Part I. Arq Neuropsiquiatr 2022;80 (08):845–861,7575 Santos PSF, Melhado EM, Kaup AO, et al. Consensus of the Brazilian Headache Society (SBCe) for prophylactic treatment of episodic migraine: part II. Arq Neuropsiquiatr 2022;80(09): 953–969 Altogether, with tricyclics, beta-adrenoceptor blockers, flunarizine, topiramate, onabotulinumtoxin A, and valproic acid, drugs mentioned in this “miscellaneous” category have in common the fact that their development was not based on previous and thought basic research on disease mechanisms with specifically pharmacodynamic drug design.

Monoclonal antibodies, the first migraine prophylactics to block the action on the ligand and receptors of CGRP to be launched on the market

The last decade may be remembered as the monoclonal antibodies era.1414 Edvinsson L, Haanes KA, Warfvinge K, Krause DN. CGRP as the target of new migraine therapies - successful translation from bench to clinic. Nat Rev Neurol 2018;14(06):338–350 In a few years, nearly a thousand (if not more) monoclonal antibodies were designed, but not all reached clinical viability. Monoclonal antibodies differ not only regarding the antigen they are aimed at, but also regarding their class (type of immunoglobulin), their level of humanization, the composition of their light chain, docking conformation, and fc fraction, for example, among other features.1414 Edvinsson L, Haanes KA, Warfvinge K, Krause DN. CGRP as the target of new migraine therapies - successful translation from bench to clinic. Nat Rev Neurol 2018;14(06):338–350,7676 Yuan H, Lauritsen CG, Kaiser EA, Silberstein SD. CGRP monoclonal antibodies for migraine: Rationale and progress. BioDrugs 2017;31(06):487–501

The monoclonal antibodies wave for the treatment of migraine was a consequence of the description of the CGRP molecule's role in migraine. The first antimigraine monoclonal antibody to be launched was erenumab,7777 Scheffler A, Messel O, Wurthmann S, et al. Erenumab in highly therapy-refractory migraine patients: First German real-world evidence. J Headache Pain 2020;21(01):848181 Tepper SJ, Diener HC, Ashina M, et al. Erenumab in chronic migraine with medication overuse: Subgroup analysis of a randomized trial. Neurology 2019;92(20):e2309–e2320 the only one to aim at the CGRP receptor. Shortly thereafter, galcanezumab,8282 Detke HC, Goadsby PJ, Wang S, Friedman DI, Selzler KJ, Aurora SK. Galcanezumab in chronic migraine: The randomized, double-blind, placebo-controlled REGAIN study. Neurology 2018;91 (24):e2211–e22218686 Stauffer VL, Dodick DW, Zhang Q, Carter JN, Ailani J, Conley RR. Evaluation of galcanezumab for the prevention of episodic migraine: The EVOLVE-1 randomized clinical trial. JAMA Neurol 2018;75(09):1080–1088 fremanezumab,8787 Dodick DW, Goadsby PJ, Silberstein SD, et al; ALD403 study investigators. Safety and efficacy of ALD403, an antibody to calcitonin gene-related peptide, for the prevention of frequent episodic migraine: a randomised, double-blind, placebo-controlled, exploratory phase 2 trial. Lancet Neurol 2014;13(11): 1100–11079292 Suzuki S, Suzuki K, Shiina T, Haruyama Y, Hirata K. Real-world experience with monthly and quarterly dosing of fremanezumab for the treatment of patients with migraine in Japan. Front Neurol 2023;14:1220285 and eptinezumab, the last three aimed against CGRP ligand, reached the market.9393 Ashina M, Saper J, Cady R, et al. Eptinezumab in episodic migraine: A randomized, double-blind, placebo-controlled study (PROMISE-1). Cephalalgia 2020;40(03):241–2549595 Diener HC, Marmura MJ, Tepper SJ, et al. Efficacy, tolerability, and safety of eptinezumab in patients with a dual diagnosis of chronic migraine and medication-overuse headache: Subgroup analysis of PROMISE-2. Headache 2021;61(01):125–136

Monoclonal antibodies proved to be preventative not only for “episodic” migraines,7878 Dodick DW, Ashina M, Brandes JL, et al. ARISE: A Phase 3 randomized trial of erenumab for episodic migraine. Cephalalgia 2018;38(06):1026–1037,7979 Goadsby PJ, Reuter U, Hallström Y, et al. A controlled trial of erenumab for episodic migraine. N Engl J Med 2017;377(22): 2123–2132,8585 Skljarevski V, Matharu M, Millen BA, Ossipov MH, Kim BK, Yang JY. Efficacy and safety of galcanezumab for the prevention of episodic migraine: Results of the EVOLVE-2 Phase 3 randomized controlled clinical trial. Cephalalgia 2018;38(08):1442–14548888 Dodick DW, Silberstein SD, Bigal ME, et al. Effect of fremanezumab compared with placebo for prevention of episodic migraine: A randomized clinical trial. JAMA 2018;319(19):1999–2008,9393 Ashina M, Saper J, Cady R, et al. Eptinezumab in episodic migraine: A randomized, double-blind, placebo-controlled study (PROMISE-1). Cephalalgia 2020;40(03):241–254 but also for chronic migraine,8080 Tepper S, Ashina M, Reuter U, et al. Safety and efficacy of erenumab for preventive treatment of chronic migraine: a randomised, double-blind, placebo-controlled phase 2 trial. Lancet Neurol 2017;16(06):425–4348282 Detke HC, Goadsby PJ, Wang S, Friedman DI, Selzler KJ, Aurora SK. Galcanezumab in chronic migraine: The randomized, double-blind, placebo-controlled REGAIN study. Neurology 2018;91 (24):e2211–e2221,8484 Dodick DW, Doty EG, Aurora SK, et al. Medication overuse in a subgroup analysis of phase 3 placebo-controlled studies of galcanezumab in the prevention of episodic and chronic migraine. Cephalalgia 2021;41(03):340–352,9090 Silberstein SD, Dodick DW, Bigal ME, et al. Fremanezumab for the preventive treatment of chronic migraine. N Engl J Med 2017; 377(22):2113–2122,9696 Lipton RB, Goadsby PJ, Smith J, et al. Efficacy and safety of eptinezumab in patients with chronic migraine: PROMISE-2. Neurology 2020;94(13):e1365–e1377 even if associated with medication overuse.7777 Scheffler A, Messel O, Wurthmann S, et al. Erenumab in highly therapy-refractory migraine patients: First German real-world evidence. J Headache Pain 2020;21(01):84,8282 Detke HC, Goadsby PJ, Wang S, Friedman DI, Selzler KJ, Aurora SK. Galcanezumab in chronic migraine: The randomized, double-blind, placebo-controlled REGAIN study. Neurology 2018;91 (24):e2211–e2221,9191 Silberstein SD, Cohen JM, Seminerio MJ, Yang R, Ashina S, Katsarava Z. The impact of fremanezumab on medication overuse in patients with chronic migraine: subgroup analysis of the HALO CM study. J Headache Pain 2020;21(01):114,9595 Diener HC, Marmura MJ, Tepper SJ, et al. Efficacy, tolerability, and safety of eptinezumab in patients with a dual diagnosis of chronic migraine and medication-overuse headache: Subgroup analysis of PROMISE-2. Headache 2021;61(01):125–136 It is worth mentioning that they showed efficacy even in those subjects with failure in the several adequate previous migraine prophylactic therapies.7777 Scheffler A, Messel O, Wurthmann S, et al. Erenumab in highly therapy-refractory migraine patients: First German real-world evidence. J Headache Pain 2020;21(01):84,8383 Mulleners WM, Kim BK, Láinez MJA, et al. Safety and efficacy of galcanezumab in patients for whom previous migraine preventive medication from two to four categories had failed (CONQUER): a multicentre, randomised, double-blind, placebo-controlled, phase 3b trial. Lancet Neurol 2020;19(10):814–825,8989 Ferrari MD, Diener HC, Ning X, et al. Fremanezumab versus placebo for migraine prevention in patients with documented failure to up to four migraine preventive medication classes (FOCUS): a randomised, double-blind, placebo-controlled, phase 3b trial. Lancet 2019;394(10203):1030–1040,9494 Ashina M, Lanteri-Minet M, Pozo-Rosich P, et al. Safety and efficacy of eptinezumab for migraine prevention in patients with two-to-four previous preventive treatment failures (DE-LIVER): a multi-arm, randomised, double-blind, placebo-controlled, phase 3b trial. Lancet Neurol 2022;21(07):597–607 These antibodies may also halt the evolution of high-frequency “episodic” migraine to chronic migraine or reverse chronic migraine to its episodic presentation.9797 Dodick DW, Goadsby PJ, Spierings ELH, Scherer JC, Sweeney SP, Grayzel DS. Safety and efficacy of LY2951742, a monoclonal antibody to calcitonin gene-related peptide, for the prevention of migraine: a phase 2, randomised, double-blind, placebo-controlled study. Lancet Neurol 2014;13(09):885–8929999 Lipton RB, Cohen JM, Bibeau K, et al. Reversion from chronic migraine to episodic migraine in patients treated with fremanezumab: Post hoc analysis from HALO CM Study. Headache 2020;60(10):2444–2453 A common feature of the monoclonal antibodies is the need for at least three consecutive trials before being considered as treatment failures.

Antimigraine mAbs are administered subcutaneously except for eptinezumab, administered intravenously. Also, while both eptinezumab and fremanezumab can be administered monthly or quarterly, erenumab and galcanezumab administration must be monthly. Because of their broad therapeutic scope, antimigraine mAbs were a major advance in migraine therapy. Another expressive advantage is their high tolerability: apart from local reactions, they are almost devoid of systemic side effects, bearing a high number-needed-to-harm index.100100 Drellia K, Kokoti L, Deligianni CI, Papadopoulos D, Mitsikostas DD. Anti-CGRP monoclonal antibodies for migraine prevention: A systematic review and likelihood to help or harm analysis. Cephalalgia 2021;41(07):851–864, Table 33 Peres MFP, Queiroz LP, Rocha-Filho PS, Sarmento EM, Katsarava Z, Steiner TJ. Migraine: a major debilitating chronic non-communicable disease in Brazil, evidence from two national surveys. J Headache Pain 2019;20(01):85 displays the most relevant features of the available anti-CGRP antibodies.

Gepants, a versatile and successful second generation

Of the gepants, both atogepant and rimegepant were tested for migraine prevention.101101 Ailani J, Lipton RB, Goadsby PJ, et al; ADVANCE Study Group. Atogepant for the preventive treatment of migraine. N Engl J Med 2021;385(08):695–706103103 Powell LC, L’Italien G, Popoff E, et al. Health state utility mapping of rimegepant for the preventive treatment of migraine: Double-blind treatment phase and open label extension (BHV3000-305). Adv Ther 2023;40(02):585–600 Atogepant seems to be the most promising of this class of drugs, since it bears the best efficacy data101101 Ailani J, Lipton RB, Goadsby PJ, et al; ADVANCE Study Group. Atogepant for the preventive treatment of migraine. N Engl J Med 2021;385(08):695–706,104104 Blumenfeld AM, Boinpally R, De Abreu Ferreira R, et al. Phase Ib, open-label, fixed-sequence, drug-drug interaction, safety, and tolerability study between atogepant and ubrogepant in participants with a history of migraine. Headache 2023;63(03): 322–332109109 Schwedt TJ, Lipton RB, Ailani J, et al. Time course of efficacy of atogepant for the preventive treatment of migraine: Results from the randomized, double-blind ADVANCE trial. Cephalalgia 2022; 42(01):3–11 and was described as effective also for preventing chronic migraine.110110 Pozo-Rosich P, Ailani J, Ashina M, et al. Atogepant for the preventive treatment of chronic migraine (PROGRESS): a randomised, double-blind, placebo-controlled, phase 3 trial. Lancet 2023;402(10404):775–785, Table 44 Foxhall K. The “Beating of Hammers”: Classical and medieval approaches to hemicrania. In: Foxhall K, ed. Migraine: a history.. Baltimore: Johns Hopkins University Press; 2019 summarizes the clinical pharmacology of the available gepants.

Figure 3 illustrates the timeline of studies of prophylactic medications for migraine.

Figure 3
Timeline of the migraine prophylactics trials.

Future directions

New molecular targets for the treatment of migraine include drugs of several classes, such as metabotropic receptors such as pituitary adenylate cyclase-activating polypeptide (PACAP-27, PACAP-38), vasoactive intestinal peptide (VIP), amylin, adrenomedullin; intracellular targets such as nitric oxide (NO), phosphodiesterase-3 (PPDE-5), phosphodiesterase-5 (PPDE-5); ion channels such as potassium channels, calcium channels, transient receptor potential (TRP) channels, acid-sensing insensitive cation channels (ASICS), and mechanosensitive Piezo channels.111111 Al-Hassany L, Boucherie DM, Creeney H, et al; European Headache Federation School of Advanced Studies (EHF-SAS) Future targets for migraine treatment beyond CGRP. J Headache Pain 2023;24(01):76,112112 Mikhailov N, Leskinen J, Fagerlund I, et al. Mechanosensitive meningeal nociception via Piezo channels: Implications for pulsa-tile pain in migraine? Neuropharmacology 2019;149:113–123 Whether their potential as targets will be confirmed remains to be proven.

Big pharma is quite discreet regarding drug development, but there were several failures on drug candidates, such as those designed to modulate nitric oxide synthase.113113 Barbanti P, Egeo G, Aurilia C, Fofi L, Della-Morte D. Drugs targeting nitric oxide synthase for migraine treatment. Expert Opin Investig Drugs 2014;23(08):1141–1148 Since levcromakalim is the most efficient substance to trigger migraine attacks, the next antimigraine drugs are quite likely to aim at potassium channels. The complexity of acting at many of these basic sites and receptors may hamper their possibility as suitable targets. However, a molecule aimed at the PACAP receptor PAC1 has been tested in a controlled trial and failed.114114 Ashina M, Doležil D, Bonner JH, et al. A phase 2, randomized, double-blind, placebo-controlled trial of AMG 301, a pituitary adenylate cyclase-activating polypeptide PAC1 receptor monoclonal antibody for migraine prevention. Cephalalgia 2021;41 (01):33–44 Two other receptors in this family, VPAC1 and VPAC2 show identical or better affinity for VIP than for PACAP. This feature compromises them as good candidates, mainly because VIP is expressed in parasympathetic nerves but not in the trigeminal ganglion.115115 Edvinsson L, Tajti J, Szalárdy L, Vécsei L. PACAP and its role in primary headaches. J Headache Pain 2018;19(01):21

Further detail on the expression and localization of PACAP and its receptors can be elucidated in the trigeminovascular system116116 Frederiksen SD, Warfvinge K, Ohlsson L, Edvinsson L. Expression of pituitary adenylate cyclase-activating peptide, calcitonin gene-related peptide and headache targets in the trigeminal ganglia of rats and humans. Neuroscience 2018;393:319–332,117117 Edvinsson JCA, Grell AS, Warfvinge K, Sheykhzade M, Edvinsson L, Haanes KA. Differences in pituitary adenylate cyclase-activating peptide and calcitonin gene-related peptide release in the trigeminovascular system. Cephalalgia 2020;40(12):1296–1309 and richly in the brain.118118 Warfvinge K, Edvinsson L. Cellular distribution of PACAP-38 and PACAP receptors in the rat brain: Relation to migraine activated regions. Cephalalgia 2020;40(06):527–542 At present we are expecting to see results from a study on a monoclonal antibody towards PACAP on migraine subjects.

Acknowledgements

The authors express their gratitude to André Pedroso Kowacs for reviewing the style.

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Publication Dates

  • Publication in this collection
    15 Jan 2024
  • Date of issue
    Dec 2023

History

  • Received
    03 Oct 2023
  • Reviewed
    19 Nov 2023
  • Accepted
    21 Nov 2023
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