Development and pharmacological characterization of novel multi- calcitonin gene-related peptide and pituitary adenylate cyclase-activating peptide receptor antagonists.

IF 5.4 2区医学 Q1 CLINICAL NEUROLOGY Headache Pub Date : 2025-02-25 DOI:10.1111/head.14916

Zoe Tasma, Andrew Siow, Paul W R Harris, Margaret A Brimble, Debbie L Hay, Christopher S Walker

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引用次数: 0

Abstract

Objective: This study aimed to provide proof-of-concept that multi-receptor antagonist peptides can be generated by covalently linking independent antagonist peptides that block calcitonin gene-related peptide (CGRP_8-37) or pituitary adenylate cyclase-activating peptide (PACAP)/vasoactive intestinal peptide (VIP) (PACAP_6-38) activity.

Background: The neuropeptides CGRP and PACAP are implicated in migraine and pain pathogenesis. CGRP and PACAP are elevated during a migraine attack, and following infusion of either peptide, patients develop migraine-like attacks. This indicates that targeting both these systems may provide therapeutic benefits. Mechanistic studies suggest that these peptides largely act independently from one another. Therefore, blocking the activity of both CGRP and PACAP simultaneously could provide a clinical advantage over individual blockade. One strategy is to develop a single antagonist capable of inhibiting the signaling of both CGRP and PACAP receptors, a multi-receptor antagonist. N-terminal truncation of CGRP and PACAP generates the antagonists CGRP_8-37 and PACAP_6-38, respectively. These are commonly used as research tools for the CGRP and PACAP receptors. These peptide antagonists were, therefore, used as the basis for the design of multi-receptor antagonists against the CGRP and PACAP receptors and to test their functionality in vitro.

Methods: To generate multi-receptor antagonists, CGRP_8-37 was linked through 1,3-dipolar cycloaddition using click chemistry to PACAP_6-38 at amino acid residues 21, 34, or 38. The ability of these multi-receptor antagonists to block CGRP activity (CGRP and AMY₁ receptors) and PACAP-38, PACAP-27, and VIP activity (PAC₁, VPAC₁, and VPAC₂ receptors) was then characterized in transfected Cos7 cells. The peptides were then further examined in pain-relevant rat spinal cord cultures, as a model of endogenous receptors.

Results: Multi-receptor antagonists were successfully generated, displaying similar antagonist potency to their parental antagonists in both transfected Cos7 cells and in spinal cord cultures. Interestingly, CGRP_8-37 linked to position 38 of PACAP_6-38 was a more potent antagonist of CGRP activity than CGRP_8-37.

Conclusion: This study provides proof-of-concept evidence for the development of potent multi-receptor antagonists capable of blocking both CGRP and PACAP activity.

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研究目的本研究旨在提供概念证明，通过共价连接阻断降钙素基因相关肽（CGRP8-37）或垂体腺苷酸环化酶激活肽（PACAP）/血管活性肠肽（VIP）（PACAP6-38）活性的独立拮抗剂肽，可以生成多受体拮抗剂肽：背景：神经肽 CGRP 和 PACAP 与偏头痛和疼痛的发病机制有关。偏头痛发作时 CGRP 和 PACAP 会升高，输注这两种肽后，患者会出现类似偏头痛的发作。这表明，针对这两种系统可能会带来治疗效果。机理研究表明，这些肽的作用在很大程度上是相互独立的。因此，同时阻断 CGRP 和 PACAP 的活性可能比单独阻断更有临床优势。一种策略是开发一种能够同时抑制 CGRP 和 PACAP 受体信号传导的单一拮抗剂，即多受体拮抗剂。CGRP 和 PACAP 的 N 端截短分别产生了拮抗剂 CGRP8-37 和 PACAP6-38。这些肽通常用作 CGRP 和 PACAP 受体的研究工具。因此，我们以这些多肽拮抗剂为基础，设计了针对 CGRP 和 PACAP 受体的多受体拮抗剂，并在体外测试其功能：为了生成多受体拮抗剂，CGRP8-37 通过 1,3-二极环加成法与 PACAP6-38 在氨基酸残基 21、34 或 38 上连接。然后在转染的 Cos7 细胞中鉴定了这些多受体拮抗剂阻断 CGRP 活性（CGRP 和 AMY1 受体）和 PACAP-38、PACAP-27 和 VIP 活性（PAC1、VPAC1 和 VPAC2 受体）的能力。然后在与疼痛相关的大鼠脊髓培养物中进一步检测了这些肽，作为内源性受体的模型：结果：成功生成了多受体拮抗剂，在转染的 Cos7 细胞和脊髓培养物中显示出与其亲代拮抗剂相似的拮抗效力。有趣的是，与 PACAP6-38 第 38 位相连的 CGRP8-37 比 CGRP8-37 对 CGRP 活性的拮抗作用更强：本研究为开发能同时阻断 CGRP 和 PACAP 活性的强效多受体拮抗剂提供了概念验证证据。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Headache 医学-临床神经学

CiteScore

9.40

自引率

10.00%

发文量

172

审稿时长

3-8 weeks

期刊介绍： Headache publishes original articles on all aspects of head and face pain including communications on clinical and basic research, diagnosis and management, epidemiology, genetics, and pathophysiology of primary and secondary headaches, cranial neuralgias, and pains referred to the head and face. Monthly issues feature case reports, short communications, review articles, letters to the editor, and news items regarding AHS plus medicolegal and socioeconomic aspects of head pain. This is the official journal of the American Headache Society.