Selective antagonism of TRPA1 produces limited efficacy in models of inflammatory- and neuropathic-induced mechanical hypersensitivity in rats

The transient receptor potential ankyrin 1 (TRPA1) channel has been implicated in pathophysiological processes that include asthma, cough, and inflammatory pain. Agonists of TRPA1 such as mustard oil and its key component allyl isothiocyanate (AITC) cause pain and neurogenic inflammation in humans a...

Descripción completa

Detalles Bibliográficos
Autores principales: Lehto, Sonya G, Weyer, Andy D, Youngblood, Beth D, Zhang, Maosheng, Yin, Ruoyuan, Wang, Weiya, Teffera, Yohannes, Cooke, Melanie, Stucky, Cheryl L, Schenkel, Laurie, Geuns-Meyer, Stephanie, Moyer, Bryan D, Wild, Kenneth D, Gavva, Narender R
Formato: Online Artículo Texto
Lenguaje:English
Publicado: SAGE Publications 2016
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5131813/
https://www.ncbi.nlm.nih.gov/pubmed/27899696
http://dx.doi.org/10.1177/1744806916677761
_version_ 1782470949541511168
author Lehto, Sonya G
Weyer, Andy D
Youngblood, Beth D
Zhang, Maosheng
Yin, Ruoyuan
Wang, Weiya
Teffera, Yohannes
Cooke, Melanie
Stucky, Cheryl L
Schenkel, Laurie
Geuns-Meyer, Stephanie
Moyer, Bryan D
Wild, Kenneth D
Gavva, Narender R
author_facet Lehto, Sonya G
Weyer, Andy D
Youngblood, Beth D
Zhang, Maosheng
Yin, Ruoyuan
Wang, Weiya
Teffera, Yohannes
Cooke, Melanie
Stucky, Cheryl L
Schenkel, Laurie
Geuns-Meyer, Stephanie
Moyer, Bryan D
Wild, Kenneth D
Gavva, Narender R
author_sort Lehto, Sonya G
collection PubMed
description The transient receptor potential ankyrin 1 (TRPA1) channel has been implicated in pathophysiological processes that include asthma, cough, and inflammatory pain. Agonists of TRPA1 such as mustard oil and its key component allyl isothiocyanate (AITC) cause pain and neurogenic inflammation in humans and rodents, and TRPA1 antagonists have been reported to be effective in rodent models of pain. In our pursuit of TRPA1 antagonists as potential therapeutics, we generated AMG0902, a potent (IC(90) of 300 nM against rat TRPA1), selective, brain penetrant (brain to plasma ratio of 0.2), and orally bioavailable small molecule TRPA1 antagonist. AMG0902 reduced mechanically evoked C-fiber action potential firing in a skin-nerve preparation from mice previously injected with complete Freund’s adjuvant, supporting the role of TRPA1 in inflammatory mechanosensation. In vivo target coverage of TRPA1 by AMG0902 was demonstrated by the prevention of AITC-induced flinching/licking in rats. However, oral administration of AMG0902 to rats resulted in little to no efficacy in models of inflammatory, mechanically evoked hypersensitivity; and no efficacy was observed in a neuropathic pain model. Unbound plasma concentrations achieved in pain models were about 4-fold higher than the IC(90) concentration in the AITC target coverage model, suggesting that either greater target coverage is required for efficacy in the pain models studied or TRPA1 may not contribute significantly to the underlying mechanisms.
format Online
Article
Text
id pubmed-5131813
institution National Center for Biotechnology Information
language English
publishDate 2016
publisher SAGE Publications
record_format MEDLINE/PubMed
spelling pubmed-51318132016-12-07 Selective antagonism of TRPA1 produces limited efficacy in models of inflammatory- and neuropathic-induced mechanical hypersensitivity in rats Lehto, Sonya G Weyer, Andy D Youngblood, Beth D Zhang, Maosheng Yin, Ruoyuan Wang, Weiya Teffera, Yohannes Cooke, Melanie Stucky, Cheryl L Schenkel, Laurie Geuns-Meyer, Stephanie Moyer, Bryan D Wild, Kenneth D Gavva, Narender R Mol Pain Research Article The transient receptor potential ankyrin 1 (TRPA1) channel has been implicated in pathophysiological processes that include asthma, cough, and inflammatory pain. Agonists of TRPA1 such as mustard oil and its key component allyl isothiocyanate (AITC) cause pain and neurogenic inflammation in humans and rodents, and TRPA1 antagonists have been reported to be effective in rodent models of pain. In our pursuit of TRPA1 antagonists as potential therapeutics, we generated AMG0902, a potent (IC(90) of 300 nM against rat TRPA1), selective, brain penetrant (brain to plasma ratio of 0.2), and orally bioavailable small molecule TRPA1 antagonist. AMG0902 reduced mechanically evoked C-fiber action potential firing in a skin-nerve preparation from mice previously injected with complete Freund’s adjuvant, supporting the role of TRPA1 in inflammatory mechanosensation. In vivo target coverage of TRPA1 by AMG0902 was demonstrated by the prevention of AITC-induced flinching/licking in rats. However, oral administration of AMG0902 to rats resulted in little to no efficacy in models of inflammatory, mechanically evoked hypersensitivity; and no efficacy was observed in a neuropathic pain model. Unbound plasma concentrations achieved in pain models were about 4-fold higher than the IC(90) concentration in the AITC target coverage model, suggesting that either greater target coverage is required for efficacy in the pain models studied or TRPA1 may not contribute significantly to the underlying mechanisms. SAGE Publications 2016-11-29 /pmc/articles/PMC5131813/ /pubmed/27899696 http://dx.doi.org/10.1177/1744806916677761 Text en © The Author(s) 2016 http://creativecommons.org/licenses/by-nc/3.0/ This article is distributed under the terms of the Creative Commons Attribution-NonCommercial 3.0 License (http://www.creativecommons.org/licenses/by-nc/3.0/) which permits non-commercial use, reproduction and distribution of the work without further permission provided the original work is attributed as specified on the SAGE and Open Access pages (https://us.sagepub.com/en-us/nam/open-access-at-sage).
spellingShingle Research Article
Lehto, Sonya G
Weyer, Andy D
Youngblood, Beth D
Zhang, Maosheng
Yin, Ruoyuan
Wang, Weiya
Teffera, Yohannes
Cooke, Melanie
Stucky, Cheryl L
Schenkel, Laurie
Geuns-Meyer, Stephanie
Moyer, Bryan D
Wild, Kenneth D
Gavva, Narender R
Selective antagonism of TRPA1 produces limited efficacy in models of inflammatory- and neuropathic-induced mechanical hypersensitivity in rats
title Selective antagonism of TRPA1 produces limited efficacy in models of inflammatory- and neuropathic-induced mechanical hypersensitivity in rats
title_full Selective antagonism of TRPA1 produces limited efficacy in models of inflammatory- and neuropathic-induced mechanical hypersensitivity in rats
title_fullStr Selective antagonism of TRPA1 produces limited efficacy in models of inflammatory- and neuropathic-induced mechanical hypersensitivity in rats
title_full_unstemmed Selective antagonism of TRPA1 produces limited efficacy in models of inflammatory- and neuropathic-induced mechanical hypersensitivity in rats
title_short Selective antagonism of TRPA1 produces limited efficacy in models of inflammatory- and neuropathic-induced mechanical hypersensitivity in rats
title_sort selective antagonism of trpa1 produces limited efficacy in models of inflammatory- and neuropathic-induced mechanical hypersensitivity in rats
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5131813/
https://www.ncbi.nlm.nih.gov/pubmed/27899696
http://dx.doi.org/10.1177/1744806916677761
work_keys_str_mv AT lehtosonyag selectiveantagonismoftrpa1produceslimitedefficacyinmodelsofinflammatoryandneuropathicinducedmechanicalhypersensitivityinrats
AT weyerandyd selectiveantagonismoftrpa1produceslimitedefficacyinmodelsofinflammatoryandneuropathicinducedmechanicalhypersensitivityinrats
AT youngbloodbethd selectiveantagonismoftrpa1produceslimitedefficacyinmodelsofinflammatoryandneuropathicinducedmechanicalhypersensitivityinrats
AT zhangmaosheng selectiveantagonismoftrpa1produceslimitedefficacyinmodelsofinflammatoryandneuropathicinducedmechanicalhypersensitivityinrats
AT yinruoyuan selectiveantagonismoftrpa1produceslimitedefficacyinmodelsofinflammatoryandneuropathicinducedmechanicalhypersensitivityinrats
AT wangweiya selectiveantagonismoftrpa1produceslimitedefficacyinmodelsofinflammatoryandneuropathicinducedmechanicalhypersensitivityinrats
AT tefferayohannes selectiveantagonismoftrpa1produceslimitedefficacyinmodelsofinflammatoryandneuropathicinducedmechanicalhypersensitivityinrats
AT cookemelanie selectiveantagonismoftrpa1produceslimitedefficacyinmodelsofinflammatoryandneuropathicinducedmechanicalhypersensitivityinrats
AT stuckycheryll selectiveantagonismoftrpa1produceslimitedefficacyinmodelsofinflammatoryandneuropathicinducedmechanicalhypersensitivityinrats
AT schenkellaurie selectiveantagonismoftrpa1produceslimitedefficacyinmodelsofinflammatoryandneuropathicinducedmechanicalhypersensitivityinrats
AT geunsmeyerstephanie selectiveantagonismoftrpa1produceslimitedefficacyinmodelsofinflammatoryandneuropathicinducedmechanicalhypersensitivityinrats
AT moyerbryand selectiveantagonismoftrpa1produceslimitedefficacyinmodelsofinflammatoryandneuropathicinducedmechanicalhypersensitivityinrats
AT wildkennethd selectiveantagonismoftrpa1produceslimitedefficacyinmodelsofinflammatoryandneuropathicinducedmechanicalhypersensitivityinrats
AT gavvanarenderr selectiveantagonismoftrpa1produceslimitedefficacyinmodelsofinflammatoryandneuropathicinducedmechanicalhypersensitivityinrats

Ejemplares similares