Calcitonin Gene‐Related Peptide Modulators – The History and Renaissance of a New Migraine Drug Class

Hargreaves, Richard; Olesen, Jes

doi:10.1111/head.13510

Cited by 104 publications

(129 citation statements)

References 154 publications

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“…Inhibition of the CGRP receptor has emerged as a promising target for the acute and preventive treatment of migraine (Edvinsson, 2018). Previously investigated small-molecule CGRP antagonists have demonstrated efficacy in the treatment of migraine; however, clinical studies involving telcagepant and MK-3207 revealed potential concerns regarding drug-induced elevation of liver enzymes, and clinical development of these compounds was discontinued (Hewitt et al, 2011;Ho et al, 2014;Hargreaves and Olesen, 2019). Although the exact mechanism of this hepatotoxicity is unknown, it was hypothesized to be partly attributable to the formation of reactive metabolites and not specific to CGRP receptor antagonism (Hargreaves and Olesen, 2019).…”

Section: Discussionmentioning

confidence: 99%

“…Previously investigated small-molecule CGRP antagonists have demonstrated efficacy in the treatment of migraine; however, clinical studies involving telcagepant and MK-3207 revealed potential concerns regarding drug-induced elevation of liver enzymes, and clinical development of these compounds was discontinued (Hewitt et al, 2011;Ho et al, 2014;Hargreaves and Olesen, 2019). Although the exact mechanism of this hepatotoxicity is unknown, it was hypothesized to be partly attributable to the formation of reactive metabolites and not specific to CGRP receptor antagonism (Hargreaves and Olesen, 2019). The absence of any ubrogepant-associated hepatotoxicity has been supported by safety data from recent clinical studies (Goadsby et al, 2019;Hutchinson et al, 2019).…”

Section: Discussionmentioning

confidence: 99%

“…A substantial amount of scientific data implicates the CGRP pathway in the underlying physiologic mechanisms associated with migraine (Goadsby et al, 1990;Lassen et al, 2002;Edvinsson, 2015). Furthermore, previously investigated small-molecule CGRP receptor antagonists have demonstrated efficacy in the treatment of migraine, although development was eventually halted because of safety concerns (Hewitt et al, 2011;Ho et al, 2014;Hargreaves and Olesen, 2019). The clinical success of monoclonal antibodies targeting CGRP also provides support for the CGRP receptors as a promising therapeutic target for migraine (Dodick, 2019).…”

Section: Introductionmentioning

confidence: 99%

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Characterization of Ubrogepant: A Potent and Selective Antagonist of the Human Calcitonin Gene‒Related Peptide Receptor*

Moore

Fraley

Bell

et al. 2020

J Pharmacol Exp Ther

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A growing body of evidence has implicated the calcitonin gene-related peptide (CGRP) receptors in migraine pathophysiology. With the approval of monoclonal antibodies targeting CGRP or the CGRP receptor, the inhibition of CGRP-mediated signaling emerged as a promising approach for preventive treatments of migraine in adults. Recently, small-molecule anti-CGRP treatments have shown efficacy for treating migraine. The current studies aimed to characterize the pharmacologic properties of ubrogepant, an orally bioavailable CGRP receptor antagonist for the acute treatment of migraine. In a series of ligand-binding assays, ubrogepant exhibited a high binding affinity for native (K i 5 0.067 nM) and cloned human (K i 5 0.070 nM) and rhesus CGRP receptors (K i 5 0.079 nM), with relatively lower affinities for CGRP receptors from rat, mouse, rabbit, and dog. In functional assays, ubrogepant potently blocked human a-CGRP2stimulated cAMP response (IC 50 of 0.08 nM) and exhibited highly selective antagonist activity for the CGRP receptor compared with other members of the human calcitonin receptor family. Furthermore, the in vivo CGRP receptor antagonist activity of ubrogepant was evaluated in a pharmacodynamic model of capsaicin-induced dermal vasodilation (CIDV) in rhesus monkeys and humans. Results demonstrated that ubrogepant produced concentration-dependent inhibition of CIDV with a mean EC 50 of 3.2 and 2.6 nM in rhesus monkeys and humans, respectively. Brain penetration studies with ubrogepant in monkeys showed a cerebrospinal fluid:plasma ratio of 0.03 and low CGRP receptor occupancy. In summary, ubrogepant is a competitive antagonist with high affinity, potency, and selectivity for the human CGRP receptor. SIGNIFICANCE STATEMENT Ubrogepant is a potent, selective, orally delivered, smallmolecule competitive antagonist of the human CGRP. In vivo studies using a pharmacodynamic model of CIDV in rhesus monkeys and humans demonstrated that ubrogepant produced concentration-dependent inhibition of CIDV, indicating a predictable pharmacokinetic-pharmacodynamic relationship.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Characterization of Ubrogepant: A Potent and Selective Antagonist of the Human Calcitonin Gene‒Related Peptide Receptor*

Moore

Fraley

Bell

et al. 2020

J Pharmacol Exp Ther

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“…When considering acute treatments, the various TTTs are characterized by a striking comparable proportion of responders in terms of pain response at 2 hours, the most common efficacy indicator for abortive migraine treatments: 59% with triptans at standard doses (range 42.4% with oral frovatriptan-75.7% with subcutaneous sumatriptan), 59% with lasmiditan (100 and 200 mg), 61.4% with telcagepant (280/300 mg), 56.2% with BI 44370 TA (400 mg), and 60.8% with MK-3207 (100-200 mg). 17 As acutely observed by Olesen, "classification of migraine into different endophenotypes could aid diagnosis and treatment, but requires detailed characterization of different phenotypes." 11 By pooling together all the aforementioned findings it emerges that TTTs are effective in approximately 60% of migraineurs regardless of the type treatment (acute o preventative) or the drug mechanism (block of the trigeminal sensory system or antagonism of its principal neuropeptide).…”

mentioning

confidence: 99%

“…[14][15][16] This hypothesis has been recently taken into account also by Hargreaves and Olesen who raised the possibility that super-responders to CGRP mAbs might be those patients with autonomic signs in cranial tissues supplied by trigeminal innervation. 17 As acutely observed by Olesen, "classification of migraine into different endophenotypes could aid diagnosis and treatment, but requires detailed characterization of different phenotypes." 18 A very simple stepping stone in identifying TTTs responders could be the identification of migraineurs with unilateral pain.…”

mentioning

confidence: 99%

Trigeminal‐Targeted Treatments in Migraine: Is 60% the Magic Number?

2019

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Trigeminal‐targeted treatments (TTTs), the most specific and selective therapeutic migraine approach to date, are effective in approximately 60% of patients regardless of treatment type or mechanism, at least if used alone. Sixty percent is also the proportion of migraineurs who develop migraine‐like episodes following experimental intravenous administration of trigeminal neuropeptides and roughly 60% is the percentage of patients with a unilateral migraine tracing the area of cutaneous distribution of the trigeminal ophthalmic branch. Hence, mechanisms other than the trigeminovascular activation are probably involved in the 40% of migraineurs who do not respond to TTTs. A closer cooperation between clinical and basic neuroscientists is needed to explore migraine models because only a careful appraisal of migraine endophenotypes may help to unravel their underlying multifaceted pathophysiological machinery.

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Anti‐migraine Calcitonin Gene–Related Peptide Receptor Antagonists Worsen Cerebral Ischemic Outcome in Mice

Mulder

Vries

et al. 2020

Annals of Neurology

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Objective: Calcitonin gene-related peptide (CGRP) pathway inhibitors are emerging treatments for migraine. CGRPmediated vasodilation is, however, a critical rescue mechanism in ischemia. We, therefore, investigated whether gepants, small molecule CGRP receptor antagonists, worsen cerebral ischemia. Methods: Middle cerebral artery was occluded for 12 to 60 minutes in mice. We compared infarct risk and volumes, collateral flow, and neurological deficits after pretreatment with olcegepant (single or 10 daily doses of 0.1-1mg/kg) or rimegepant (single doses of 10-100mg/kg) versus vehicle. We also determined their potency on CGRP-induced relaxations in mouse and human vessels, in vitro. Results: Olcegepant (1mg/kg, single dose) increased infarct risk after 12-to 20-minute occlusions mimicking transient ischemic attacks (14/19 vs 6/18 with vehicle, relative risk = 2.21, p < 0.022), and doubled infarct volumes (p < 0.001) and worsened neurological deficits (median score = 9 vs 5 with vehicle, p = 0.008) after 60-minute occlusion. Ten daily doses of 0.1 to 1mg/kg olcegepant yielded similar results. Rimegepant 10mg/kg increased infarct volumes by 60% after 20-minute ischemia (p = 0.03); 100mg/kg caused 75% mortality after 60-minute occlusion. In familial hemiplegic migraine type 1 mice, olcegepant 1mg/kg increased infarct size after 30-minute occlusion (1.6-fold, p = 0.017). Both gepants consistently diminished collateral flow and reduced reperfusion success. Olcegepant was 10-fold more potent than rimegepant on CGRP-induced relaxations in mouse aorta. Interpretation: Gepants worsened ischemic stroke in mice via collateral dysfunction. CGRP pathway blockers might thus aggravate coincidental cerebral ischemic events. The cerebrovascular safety of these agents must therefore be better delineated, especially in patients at increased risk of ischemic events or on prophylactic CGRP inhibition.

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Calcitonin Gene‐Related Peptide Modulators – The History and Renaissance of a New Migraine Drug Class

Cited by 104 publications

References 154 publications

Characterization of Ubrogepant: A Potent and Selective Antagonist of the Human Calcitonin Gene‒Related Peptide Receptor*

Characterization of Ubrogepant: A Potent and Selective Antagonist of the Human Calcitonin Gene‒Related Peptide Receptor*

Trigeminal‐Targeted Treatments in Migraine: Is 60% the Magic Number?

Anti‐migraine Calcitonin Gene–Related Peptide Receptor Antagonists Worsen Cerebral Ischemic Outcome in Mice

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