CGRP Receptor Activity in Mice with Global Expression of Human Receptor Activity Modifying Protein 1

Overview

Journal Br J Pharmacol

Publisher Wiley

Specialty Pharmacology

Date 2017 Mar 21

PMID 28317098

Citations 16

Authors

Keegan J Bohn

Baolin Li

Xiaofang Huang

Bianca N Mason

Anne-Sophie Wattiez

Adisa Kuburas

Christopher S Walker

Peiyi Yang

Jianliang Yu

Beverly A Heinz

Kirk W Johnson

Andrew F Russo

Affiliations

Soon will be listed here.

Abstract

Background And Purpose: CGRP is a potent vasodilator and nociceptive neuropeptide linked to migraine. CGRP receptors are heterodimers of receptor activity modifying protein 1 (RAMP1) and either calcitonin receptor-like receptor (CLR; forms canonical CGRP receptor) or calcitonin receptor (CT receptor; forms AMY receptor). The goal of this study was to test whether transgenic mice globally expressing human RAMP1 have increased CGRP receptor activity and whether the receptors are sensitive to human selective antagonist telcagepant.

Experimental Approach: cAMP production was measured in primary cultures of aortic smooth muscle and trigeminal ganglia neurons from global hRAMP1 mice and non-transgenic littermates. Functional activity and inhibition were compared with clonal cell lines expressing combinations of CLR or CT receptors with RAMP1.

Key Results: Cultured smooth muscle from global hRAMP1 mice had a 10-fold greater CGRP-induced cAMP maximal response (Rmax) than non-transgenic littermates, with similar EC s. In contrast, cultured trigeminal ganglia from global hRAMP1 mice had a 40-fold leftward shift of the EC , with similar Rmax values as littermates. In both hRAMP1 cultures, telcagepant blocked CGRP-induced cAMP production, but was not effective in non-transgenic cultures. IC values were closer to those observed for CT receptor/hRAMP1 than CLR/hRAMP1 in clonal cell lines.

Conclusions And Implications: Overexpression of hRAMP1 increases CGRP signalling by changing the maximal response or ligand sensitivity, depending on tissue type. Furthermore, telcagepant inhibited transgenic hRAMP1 CGRP receptors, but the degree of inhibition suggests that the transgenic mice are only partially humanized or both canonical CGRP and AMY receptors are functional in trigeminal ganglia neurons and vascular smooth muscle.

Citing Articles

Characterization of Antibodies against Receptor Activity-Modifying Protein 1 (RAMP1): A Cautionary Tale.

Hendrikse E, Rees T, Tasma Z, Garelja M, Siow A, Harris P Int J Mol Sci. 2022; 23(24).

PMID: 36555690 PMC: 9787598. DOI: 10.3390/ijms232416035.

CGRP physiology, pharmacology, and therapeutic targets: migraine and beyond.

Russo A, Hay D Physiol Rev. 2022; 103(2):1565-1644.

PMID: 36454715 PMC: 9988538. DOI: 10.1152/physrev.00059.2021.

A narrative review of the calcitonin peptide family and associated receptors as migraine targets: Calcitonin gene-related peptide and beyond.

Garelja M, Hay D Headache. 2022; 62(9):1093-1104.

PMID: 36226379 PMC: 9613588. DOI: 10.1111/head.14388.

Characterization of transit rates in the large intestine of mice following treatment with a CGRP antibody, CGRP receptor antibody, and small molecule CGRP receptor antagonists.

Johnson K, Li X, Huang X, Heinz B, Yu J, Li B Headache. 2022; 62(7):848-857.

PMID: 35822594 PMC: 9545683. DOI: 10.1111/head.14336.

CGRP and the Calcitonin Receptor are Co-Expressed in Mouse, Rat and Human Trigeminal Ganglia Neurons.

Rees T, Russo A, OCarroll S, Hay D, Walker C Front Physiol. 2022; 13:860037.

PMID: 35620595 PMC: 9128745. DOI: 10.3389/fphys.2022.860037.

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