A SAGE-based screen for genes expressed in sub-populations of neurons in the mouse dorsal root ganglion

BACKGROUND: The different sensory modalities temperature, pain, touch and muscle proprioception are carried by somatosensory neurons of the dorsal root ganglia. Study of this system is hampered by the lack of molecular markers for many of these neuronal sub-types. In order to detect genes expressed...

Descripción completa

Detalles Bibliográficos
Autores principales: Bourane, Steeve, Méchaly, Ilana, Venteo, Stéphanie, Garces, Alain, Fichard, Agnes, Valmier, Jean, Carroll, Patrick
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2007
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2241628/
https://www.ncbi.nlm.nih.gov/pubmed/18021428
http://dx.doi.org/10.1186/1471-2202-8-97
_version_ 1782150524562309120
author Bourane, Steeve
Méchaly, Ilana
Venteo, Stéphanie
Garces, Alain
Fichard, Agnes
Valmier, Jean
Carroll, Patrick
author_facet Bourane, Steeve
Méchaly, Ilana
Venteo, Stéphanie
Garces, Alain
Fichard, Agnes
Valmier, Jean
Carroll, Patrick
author_sort Bourane, Steeve
collection PubMed
description BACKGROUND: The different sensory modalities temperature, pain, touch and muscle proprioception are carried by somatosensory neurons of the dorsal root ganglia. Study of this system is hampered by the lack of molecular markers for many of these neuronal sub-types. In order to detect genes expressed in sub-populations of somatosensory neurons, gene profiling was carried out on wild-type and TrkA mutant neonatal dorsal root ganglia (DRG) using SAGE (serial analysis of gene expression) methodology. Thermo-nociceptors constitute up to 80 % of the neurons in the DRG. In TrkA mutant DRGs, the nociceptor sub-class of sensory neurons is lost due to absence of nerve growth factor survival signaling through its receptor TrkA. Thus, comparison of wild-type and TrkA mutants allows the identification of transcripts preferentially expressed in the nociceptor or mechano-proprioceptor subclasses, respectively. RESULTS: Our comparison revealed 240 genes differentially expressed between the two tissues (P < 0.01). Some of these genes, CGRP, Scn10a are known markers of sensory neuron sub-types. Several potential markers of sub-populations, Dok4, Crip2 and Grik1/GluR5 were further analyzed by quantitative RT-PCR and double labeling with TrkA,-B,-C, c-ret, parvalbumin and isolectin B4, known markers of DRG neuron sub-types. Expression of Grik1/GluR5 was restricted to the isolectin B4+ nociceptive population, while Dok4 and Crip2 had broader expression profiles. Crip2 expression was however excluded from the proprioceptor sub-population. CONCLUSION: We have identified and characterized the detailed expression patterns of three genes in the developing DRG, placing them in the context of the known major neuronal sub-types defined by molecular markers. Further analysis of differentially expressed genes in this tissue promises to extend our knowledge of the molecular diversity of different cell types and forms the basis for understanding their particular functional specificities.
format Text
id pubmed-2241628
institution National Center for Biotechnology Information
language English
publishDate 2007
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-22416282008-02-13 A SAGE-based screen for genes expressed in sub-populations of neurons in the mouse dorsal root ganglion Bourane, Steeve Méchaly, Ilana Venteo, Stéphanie Garces, Alain Fichard, Agnes Valmier, Jean Carroll, Patrick BMC Neurosci Research Article BACKGROUND: The different sensory modalities temperature, pain, touch and muscle proprioception are carried by somatosensory neurons of the dorsal root ganglia. Study of this system is hampered by the lack of molecular markers for many of these neuronal sub-types. In order to detect genes expressed in sub-populations of somatosensory neurons, gene profiling was carried out on wild-type and TrkA mutant neonatal dorsal root ganglia (DRG) using SAGE (serial analysis of gene expression) methodology. Thermo-nociceptors constitute up to 80 % of the neurons in the DRG. In TrkA mutant DRGs, the nociceptor sub-class of sensory neurons is lost due to absence of nerve growth factor survival signaling through its receptor TrkA. Thus, comparison of wild-type and TrkA mutants allows the identification of transcripts preferentially expressed in the nociceptor or mechano-proprioceptor subclasses, respectively. RESULTS: Our comparison revealed 240 genes differentially expressed between the two tissues (P < 0.01). Some of these genes, CGRP, Scn10a are known markers of sensory neuron sub-types. Several potential markers of sub-populations, Dok4, Crip2 and Grik1/GluR5 were further analyzed by quantitative RT-PCR and double labeling with TrkA,-B,-C, c-ret, parvalbumin and isolectin B4, known markers of DRG neuron sub-types. Expression of Grik1/GluR5 was restricted to the isolectin B4+ nociceptive population, while Dok4 and Crip2 had broader expression profiles. Crip2 expression was however excluded from the proprioceptor sub-population. CONCLUSION: We have identified and characterized the detailed expression patterns of three genes in the developing DRG, placing them in the context of the known major neuronal sub-types defined by molecular markers. Further analysis of differentially expressed genes in this tissue promises to extend our knowledge of the molecular diversity of different cell types and forms the basis for understanding their particular functional specificities. BioMed Central 2007-11-19 /pmc/articles/PMC2241628/ /pubmed/18021428 http://dx.doi.org/10.1186/1471-2202-8-97 Text en Copyright © 2007 Bourane et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( (http://creativecommons.org/licenses/by/2.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Bourane, Steeve
Méchaly, Ilana
Venteo, Stéphanie
Garces, Alain
Fichard, Agnes
Valmier, Jean
Carroll, Patrick
A SAGE-based screen for genes expressed in sub-populations of neurons in the mouse dorsal root ganglion
title A SAGE-based screen for genes expressed in sub-populations of neurons in the mouse dorsal root ganglion
title_full A SAGE-based screen for genes expressed in sub-populations of neurons in the mouse dorsal root ganglion
title_fullStr A SAGE-based screen for genes expressed in sub-populations of neurons in the mouse dorsal root ganglion
title_full_unstemmed A SAGE-based screen for genes expressed in sub-populations of neurons in the mouse dorsal root ganglion
title_short A SAGE-based screen for genes expressed in sub-populations of neurons in the mouse dorsal root ganglion
title_sort sage-based screen for genes expressed in sub-populations of neurons in the mouse dorsal root ganglion
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2241628/
https://www.ncbi.nlm.nih.gov/pubmed/18021428
http://dx.doi.org/10.1186/1471-2202-8-97
work_keys_str_mv AT bouranesteeve asagebasedscreenforgenesexpressedinsubpopulationsofneuronsinthemousedorsalrootganglion
AT mechalyilana asagebasedscreenforgenesexpressedinsubpopulationsofneuronsinthemousedorsalrootganglion
AT venteostephanie asagebasedscreenforgenesexpressedinsubpopulationsofneuronsinthemousedorsalrootganglion
AT garcesalain asagebasedscreenforgenesexpressedinsubpopulationsofneuronsinthemousedorsalrootganglion
AT fichardagnes asagebasedscreenforgenesexpressedinsubpopulationsofneuronsinthemousedorsalrootganglion
AT valmierjean asagebasedscreenforgenesexpressedinsubpopulationsofneuronsinthemousedorsalrootganglion
AT carrollpatrick asagebasedscreenforgenesexpressedinsubpopulationsofneuronsinthemousedorsalrootganglion
AT bouranesteeve sagebasedscreenforgenesexpressedinsubpopulationsofneuronsinthemousedorsalrootganglion
AT mechalyilana sagebasedscreenforgenesexpressedinsubpopulationsofneuronsinthemousedorsalrootganglion
AT venteostephanie sagebasedscreenforgenesexpressedinsubpopulationsofneuronsinthemousedorsalrootganglion
AT garcesalain sagebasedscreenforgenesexpressedinsubpopulationsofneuronsinthemousedorsalrootganglion
AT fichardagnes sagebasedscreenforgenesexpressedinsubpopulationsofneuronsinthemousedorsalrootganglion
AT valmierjean sagebasedscreenforgenesexpressedinsubpopulationsofneuronsinthemousedorsalrootganglion
AT carrollpatrick sagebasedscreenforgenesexpressedinsubpopulationsofneuronsinthemousedorsalrootganglion

Ejemplares similares