CD24 Expression Identifies Teratogen-Sensitive Fetal Neural Stem Cell Subpopulations: Evidence from Developmental Ethanol Exposure and Orthotopic Cell Transfer Models

BACKGROUND: Ethanol is a potent teratogen. Its adverse neural effects are partly mediated by disrupting fetal neurogenesis. The teratogenic process is poorly understood, and vulnerable neurogenic stages have not been identified. Identifying these is a prerequisite for therapeutic interventions to mi...

Descripción completa

Detalles Bibliográficos
Autores principales: Tingling, Joseph D., Bake, Shameena, Holgate, Rhonda, Rawlings, Jeremy, Nagsuk, Phillips P., Chandrasekharan, Jayashree, Schneider, Sarah L., Miranda, Rajesh C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3718834/
https://www.ncbi.nlm.nih.gov/pubmed/23894503
http://dx.doi.org/10.1371/journal.pone.0069560
_version_ 1782277832902180864
author Tingling, Joseph D.
Bake, Shameena
Holgate, Rhonda
Rawlings, Jeremy
Nagsuk, Phillips P.
Chandrasekharan, Jayashree
Schneider, Sarah L.
Miranda, Rajesh C.
author_facet Tingling, Joseph D.
Bake, Shameena
Holgate, Rhonda
Rawlings, Jeremy
Nagsuk, Phillips P.
Chandrasekharan, Jayashree
Schneider, Sarah L.
Miranda, Rajesh C.
author_sort Tingling, Joseph D.
collection PubMed
description BACKGROUND: Ethanol is a potent teratogen. Its adverse neural effects are partly mediated by disrupting fetal neurogenesis. The teratogenic process is poorly understood, and vulnerable neurogenic stages have not been identified. Identifying these is a prerequisite for therapeutic interventions to mitigate effects of teratogen exposures. METHODS: We used flow cytometry and qRT-PCR to screen fetal mouse-derived neurosphere cultures for ethanol-sensitive neural stem cell (NSC) subpopulations, to study NSC renewal and differentiation. The identity of vulnerable NSC populations was validated in vivo, using a maternal ethanol exposure model. Finally, the effect of ethanol exposure on the ability of vulnerable NSC subpopulations to integrate into the fetal neurogenic environment was assessed following ultrasound guided, adoptive transfer. RESULTS: Ethanol decreased NSC mRNAs for c-kit, Musashi-1and GFAP. The CD24(+) NSC population, specifically the CD24(+)CD15(+) double-positive subpopulation, was selectively decreased by ethanol. Maternal ethanol exposure also resulted in decreased fetal forebrain CD24 expression. Ethanol pre-exposed CD24(+) cells exhibited increased proliferation, and deficits in cell-autonomous and cue-directed neuronal differentiation, and following orthotopic transplantation into naïve fetuses, were unable to integrate into neurogenic niches. CD24(depleted) cells retained neurosphere regeneration capacity, but following ethanol exposure, generated increased numbers of CD24(+) cells relative to controls. CONCLUSIONS: Neuronal lineage committed CD24(+) cells exhibit specific vulnerability, and ethanol exposure persistently impairs this population’s cell-autonomous differentiation capacity. CD24(+) cells may additionally serve as quorum sensors within neurogenic niches; their loss, leading to compensatory NSC activation, perhaps depleting renewal capacity. These data collectively advance a mechanistic hypothesis for teratogenesis leading to microencephaly.
format Online
Article
Text
id pubmed-3718834
institution National Center for Biotechnology Information
language English
publishDate 2013
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-37188342013-07-26 CD24 Expression Identifies Teratogen-Sensitive Fetal Neural Stem Cell Subpopulations: Evidence from Developmental Ethanol Exposure and Orthotopic Cell Transfer Models Tingling, Joseph D. Bake, Shameena Holgate, Rhonda Rawlings, Jeremy Nagsuk, Phillips P. Chandrasekharan, Jayashree Schneider, Sarah L. Miranda, Rajesh C. PLoS One Research Article BACKGROUND: Ethanol is a potent teratogen. Its adverse neural effects are partly mediated by disrupting fetal neurogenesis. The teratogenic process is poorly understood, and vulnerable neurogenic stages have not been identified. Identifying these is a prerequisite for therapeutic interventions to mitigate effects of teratogen exposures. METHODS: We used flow cytometry and qRT-PCR to screen fetal mouse-derived neurosphere cultures for ethanol-sensitive neural stem cell (NSC) subpopulations, to study NSC renewal and differentiation. The identity of vulnerable NSC populations was validated in vivo, using a maternal ethanol exposure model. Finally, the effect of ethanol exposure on the ability of vulnerable NSC subpopulations to integrate into the fetal neurogenic environment was assessed following ultrasound guided, adoptive transfer. RESULTS: Ethanol decreased NSC mRNAs for c-kit, Musashi-1and GFAP. The CD24(+) NSC population, specifically the CD24(+)CD15(+) double-positive subpopulation, was selectively decreased by ethanol. Maternal ethanol exposure also resulted in decreased fetal forebrain CD24 expression. Ethanol pre-exposed CD24(+) cells exhibited increased proliferation, and deficits in cell-autonomous and cue-directed neuronal differentiation, and following orthotopic transplantation into naïve fetuses, were unable to integrate into neurogenic niches. CD24(depleted) cells retained neurosphere regeneration capacity, but following ethanol exposure, generated increased numbers of CD24(+) cells relative to controls. CONCLUSIONS: Neuronal lineage committed CD24(+) cells exhibit specific vulnerability, and ethanol exposure persistently impairs this population’s cell-autonomous differentiation capacity. CD24(+) cells may additionally serve as quorum sensors within neurogenic niches; their loss, leading to compensatory NSC activation, perhaps depleting renewal capacity. These data collectively advance a mechanistic hypothesis for teratogenesis leading to microencephaly. Public Library of Science 2013-07-22 /pmc/articles/PMC3718834/ /pubmed/23894503 http://dx.doi.org/10.1371/journal.pone.0069560 Text en © 2013 Tingling et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Tingling, Joseph D.
Bake, Shameena
Holgate, Rhonda
Rawlings, Jeremy
Nagsuk, Phillips P.
Chandrasekharan, Jayashree
Schneider, Sarah L.
Miranda, Rajesh C.
CD24 Expression Identifies Teratogen-Sensitive Fetal Neural Stem Cell Subpopulations: Evidence from Developmental Ethanol Exposure and Orthotopic Cell Transfer Models
title CD24 Expression Identifies Teratogen-Sensitive Fetal Neural Stem Cell Subpopulations: Evidence from Developmental Ethanol Exposure and Orthotopic Cell Transfer Models
title_full CD24 Expression Identifies Teratogen-Sensitive Fetal Neural Stem Cell Subpopulations: Evidence from Developmental Ethanol Exposure and Orthotopic Cell Transfer Models
title_fullStr CD24 Expression Identifies Teratogen-Sensitive Fetal Neural Stem Cell Subpopulations: Evidence from Developmental Ethanol Exposure and Orthotopic Cell Transfer Models
title_full_unstemmed CD24 Expression Identifies Teratogen-Sensitive Fetal Neural Stem Cell Subpopulations: Evidence from Developmental Ethanol Exposure and Orthotopic Cell Transfer Models
title_short CD24 Expression Identifies Teratogen-Sensitive Fetal Neural Stem Cell Subpopulations: Evidence from Developmental Ethanol Exposure and Orthotopic Cell Transfer Models
title_sort cd24 expression identifies teratogen-sensitive fetal neural stem cell subpopulations: evidence from developmental ethanol exposure and orthotopic cell transfer models
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3718834/
https://www.ncbi.nlm.nih.gov/pubmed/23894503
http://dx.doi.org/10.1371/journal.pone.0069560
work_keys_str_mv AT tinglingjosephd cd24expressionidentifiesteratogensensitivefetalneuralstemcellsubpopulationsevidencefromdevelopmentalethanolexposureandorthotopiccelltransfermodels
AT bakeshameena cd24expressionidentifiesteratogensensitivefetalneuralstemcellsubpopulationsevidencefromdevelopmentalethanolexposureandorthotopiccelltransfermodels
AT holgaterhonda cd24expressionidentifiesteratogensensitivefetalneuralstemcellsubpopulationsevidencefromdevelopmentalethanolexposureandorthotopiccelltransfermodels
AT rawlingsjeremy cd24expressionidentifiesteratogensensitivefetalneuralstemcellsubpopulationsevidencefromdevelopmentalethanolexposureandorthotopiccelltransfermodels
AT nagsukphillipsp cd24expressionidentifiesteratogensensitivefetalneuralstemcellsubpopulationsevidencefromdevelopmentalethanolexposureandorthotopiccelltransfermodels
AT chandrasekharanjayashree cd24expressionidentifiesteratogensensitivefetalneuralstemcellsubpopulationsevidencefromdevelopmentalethanolexposureandorthotopiccelltransfermodels
AT schneidersarahl cd24expressionidentifiesteratogensensitivefetalneuralstemcellsubpopulationsevidencefromdevelopmentalethanolexposureandorthotopiccelltransfermodels
AT mirandarajeshc cd24expressionidentifiesteratogensensitivefetalneuralstemcellsubpopulationsevidencefromdevelopmentalethanolexposureandorthotopiccelltransfermodels

Ejemplares similares