Activation of p38 MAPK pathway in the skull abnormalities of Apert syndrome Fgfr2(+P253R )mice

BACKGROUND: Apert syndrome is characterized by craniosynostosis and limb abnormalities and is primarily caused by FGFR2 +/P253R and +/S252W mutations. The former mutation is present in approximately one third whereas the latter mutation is present in two-thirds of the patients with this condition. W...

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Autores principales: Wang, Yingli, Sun, Miao, Uhlhorn, Victoria L, Zhou, Xueyan, Peter, Inga, Martinez-Abadias, Neus, Hill, Cheryl A, Percival, Christopher J, Richtsmeier, Joan T, Huso, David L, Jabs, Ethylin Wang
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2010
Materias:
Research article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2838826/
https://www.ncbi.nlm.nih.gov/pubmed/20175913
http://dx.doi.org/10.1186/1471-213X-10-22
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author Wang, Yingli
Sun, Miao
Uhlhorn, Victoria L
Zhou, Xueyan
Peter, Inga
Martinez-Abadias, Neus
Hill, Cheryl A
Percival, Christopher J
Richtsmeier, Joan T
Huso, David L
Jabs, Ethylin Wang
author_facet Wang, Yingli
Sun, Miao
Uhlhorn, Victoria L
Zhou, Xueyan
Peter, Inga
Martinez-Abadias, Neus
Hill, Cheryl A
Percival, Christopher J
Richtsmeier, Joan T
Huso, David L
Jabs, Ethylin Wang
author_sort Wang, Yingli
collection PubMed
description BACKGROUND: Apert syndrome is characterized by craniosynostosis and limb abnormalities and is primarily caused by FGFR2 +/P253R and +/S252W mutations. The former mutation is present in approximately one third whereas the latter mutation is present in two-thirds of the patients with this condition. We previously reported an inbred transgenic mouse model with the Fgfr2 +/S252W mutation on the C57BL/6J background for Apert syndrome. Here we present a mouse model for the Fgfr2+/P253R mutation. RESULTS: We generated inbred Fgfr2(+/P253R )mice on the same C56BL/6J genetic background and analyzed their skeletal abnormalities. 3D micro-CT scans of the skulls of the Fgfr2(+/P253R )mice revealed that the skull length was shortened with the length of the anterior cranial base significantly shorter than that of the Fgfr2(+/S252W )mice at P0. The Fgfr2(+/P253R )mice presented with synostosis of the coronal suture and proximate fronts with disorganized cellularity in sagittal and lambdoid sutures. Abnormal osteogenesis and proliferation were observed at the developing coronal suture and long bones of the Fgfr2(+/P253R )mice as in the Fgfr2(+/S252W )mice. Activation of mitogen-activated protein kinases (MAPK) was observed in the Fgfr2(+/P253R )neurocranium with an increase in phosphorylated p38 as well as ERK1/2, whereas phosphorylated AKT and PKCα were not obviously changed as compared to those of wild-type controls. There were localized phenotypic and molecular variations among individual embryos with different mutations and among those with the same mutation. CONCLUSIONS: Our in vivo studies demonstrated that the Fgfr2 +/P253R mutation resulted in mice with cranial features that resemble those of the Fgfr2(+/S252W )mice and human Apert syndrome. Activated p38 in addition to the ERK1/2 signaling pathways may mediate the mutant neurocranial phenotype. Though Apert syndrome is traditionally thought to be a consistent phenotype, our results suggest localized and regional variations in the phenotypes that characterize Apert syndrome.
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spelling pubmed-28388262010-03-16 Activation of p38 MAPK pathway in the skull abnormalities of Apert syndrome Fgfr2(+P253R )mice Wang, Yingli Sun, Miao Uhlhorn, Victoria L Zhou, Xueyan Peter, Inga Martinez-Abadias, Neus Hill, Cheryl A Percival, Christopher J Richtsmeier, Joan T Huso, David L Jabs, Ethylin Wang BMC Dev Biol Research article BACKGROUND: Apert syndrome is characterized by craniosynostosis and limb abnormalities and is primarily caused by FGFR2 +/P253R and +/S252W mutations. The former mutation is present in approximately one third whereas the latter mutation is present in two-thirds of the patients with this condition. We previously reported an inbred transgenic mouse model with the Fgfr2 +/S252W mutation on the C57BL/6J background for Apert syndrome. Here we present a mouse model for the Fgfr2+/P253R mutation. RESULTS: We generated inbred Fgfr2(+/P253R )mice on the same C56BL/6J genetic background and analyzed their skeletal abnormalities. 3D micro-CT scans of the skulls of the Fgfr2(+/P253R )mice revealed that the skull length was shortened with the length of the anterior cranial base significantly shorter than that of the Fgfr2(+/S252W )mice at P0. The Fgfr2(+/P253R )mice presented with synostosis of the coronal suture and proximate fronts with disorganized cellularity in sagittal and lambdoid sutures. Abnormal osteogenesis and proliferation were observed at the developing coronal suture and long bones of the Fgfr2(+/P253R )mice as in the Fgfr2(+/S252W )mice. Activation of mitogen-activated protein kinases (MAPK) was observed in the Fgfr2(+/P253R )neurocranium with an increase in phosphorylated p38 as well as ERK1/2, whereas phosphorylated AKT and PKCα were not obviously changed as compared to those of wild-type controls. There were localized phenotypic and molecular variations among individual embryos with different mutations and among those with the same mutation. CONCLUSIONS: Our in vivo studies demonstrated that the Fgfr2 +/P253R mutation resulted in mice with cranial features that resemble those of the Fgfr2(+/S252W )mice and human Apert syndrome. Activated p38 in addition to the ERK1/2 signaling pathways may mediate the mutant neurocranial phenotype. Though Apert syndrome is traditionally thought to be a consistent phenotype, our results suggest localized and regional variations in the phenotypes that characterize Apert syndrome. BioMed Central 2010-02-22 /pmc/articles/PMC2838826/ /pubmed/20175913 http://dx.doi.org/10.1186/1471-213X-10-22 Text en Copyright ©2010 Wang 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
Wang, Yingli
Sun, Miao
Uhlhorn, Victoria L
Zhou, Xueyan
Peter, Inga
Martinez-Abadias, Neus
Hill, Cheryl A
Percival, Christopher J
Richtsmeier, Joan T
Huso, David L
Jabs, Ethylin Wang
Activation of p38 MAPK pathway in the skull abnormalities of Apert syndrome Fgfr2(+P253R )mice
title Activation of p38 MAPK pathway in the skull abnormalities of Apert syndrome Fgfr2(+P253R )mice
title_full Activation of p38 MAPK pathway in the skull abnormalities of Apert syndrome Fgfr2(+P253R )mice
title_fullStr Activation of p38 MAPK pathway in the skull abnormalities of Apert syndrome Fgfr2(+P253R )mice
title_full_unstemmed Activation of p38 MAPK pathway in the skull abnormalities of Apert syndrome Fgfr2(+P253R )mice
title_short Activation of p38 MAPK pathway in the skull abnormalities of Apert syndrome Fgfr2(+P253R )mice
title_sort activation of p38 mapk pathway in the skull abnormalities of apert syndrome fgfr2(+p253r )mice
topic Research article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2838826/
https://www.ncbi.nlm.nih.gov/pubmed/20175913
http://dx.doi.org/10.1186/1471-213X-10-22
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