TRP Channels in Visceral Pain

Blackshaw, L. Ashley; Brierley, Stuart M.; Harrington, Andrea M.; Hughes, Patrick A.

TRP Channels in Visceral Pain

L. Ashley Blackshaw^{1, 2, *}, Stuart M. Brierley², Andrea M. Harrington², Patrick A. Hughes²

¹ Wingate Institute for Neurogastroenterology, Centre for Digestive Diseases, Institute of Cell and Molecular Science, Barts and The London School of Medicine and Dentistry, Queen Mary University of London

² Nerve-Gut Research Laboratory, Discipline of Medicine, The University of Adelaide, Adelaide, South Australia, Australia 5000

Article Information

Identifiers and Pagination:

Year: 2013
Volume: 6
First Page: 23
Last Page: 30
Publisher ID: TOPAINJ-6-23
DOI: 10.2174/1876386301306010023

Article History:

Received Date: 09/08/2012
Revision Received Date: 09/08/2012
Acceptance Date: 16/08/2012
Electronic publication date: 08/3/2013
Collection year: 2013

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© 2013 Blackshaw et al.

open-access license: This is an open access article distributed under the terms of the Creative Commons Attribution 4.0 International Public License (CC-BY 4.0), a copy of which is available at: https://creativecommons.org/licenses/by/4.0/legalcode. This license permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

^* Address correspondence to this author at the Wingate Institute, 26 Ashfield Street, London E1 2AJ, UK; Tel: +44 207 882 2636; E-mail: a.blackshaw@qmul.ac.uk

Visceral pain is both different and similar to somatic pain - different in being poorly localized and usually referred elsewhere to the body wall, but similar in many of the molecular mechanisms it employs (like TRP channels) and the specialization of afferent endings to detect painful stimuli. TRPV1 is sensitive to low pH. pH is lowest in gastric juice, which may cause severe pain when exposed to the oesophageal mucosa, and probably works via TRPV1. TRPV1 is found in afferent fibres throughout the viscera, and the TRPV1 agonist capsaicin can recapitulate symptoms experienced in disease. TRPV1 is also involved in normal mechanosensory function in the gut. Roles for TRPV4 and TRPA1 have also been described in visceral afferents, and TRPV4 is highly enriched in them, where it plays a major role in both mechanonociception and chemonociception. It may provide a visceral-specific nociceptor target for drug development. TRPA1 is also involved in mechano-and chemosensory function, but not as selectively as TRPV4. TRPA1 is colocalized with TRPV1 in visceral afferents, where they influence each other's function. Another modulator of TRPV1 is the cool/mint receptor TRPM8, which, when activated can abrogate responses mediated via TRPV1, suggesting that TRPM8 agonists may provide analgesia via this pathway. In all, the viscera are rich in TRP channel targets on nociceptive neurones which we hope will provide opportunities for therapeutic analgesia.

Keywords: Pain, Mechanosensitivity, Inflammation.

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RESEARCH ARTICLE

TRP Channels in Visceral Pain

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