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神经系统中降钙素基因相关受体成分蛋白(RCP)的缺失会使“gepant”拮抗作用产生偏差。

Loss of Calcitonin Gene Related Receptor component protein (RCP) in nervous system can bias "gepant" antagonism.

作者信息

Rahman Shafaqat M, Dickerson Ian, Luebke Anne E

出版信息

bioRxiv. 2024 Oct 26:2024.10.25.620369. doi: 10.1101/2024.10.25.620369.

DOI:10.1101/2024.10.25.620369
PMID:39484482
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11527201/
Abstract

UNLABELLED

We examined calcitonin gene-related peptide (CGRP)'s effects on behavioral surrogates for motion-induced nausea and static imbalance in the nestinRCP (-/-), a novel mouse model that loses expression of receptor component protein (RCP) in the nervous system after tamoxifen induction. The assays used were the motion-induced thermoregulation and center of pressure (CoP) assays. Findings suggest CGRP's affects behavioral measures in the nestinRCP (-/-) similarly to littermate controls, since CGRP was observed to increase female sway and diminishes tail vasodilations to provocative motion in both sexes. However, the CGRP-receptor antagonist olcegepant did not antagonize CGRP's effects in the nestinRCP (-/-), whereas it was effective in littermate controls. Findings suggest RCP loss may change the sensitivity of the CGRP receptor and affect the efficacy of receptor antagonists.

SIGNIFICANCE STATEMENT

Research in calcitonin gene-related peptide (CGRP) has primarily focused on ligand- receptor interactions at the calcitonin-like receptor (CLR) and receptor activity-modifying unit 1 (RAMP1) subunits. However, the role of receptor component protein (RCP), which mediates signaling via the Gα-stimulatory pathway, is less understood. A novel tamoxifen-inducible mouse model, nestinRCP (-/-), was generated to study loss of RCP in CGRP signaling in the nervous system, and behavioral changes to motion-induced nausea and postural sway were studied after systemic injections of CGRP or CGRP co-delivered with migraine drugs. Findings from this study suggest the loss of CGRP-RCP can bias "gepant" antagonists like olcegepant, and may promote development of therapies to inhibit the RCP-CLR interactions.

摘要

未标记

我们研究了降钙素基因相关肽(CGRP)对运动诱发恶心和静态失衡行为替代指标的影响,实验对象是nestinRCP(-/-)小鼠,这是一种新型小鼠模型,在他莫昔芬诱导后神经系统中失去受体成分蛋白(RCP)的表达。所采用的检测方法是运动诱发体温调节和压力中心(CoP)检测。研究结果表明,CGRP对nestinRCP(-/-)行为指标的影响与同窝对照相似,因为观察到CGRP会增加雌性的摇摆,并减少两性对刺激性运动的尾部血管舒张。然而,CGRP受体拮抗剂olcegepant在nestinRCP(-/-)中并未拮抗CGRP的作用,而在同窝对照中却有效。研究结果表明,RCP缺失可能会改变CGRP受体的敏感性,并影响受体拮抗剂的疗效。

意义声明

降钙素基因相关肽(CGRP)的研究主要集中在降钙素样受体(CLR)和受体活性修饰单位1(RAMP1)亚基的配体-受体相互作用上。然而,介导通过Gα刺激途径信号传导的受体成分蛋白(RCP)的作用却鲜为人知。我们构建了一种新型的他莫昔芬诱导型小鼠模型nestinRCP(-/-),以研究神经系统中CGRP信号传导中RCP的缺失情况,并在全身注射CGRP或与偏头痛药物共同递送的CGRP后,研究运动诱发恶心和姿势摇摆的行为变化。这项研究的结果表明,CGRP-RCP的缺失可能会使olcegepant等“gepant”拮抗剂产生偏差,并可能促进抑制RCP-CLR相互作用疗法的开发。