Literature DB >> 29087309

Endosomal signaling of the receptor for calcitonin gene-related peptide mediates pain transmission.

Rebecca E Yarwood1,2, Wendy L Imlach3,4, TinaMarie Lieu1,2, Nicholas A Veldhuis1,2, Dane D Jensen1,2, Carmen Klein Herenbrink1,2, Luigi Aurelio1,2, Zhijian Cai3,4, MacDonald J Christie5, Daniel P Poole1,2,6, Christopher J H Porter1,2, Peter McLean7, Gareth A Hicks7, Pierangelo Geppetti8, Michelle L Halls1,2, Meritxell Canals9,2, Nigel W Bunnett9,2,10,11,12.   

Abstract

G protein-coupled receptors (GPCRs) are considered to function primarily at the plasma membrane, where they interact with extracellular ligands and couple to G proteins that transmit intracellular signals. Consequently, therapeutic drugs are designed to target GPCRs at the plasma membrane. Activated GPCRs undergo clathrin-dependent endocytosis. Whether GPCRs in endosomes control pathophysiological processes in vivo and are therapeutic targets remains uncertain. We investigated the contribution of endosomal signaling of the calcitonin receptor-like receptor (CLR) to pain transmission. Calcitonin gene-related peptide (CGRP) stimulated CLR endocytosis and activated protein kinase C (PKC) in the cytosol and extracellular signal regulated kinase (ERK) in the cytosol and nucleus. Inhibitors of clathrin and dynamin prevented CLR endocytosis and activation of cytosolic PKC and nuclear ERK, which derive from endosomal CLR. A cholestanol-conjugated antagonist, CGRP8-37, accumulated in CLR-containing endosomes and selectively inhibited CLR signaling in endosomes. CGRP caused sustained excitation of neurons in slices of rat spinal cord. Inhibitors of dynamin, ERK, and PKC suppressed persistent neuronal excitation. CGRP8-37-cholestanol, but not unconjugated CGRP8-37, prevented sustained neuronal excitation. When injected intrathecally to mice, CGRP8-37-cholestanol inhibited nociceptive responses to intraplantar injection of capsaicin, formalin, or complete Freund's adjuvant more effectively than unconjugated CGRP8-37 Our results show that CLR signals from endosomes to control pain transmission and identify CLR in endosomes as a therapeutic target for pain. Thus, GPCRs function not only at the plasma membrane but also in endosomes to control complex processes in vivo. Endosomal GPCRs are a drug target that deserve further attention.

Entities:  

Keywords:  G protein-coupled receptors; endocytosis; neuropeptides; nociception; pain

Mesh:

Substances:

Year:  2017        PMID: 29087309      PMCID: PMC5699040          DOI: 10.1073/pnas.1706656114

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  27 in total

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Authors:  Michelle L Halls; Daniel P Poole; Andrew M Ellisdon; Cameron J Nowell; Meritxell Canals
Journal:  Methods Mol Biol       Date:  2015

2.  Dynamins at a glance.

Authors:  Jürgen A W Heymann; Jenny E Hinshaw
Journal:  J Cell Sci       Date:  2009-10-01       Impact factor: 5.285

3.  The proliferative and antiapoptotic effects of substance P are facilitated by formation of a beta -arrestin-dependent scaffolding complex.

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Journal:  Proc Natl Acad Sci U S A       Date:  2000-09-26       Impact factor: 11.205

4.  Localization of calcitonin receptor-like receptor and receptor activity modifying protein 1 in enteric neurons, dorsal root ganglia, and the spinal cord of the rat.

Authors:  Graeme S Cottrell; Dirk Roosterman; Juan-Carlos Marvizon; B Song; Elizabeth Wick; Stella Pikios; Helen Wong; Claire Berthelier; Yat Tang; Catia Sternini; Nigel W Bunnett; Eileen F Grady
Journal:  J Comp Neurol       Date:  2005-09-26       Impact factor: 3.215

5.  Cathepsin S causes inflammatory pain via biased agonism of PAR2 and TRPV4.

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Journal:  J Biol Chem       Date:  2014-08-12       Impact factor: 5.157

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Authors:  Ross W Cheloha; Samuel H Gellman; Jean-Pierre Vilardaga; Thomas J Gardella
Journal:  Nat Rev Endocrinol       Date:  2015-08-25       Impact factor: 43.330

Review 7.  Calcitonin gene-related peptide: physiology and pathophysiology.

Authors:  F A Russell; R King; S-J Smillie; X Kodji; S D Brain
Journal:  Physiol Rev       Date:  2014-10       Impact factor: 37.312

8.  Conformational biosensors reveal GPCR signalling from endosomes.

Authors:  Roshanak Irannejad; Jin C Tomshine; Jon R Tomshine; Michael Chevalier; Jacob P Mahoney; Jan Steyaert; Søren G F Rasmussen; Roger K Sunahara; Hana El-Samad; Bo Huang; Mark von Zastrow
Journal:  Nature       Date:  2013-03-20       Impact factor: 49.962

9.  GPCR-G Protein-β-Arrestin Super-Complex Mediates Sustained G Protein Signaling.

Authors:  Alex R B Thomsen; Bianca Plouffe; Thomas J Cahill; Arun K Shukla; Jeffrey T Tarrasch; Annie M Dosey; Alem W Kahsai; Ryan T Strachan; Biswaranjan Pani; Jacob P Mahoney; Liyin Huang; Billy Breton; Franziska M Heydenreich; Roger K Sunahara; Georgios Skiniotis; Michel Bouvier; Robert J Lefkowitz
Journal:  Cell       Date:  2016-08-04       Impact factor: 41.582

10.  Persistent cAMP-signals triggered by internalized G-protein-coupled receptors.

Authors:  Davide Calebiro; Viacheslav O Nikolaev; Maria Cristina Gagliani; Tiziana de Filippis; Christian Dees; Carlo Tacchetti; Luca Persani; Martin J Lohse
Journal:  PLoS Biol       Date:  2009-08-18       Impact factor: 8.029

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6.  Homologous Regulation of Mu Opioid Receptor Recycling by G βγ , Protein Kinase C, and Receptor Phosphorylation.

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7.  Protein kinase D and Gβγ mediate sustained nociceptive signaling by biased agonists of protease-activated receptor-2.

Authors:  Peishen Zhao; Luke A Pattison; Dane D Jensen; Nestor N Jimenez-Vargas; Rocco Latorre; TinaMarie Lieu; Josue O Jaramillo; Cintya Lopez-Lopez; Daniel P Poole; Stephen J Vanner; Brian L Schmidt; Nigel W Bunnett
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8.  Molecular Mechanisms of Class B GPCR Activation: Insights from Adrenomedullin Receptors.

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Journal:  ACS Pharmacol Transl Sci       Date:  2020-02-26

9.  Distinct Patterns of Internalization of Different Calcitonin Gene-Related Peptide Receptors.

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10.  Picomolar Affinity Antagonist and Sustained Signaling Agonist Peptide Ligands for the Adrenomedullin and Calcitonin Gene-Related Peptide Receptors.

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