Modulating the activity of human nociceptors with a SCN10A promoter-specific viral vector tool

Despite the high prevalence of chronic pain as a disease in our society, there is a lack of effective treatment options for patients living with this condition. Gene therapies using recombinant AAVs are a direct method to selectively express genes of interest in target cells with the potential of, i...

Descripción completa

Detalles Bibliográficos
Autores principales: Mouchbahani-Constance, Stephanie, Lagard, Camille, Schweizer, Justine, Labonté, Isabelle, Georgiopoulos, Miltiadis, Otis, Colombe, St-Louis, Manon, Troncy, Eric, Sarret, Philippe, Ribeiro-Da-Silva, Alfredo, Ouellet, Jean A., Séguéla, Philippe, Paquet, Marie-Eve, Sharif-Naeini, Reza
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2023
Materias:
Original Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9932673/
https://www.ncbi.nlm.nih.gov/pubmed/36816616
http://dx.doi.org/10.1016/j.ynpai.2023.100120
_version_ 1784889505941028864
author Mouchbahani-Constance, Stephanie
Lagard, Camille
Schweizer, Justine
Labonté, Isabelle
Georgiopoulos, Miltiadis
Otis, Colombe
St-Louis, Manon
Troncy, Eric
Sarret, Philippe
Ribeiro-Da-Silva, Alfredo
Ouellet, Jean A.
Séguéla, Philippe
Paquet, Marie-Eve
Sharif-Naeini, Reza
author_facet Mouchbahani-Constance, Stephanie
Lagard, Camille
Schweizer, Justine
Labonté, Isabelle
Georgiopoulos, Miltiadis
Otis, Colombe
St-Louis, Manon
Troncy, Eric
Sarret, Philippe
Ribeiro-Da-Silva, Alfredo
Ouellet, Jean A.
Séguéla, Philippe
Paquet, Marie-Eve
Sharif-Naeini, Reza
author_sort Mouchbahani-Constance, Stephanie
collection PubMed
description Despite the high prevalence of chronic pain as a disease in our society, there is a lack of effective treatment options for patients living with this condition. Gene therapies using recombinant AAVs are a direct method to selectively express genes of interest in target cells with the potential of, in the case of nociceptors, reducing neuronal firing in pain conditions. We designed a recombinant AAV vector expressing cargos whose expression was driven by a portion of the SCN10A (Na(V)1.8) promoter, which is predominantly active in nociceptors. We validated its specificity for nociceptors in mouse and human dorsal root ganglia and showed that it can drive the expression of functional proteins. Our viral vector and promoter package drove the expression of both excitatory or inhibitory DREADDs in primary human DRG cultures and in whole cell electrophysiology experiments, increased or decreased neuronal firing, respectively. Taken together, we present a novel viral tool that drives expression of cargo specifically in human nociceptors. This will allow for future specific studies of human nociceptor properties as well as pave the way for potential future gene therapies for chronic pain.
format Online
Article
Text
id pubmed-9932673
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher Elsevier
record_format MEDLINE/PubMed
spelling pubmed-99326732023-02-17 Modulating the activity of human nociceptors with a SCN10A promoter-specific viral vector tool Mouchbahani-Constance, Stephanie Lagard, Camille Schweizer, Justine Labonté, Isabelle Georgiopoulos, Miltiadis Otis, Colombe St-Louis, Manon Troncy, Eric Sarret, Philippe Ribeiro-Da-Silva, Alfredo Ouellet, Jean A. Séguéla, Philippe Paquet, Marie-Eve Sharif-Naeini, Reza Neurobiol Pain Original Research Article Despite the high prevalence of chronic pain as a disease in our society, there is a lack of effective treatment options for patients living with this condition. Gene therapies using recombinant AAVs are a direct method to selectively express genes of interest in target cells with the potential of, in the case of nociceptors, reducing neuronal firing in pain conditions. We designed a recombinant AAV vector expressing cargos whose expression was driven by a portion of the SCN10A (Na(V)1.8) promoter, which is predominantly active in nociceptors. We validated its specificity for nociceptors in mouse and human dorsal root ganglia and showed that it can drive the expression of functional proteins. Our viral vector and promoter package drove the expression of both excitatory or inhibitory DREADDs in primary human DRG cultures and in whole cell electrophysiology experiments, increased or decreased neuronal firing, respectively. Taken together, we present a novel viral tool that drives expression of cargo specifically in human nociceptors. This will allow for future specific studies of human nociceptor properties as well as pave the way for potential future gene therapies for chronic pain. Elsevier 2023-01-30 /pmc/articles/PMC9932673/ /pubmed/36816616 http://dx.doi.org/10.1016/j.ynpai.2023.100120 Text en © 2023 The Authors https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Original Research Article
Mouchbahani-Constance, Stephanie
Lagard, Camille
Schweizer, Justine
Labonté, Isabelle
Georgiopoulos, Miltiadis
Otis, Colombe
St-Louis, Manon
Troncy, Eric
Sarret, Philippe
Ribeiro-Da-Silva, Alfredo
Ouellet, Jean A.
Séguéla, Philippe
Paquet, Marie-Eve
Sharif-Naeini, Reza
Modulating the activity of human nociceptors with a SCN10A promoter-specific viral vector tool
title Modulating the activity of human nociceptors with a SCN10A promoter-specific viral vector tool
title_full Modulating the activity of human nociceptors with a SCN10A promoter-specific viral vector tool
title_fullStr Modulating the activity of human nociceptors with a SCN10A promoter-specific viral vector tool
title_full_unstemmed Modulating the activity of human nociceptors with a SCN10A promoter-specific viral vector tool
title_short Modulating the activity of human nociceptors with a SCN10A promoter-specific viral vector tool
title_sort modulating the activity of human nociceptors with a scn10a promoter-specific viral vector tool
topic Original Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9932673/
https://www.ncbi.nlm.nih.gov/pubmed/36816616
http://dx.doi.org/10.1016/j.ynpai.2023.100120
work_keys_str_mv AT mouchbahaniconstancestephanie modulatingtheactivityofhumannociceptorswithascn10apromoterspecificviralvectortool
AT lagardcamille modulatingtheactivityofhumannociceptorswithascn10apromoterspecificviralvectortool
AT schweizerjustine modulatingtheactivityofhumannociceptorswithascn10apromoterspecificviralvectortool
AT labonteisabelle modulatingtheactivityofhumannociceptorswithascn10apromoterspecificviralvectortool
AT georgiopoulosmiltiadis modulatingtheactivityofhumannociceptorswithascn10apromoterspecificviralvectortool
AT otiscolombe modulatingtheactivityofhumannociceptorswithascn10apromoterspecificviralvectortool
AT stlouismanon modulatingtheactivityofhumannociceptorswithascn10apromoterspecificviralvectortool
AT troncyeric modulatingtheactivityofhumannociceptorswithascn10apromoterspecificviralvectortool
AT sarretphilippe modulatingtheactivityofhumannociceptorswithascn10apromoterspecificviralvectortool
AT ribeirodasilvaalfredo modulatingtheactivityofhumannociceptorswithascn10apromoterspecificviralvectortool
AT ouelletjeana modulatingtheactivityofhumannociceptorswithascn10apromoterspecificviralvectortool
AT seguelaphilippe modulatingtheactivityofhumannociceptorswithascn10apromoterspecificviralvectortool
AT paquetmarieeve modulatingtheactivityofhumannociceptorswithascn10apromoterspecificviralvectortool
AT sharifnaeinireza modulatingtheactivityofhumannociceptorswithascn10apromoterspecificviralvectortool

Ejemplares similares