Calcitonin Gene-Related Peptide (CGRP)-Targeted Treatments—New Therapeutic Technologies for Migraine

L. Sangalli, S. Brazzoli
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引用次数: 1

Abstract

Migraine is ranked as the third most common disorder worldwide and is considered one of the most disabling neurological conditions. Its treatment has mostly relied on medications that were non-specifically developed for migraine, thus accompanied by low adherence, inadequate effectiveness and intolerable side effects. These recent years have seen the development of new migraine-specific therapies targeting the calcitonin gene-related peptide (CGRP) and its receptor. These newly developed therapies, the small molecule gepants targeting the CGRP receptor and the anti-CGRP monoclonal antibodies (mAbs), are currently available in the market and FDA-approved for migraine treatment. As they are migraine-specific therapies, they largely expand their use to patients that could not tolerate previous treatments, either for systemic contraindications or drug-to-drug interactions, or where any other available option was not efficacious. Randomized controlled trials have demonstrated the efficacy of these new medications, with minor adverse effects reported (most commonly nausea and constipation). This article will review the mechanism of action, indications, contraindications, and tolerability profile of gepants and anti-CGRP mAbs, by summarizing the available literature. Finally, avenues for future research will be identified, so that upcoming controlled studies may be designed to fill such gaps.
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降钙素基因相关肽(CGRP)靶向治疗——偏头痛的新治疗技术
偏头痛是世界上第三大最常见的疾病,被认为是最致残的神经系统疾病之一。它的治疗主要依赖于非专门为偏头痛开发的药物,因此伴随着低依从性,有效性不足和难以忍受的副作用。近年来,针对降钙素基因相关肽(CGRP)及其受体的偏头痛特异性治疗有了新的发展。这些新开发的治疗方法,靶向CGRP受体的小分子基因和抗CGRP单克隆抗体(mab),目前已在市场上销售,并已获得fda批准用于偏头痛治疗。由于它们是偏头痛的特异性治疗方法,它们在很大程度上扩大了对以前治疗不能耐受的患者的使用,无论是系统性禁忌症或药物对药物的相互作用,还是任何其他可用的选择都无效。随机对照试验证明了这些新药物的有效性,并报告了轻微的不良反应(最常见的是恶心和便秘)。本文将通过对现有文献的总结,对抗cgrp单克隆抗体的作用机制、适应症、禁忌证和耐受性进行综述。最后,将确定未来研究的途径,以便设计即将进行的对照研究来填补这些空白。
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