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Striking parallels between carotid body glomus cell and adrenal chromaffin cell development

Carotid body glomus cells mediate essential reflex responses to arterial blood hypoxia. They are dopaminergic and secrete growth factors that support dopaminergic neurons, making the carotid body a potential source of patient-specific cells for Parkinson's disease therapy. Like adrenal chromaff...

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Autores principales: Hockman, Dorit, Adameyko, Igor, Kaucka, Marketa, Barraud, Perrine, Otani, Tomoki, Hunt, Adam, Hartwig, Anna C., Sock, Elisabeth, Waithe, Dominic, Franck, Marina C.M., Ernfors, Patrik, Ehinger, Sean, Howard, Marthe J., Brown, Naoko, Reese, Jeffrey, Baker, Clare V.H.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6453021/
https://www.ncbi.nlm.nih.gov/pubmed/29807017
http://dx.doi.org/10.1016/j.ydbio.2018.05.016
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author Hockman, Dorit
Adameyko, Igor
Kaucka, Marketa
Barraud, Perrine
Otani, Tomoki
Hunt, Adam
Hartwig, Anna C.
Sock, Elisabeth
Waithe, Dominic
Franck, Marina C.M.
Ernfors, Patrik
Ehinger, Sean
Howard, Marthe J.
Brown, Naoko
Reese, Jeffrey
Baker, Clare V.H.
author_facet Hockman, Dorit
Adameyko, Igor
Kaucka, Marketa
Barraud, Perrine
Otani, Tomoki
Hunt, Adam
Hartwig, Anna C.
Sock, Elisabeth
Waithe, Dominic
Franck, Marina C.M.
Ernfors, Patrik
Ehinger, Sean
Howard, Marthe J.
Brown, Naoko
Reese, Jeffrey
Baker, Clare V.H.
author_sort Hockman, Dorit
collection PubMed
description Carotid body glomus cells mediate essential reflex responses to arterial blood hypoxia. They are dopaminergic and secrete growth factors that support dopaminergic neurons, making the carotid body a potential source of patient-specific cells for Parkinson's disease therapy. Like adrenal chromaffin cells, which are also hypoxia-sensitive, glomus cells are neural crest-derived and require the transcription factors Ascl1 and Phox2b; otherwise, their development is little understood at the molecular level. Here, analysis in chicken and mouse reveals further striking molecular parallels, though also some differences, between glomus and adrenal chromaffin cell development. Moreover, histology has long suggested that glomus cell precursors are ‘émigrés’ from neighbouring ganglia/nerves, while multipotent nerve-associated glial cells are now known to make a significant contribution to the adrenal chromaffin cell population in the mouse. We present conditional genetic lineage-tracing data from mice supporting the hypothesis that progenitors expressing the glial marker proteolipid protein 1, presumably located in adjacent ganglia/nerves, also contribute to glomus cells. Finally, we resolve a paradox for the ‘émigré’ hypothesis in the chicken - where the nearest ganglion to the carotid body is the nodose, in which the satellite glia are neural crest-derived, but the neurons are almost entirely placode-derived - by fate-mapping putative nodose neuronal 'émigrés' to the neural crest.
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spelling pubmed-64530212019-04-19 Striking parallels between carotid body glomus cell and adrenal chromaffin cell development Hockman, Dorit Adameyko, Igor Kaucka, Marketa Barraud, Perrine Otani, Tomoki Hunt, Adam Hartwig, Anna C. Sock, Elisabeth Waithe, Dominic Franck, Marina C.M. Ernfors, Patrik Ehinger, Sean Howard, Marthe J. Brown, Naoko Reese, Jeffrey Baker, Clare V.H. Dev Biol Article Carotid body glomus cells mediate essential reflex responses to arterial blood hypoxia. They are dopaminergic and secrete growth factors that support dopaminergic neurons, making the carotid body a potential source of patient-specific cells for Parkinson's disease therapy. Like adrenal chromaffin cells, which are also hypoxia-sensitive, glomus cells are neural crest-derived and require the transcription factors Ascl1 and Phox2b; otherwise, their development is little understood at the molecular level. Here, analysis in chicken and mouse reveals further striking molecular parallels, though also some differences, between glomus and adrenal chromaffin cell development. Moreover, histology has long suggested that glomus cell precursors are ‘émigrés’ from neighbouring ganglia/nerves, while multipotent nerve-associated glial cells are now known to make a significant contribution to the adrenal chromaffin cell population in the mouse. We present conditional genetic lineage-tracing data from mice supporting the hypothesis that progenitors expressing the glial marker proteolipid protein 1, presumably located in adjacent ganglia/nerves, also contribute to glomus cells. Finally, we resolve a paradox for the ‘émigré’ hypothesis in the chicken - where the nearest ganglion to the carotid body is the nodose, in which the satellite glia are neural crest-derived, but the neurons are almost entirely placode-derived - by fate-mapping putative nodose neuronal 'émigrés' to the neural crest. Elsevier 2018-12-01 /pmc/articles/PMC6453021/ /pubmed/29807017 http://dx.doi.org/10.1016/j.ydbio.2018.05.016 Text en © 2018 The Authors http://creativecommons.org/licenses/by/4.0/ This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Hockman, Dorit
Adameyko, Igor
Kaucka, Marketa
Barraud, Perrine
Otani, Tomoki
Hunt, Adam
Hartwig, Anna C.
Sock, Elisabeth
Waithe, Dominic
Franck, Marina C.M.
Ernfors, Patrik
Ehinger, Sean
Howard, Marthe J.
Brown, Naoko
Reese, Jeffrey
Baker, Clare V.H.
Striking parallels between carotid body glomus cell and adrenal chromaffin cell development
title Striking parallels between carotid body glomus cell and adrenal chromaffin cell development
title_full Striking parallels between carotid body glomus cell and adrenal chromaffin cell development
title_fullStr Striking parallels between carotid body glomus cell and adrenal chromaffin cell development
title_full_unstemmed Striking parallels between carotid body glomus cell and adrenal chromaffin cell development
title_short Striking parallels between carotid body glomus cell and adrenal chromaffin cell development
title_sort striking parallels between carotid body glomus cell and adrenal chromaffin cell development
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6453021/
https://www.ncbi.nlm.nih.gov/pubmed/29807017
http://dx.doi.org/10.1016/j.ydbio.2018.05.016
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