Neural crest cell survival is dependent on Rho kinase and is required for development of the mid face in mouse embryos.

Neural crest cell survival is dependent on Rho kinase and is required for development of the mid face in mouse embryos.

Neural crest cells (NCC) give rise to much of the tissue that forms the vertebrate head and face, including cartilage and bone, cranial ganglia and teeth. In this study we show that conditional expression of a dominant-negative (DN) form of Rho kinase (Rock) in mouse NCC results in severe hypoplasia...

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Main Authors: Helen M Phillips, Tania Papoutsi, Helena Soenen, Patricia Ybot-Gonzalez, Deborah J Henderson, Bill Chaudhry
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3357402?pdf=render
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spelling doaj-2d40986f34ef450587231f50ca5358002020-11-25T01:52:50ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-0175e3768510.1371/journal.pone.0037685Neural crest cell survival is dependent on Rho kinase and is required for development of the mid face in mouse embryos.Helen M PhillipsTania PapoutsiHelena SoenenPatricia Ybot-GonzalezDeborah J HendersonBill ChaudhryNeural crest cells (NCC) give rise to much of the tissue that forms the vertebrate head and face, including cartilage and bone, cranial ganglia and teeth. In this study we show that conditional expression of a dominant-negative (DN) form of Rho kinase (Rock) in mouse NCC results in severe hypoplasia of the frontonasal processes and first pharyngeal arch, ultimately resulting in reduction of the maxilla and nasal bones and severe craniofacial clefting affecting the nose, palate and lip. These defects resemble frontonasal dysplasia in humans. Disruption of the actin cytoskeleton, which leads to abnormalities in cell-matrix attachment, is seen in the RockDN;Wnt1-cre mutant embryos. This leads to elevated cell death, resulting in NCC deficiency and hypoplastic NCC-derived craniofacial structures. Rock is thus essential for survival of NCC that form the craniofacial region. We propose that reduced NCC numbers in the frontonasal processes and first pharyngeal arch, resulting from exacerbated cell death, may be the common mechanism underlying frontonasal dysplasia.http://europepmc.org/articles/PMC3357402?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Helen M Phillips
Tania Papoutsi
Helena Soenen
Patricia Ybot-Gonzalez
Deborah J Henderson
Bill Chaudhry
spellingShingle Helen M Phillips
Tania Papoutsi
Helena Soenen
Patricia Ybot-Gonzalez
Deborah J Henderson
Bill Chaudhry
Neural crest cell survival is dependent on Rho kinase and is required for development of the mid face in mouse embryos.
PLoS ONE
author_facet Helen M Phillips
Tania Papoutsi
Helena Soenen
Patricia Ybot-Gonzalez
Deborah J Henderson
Bill Chaudhry
author_sort Helen M Phillips
title Neural crest cell survival is dependent on Rho kinase and is required for development of the mid face in mouse embryos.
title_short Neural crest cell survival is dependent on Rho kinase and is required for development of the mid face in mouse embryos.
title_full Neural crest cell survival is dependent on Rho kinase and is required for development of the mid face in mouse embryos.
title_fullStr Neural crest cell survival is dependent on Rho kinase and is required for development of the mid face in mouse embryos.
title_full_unstemmed Neural crest cell survival is dependent on Rho kinase and is required for development of the mid face in mouse embryos.
title_sort neural crest cell survival is dependent on rho kinase and is required for development of the mid face in mouse embryos.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description Neural crest cells (NCC) give rise to much of the tissue that forms the vertebrate head and face, including cartilage and bone, cranial ganglia and teeth. In this study we show that conditional expression of a dominant-negative (DN) form of Rho kinase (Rock) in mouse NCC results in severe hypoplasia of the frontonasal processes and first pharyngeal arch, ultimately resulting in reduction of the maxilla and nasal bones and severe craniofacial clefting affecting the nose, palate and lip. These defects resemble frontonasal dysplasia in humans. Disruption of the actin cytoskeleton, which leads to abnormalities in cell-matrix attachment, is seen in the RockDN;Wnt1-cre mutant embryos. This leads to elevated cell death, resulting in NCC deficiency and hypoplastic NCC-derived craniofacial structures. Rock is thus essential for survival of NCC that form the craniofacial region. We propose that reduced NCC numbers in the frontonasal processes and first pharyngeal arch, resulting from exacerbated cell death, may be the common mechanism underlying frontonasal dysplasia.
url http://europepmc.org/articles/PMC3357402?pdf=render
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AT taniapapoutsi neuralcrestcellsurvivalisdependentonrhokinaseandisrequiredfordevelopmentofthemidfaceinmouseembryos
AT helenasoenen neuralcrestcellsurvivalisdependentonrhokinaseandisrequiredfordevelopmentofthemidfaceinmouseembryos
AT patriciaybotgonzalez neuralcrestcellsurvivalisdependentonrhokinaseandisrequiredfordevelopmentofthemidfaceinmouseembryos
AT deborahjhenderson neuralcrestcellsurvivalisdependentonrhokinaseandisrequiredfordevelopmentofthemidfaceinmouseembryos
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