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Review
. 2022 Apr;19(3):922-930.
doi: 10.1007/s13311-022-01230-x. Epub 2022 Apr 14.

The Arrival of Anti-CGRP Monoclonal Antibodies in Migraine

Fred Cohen  1 Hsiangkuo Yuan  1 E M G DePoy  1 Stephen D Silberstein  2
Affiliations
Review

The Arrival of Anti-CGRP Monoclonal Antibodies in Migraine

Fred Cohen et al. Neurotherapeutics. 2022 Apr.

Abstract

Remarkable advancements have been made in the field of migraine pathophysiology and pharmacotherapy over the past decade. Understanding the molecular mechanism of calcitonin gene-related peptide (CGRP) has led to the discovery of a novel class of drugs, CGRP functional blocking monoclonal antibodies (mAbs), for migraine prevention. CGRP is a neuropeptide inherently involved in migraine physiology where its receptors are found dispersed throughout the central and peripheral nervous systems. CGRP-targeted mAbs are effective in the preventive treatment of both chronic and episodic migraine. The advantages of mAbs over oral migraine preventives are numerous. Favorable attributes of the mAbs include high affinity and selectivity for CGRP molecular targets, long-circulating plasma half-lives, and limited risk for nonspecific hepatic and renal toxicity. This pharmacological profile leads to fewer off-target (side) effects and drug-drug interactions rendering mAbs an attractive alternative to traditional small molecule therapies, especially for the preventive treatment of migraine. MAbs display minimal drug interaction thus are excellent for patients prescribed with multiple medications. However, the long-term safety of CGRP blockade is incompletely known, and CGRP mAbs use should be avoided during pregnancy. CGRP mAbs represent a radical shift in preventing chronic and episodic migraine.

Keywords: CGRP; Calcitonin gene-related peptide; Migraine; Monoclonal antibody; Neurogenic inflammation; Trigeminovascular system.

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Conflict of interest statement

F.C. has no conflicts of interest or financial disclosures. H.Y. has previously served as a consultant for Supernus Pharmaceuticals, Inc. and Trillen Medical Inc., and currently received research grants from NIH (R44NS115460). E.D. has no conflicts of interest or financial disclosures. S.S. receives honoraria from Alder Biopharmaceuticals; Allergan, Inc.; Amgen; Avanir Pharmaceuticals, Inc.; Depomed; Dr. Reddy’s Laboratories; eNeura Inc.; electroCore Medical, LLC; Ipsen Biopharmaceuticals; Medscape, LLC; Medtronic, Inc.; Mitsubishi Tanabe Pharma America, Inc.; NINDS; St. Jude Medical; Supernus Pharmaceuticals, Inc.; Teva Pharmaceuticals and Trigemina, Inc.

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