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阻断 CGRP 通路治疗偏头痛急性发作和预防:成功的演进。

Blocking the CGRP Pathway for Acute and Preventive Treatment of Migraine: The Evolution of Success.

机构信息

Biohaven Pharmaceuticals Inc., 215 Church Street, New Haven, Connecticut 06510, United States.

出版信息

J Med Chem. 2020 Jul 9;63(13):6600-6623. doi: 10.1021/acs.jmedchem.9b01810. Epub 2020 Feb 20.

Abstract

The pivotal role of calcitonin gene-related peptide (CGRP) in migraine pathophysiology was identified over 30 years ago, but the successful clinical development of targeted therapies has only recently been realized. This Perspective traces the decades long evolution of medicinal chemistry required to advance small molecule CGRP receptor antagonists, also called gepants, including the current clinical agents rimegepant, vazegepant, ubrogepant, and atogepant. Providing clinically effective blockade of CGRP signaling required surmounting multiple challenging hurdles, including defeating a sizable ligand with subnanomolar affinity for its receptor, designing antagonists with an extended confirmation and multiple pharmacophores while retaining solubility and oral bioavailability, and achieving circulating free plasma levels that provided near maximal CGRP receptor coverage. The clinical efficacy of oral and intranasal gepants and the injectable CGRP monoclonal antibodies (mAbs) are described, as are recent synthetic developments that have benefited from new structural biology data. The first oral gepant was recently approved and heralds a new era in the treatment of migraine.

摘要

降钙素基因相关肽 (CGRP) 在偏头痛病理生理学中的关键作用在 30 多年前就已确定,但靶向治疗的成功临床开发直到最近才得以实现。本观点追溯了推进小分子 CGRP 受体拮抗剂(也称为 gepants)所需的数十年药物化学发展历程,其中包括目前的临床药物rimegepant、vazegepant、ubrogepant 和 atogepant。为了提供对 CGRP 信号的有效临床阻断,需要克服多个具有挑战性的障碍,包括击败对其受体具有亚纳摩尔亲和力的相当大的配体,设计具有扩展构象和多个药效团的拮抗剂,同时保持溶解度和口服生物利用度,并实现提供接近最大 CGRP 受体覆盖的循环游离血浆水平。本文描述了口服和鼻内 gepants 以及可注射 CGRP 单克隆抗体 (mAb) 的临床疗效,以及最近从新结构生物学数据中受益的合成进展。第一种口服 gepant 最近获得批准,标志着偏头痛治疗的新时代的到来。

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