CDC42 is required for epicardial and pro-epicardial development by mediating FGF receptor trafficking to the plasma membrane

The epicardium contributes to multiple cardiac lineages and is essential for cardiac development and regeneration. However, the mechanism of epicardium formation is unclear. This study aimed to establish the cellular and molecular mechanisms underlying the dissociation of pro-epicardial cells (PECs)...

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Autores principales: Li, Jingjing, Miao, Lianjie, Zhao, Chen, Shaikh Qureshi, Wasay Mohiuddin, Shieh, David, Guo, Hua, Lu, Yangyang, Hu, Saiyang, Huang, Alice, Zhang, Lu, Cai, Chen-leng, Wan, Leo Q., Xin, Hongbo, Vincent, Peter, Singer, Harold A., Zheng, Yi, Cleaver, Ondine, Fan, Zhen-Chuan, Wu, Mingfu
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Company of Biologists Ltd 2017
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5450847/
https://www.ncbi.nlm.nih.gov/pubmed/28465335
http://dx.doi.org/10.1242/dev.147173
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author Li, Jingjing
Miao, Lianjie
Zhao, Chen
Shaikh Qureshi, Wasay Mohiuddin
Shieh, David
Guo, Hua
Lu, Yangyang
Hu, Saiyang
Huang, Alice
Zhang, Lu
Cai, Chen-leng
Wan, Leo Q.
Xin, Hongbo
Vincent, Peter
Singer, Harold A.
Zheng, Yi
Cleaver, Ondine
Fan, Zhen-Chuan
Wu, Mingfu
author_facet Li, Jingjing
Miao, Lianjie
Zhao, Chen
Shaikh Qureshi, Wasay Mohiuddin
Shieh, David
Guo, Hua
Lu, Yangyang
Hu, Saiyang
Huang, Alice
Zhang, Lu
Cai, Chen-leng
Wan, Leo Q.
Xin, Hongbo
Vincent, Peter
Singer, Harold A.
Zheng, Yi
Cleaver, Ondine
Fan, Zhen-Chuan
Wu, Mingfu
author_sort Li, Jingjing
collection PubMed
description The epicardium contributes to multiple cardiac lineages and is essential for cardiac development and regeneration. However, the mechanism of epicardium formation is unclear. This study aimed to establish the cellular and molecular mechanisms underlying the dissociation of pro-epicardial cells (PECs) from the pro-epicardium (PE) and their subsequent translocation to the heart to form the epicardium. We used lineage tracing, conditional deletion, mosaic analysis and ligand stimulation in mice to determine that both villous protrusions and floating cysts contribute to PEC translocation to myocardium in a CDC42-dependent manner. We resolved a controversy by demonstrating that physical contact of the PE with the myocardium constitutes a third mechanism for PEC translocation to myocardium, and observed a fourth mechanism in which PECs migrate along the surface of the inflow tract to reach the ventricles. Epicardial-specific Cdc42 deletion disrupted epicardium formation, and Cdc42 null PECs proliferated less, lost polarity and failed to form villous protrusions and floating cysts. FGF signaling promotes epicardium formation in vivo, and biochemical studies demonstrated that CDC42 is involved in the trafficking of FGF receptors to the cell membrane to regulate epicardium formation.
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spelling pubmed-54508472017-06-19 CDC42 is required for epicardial and pro-epicardial development by mediating FGF receptor trafficking to the plasma membrane Li, Jingjing Miao, Lianjie Zhao, Chen Shaikh Qureshi, Wasay Mohiuddin Shieh, David Guo, Hua Lu, Yangyang Hu, Saiyang Huang, Alice Zhang, Lu Cai, Chen-leng Wan, Leo Q. Xin, Hongbo Vincent, Peter Singer, Harold A. Zheng, Yi Cleaver, Ondine Fan, Zhen-Chuan Wu, Mingfu Development Research Article The epicardium contributes to multiple cardiac lineages and is essential for cardiac development and regeneration. However, the mechanism of epicardium formation is unclear. This study aimed to establish the cellular and molecular mechanisms underlying the dissociation of pro-epicardial cells (PECs) from the pro-epicardium (PE) and their subsequent translocation to the heart to form the epicardium. We used lineage tracing, conditional deletion, mosaic analysis and ligand stimulation in mice to determine that both villous protrusions and floating cysts contribute to PEC translocation to myocardium in a CDC42-dependent manner. We resolved a controversy by demonstrating that physical contact of the PE with the myocardium constitutes a third mechanism for PEC translocation to myocardium, and observed a fourth mechanism in which PECs migrate along the surface of the inflow tract to reach the ventricles. Epicardial-specific Cdc42 deletion disrupted epicardium formation, and Cdc42 null PECs proliferated less, lost polarity and failed to form villous protrusions and floating cysts. FGF signaling promotes epicardium formation in vivo, and biochemical studies demonstrated that CDC42 is involved in the trafficking of FGF receptors to the cell membrane to regulate epicardium formation. The Company of Biologists Ltd 2017-05-01 /pmc/articles/PMC5450847/ /pubmed/28465335 http://dx.doi.org/10.1242/dev.147173 Text en © 2017. Published by The Company of Biologists Ltd http://creativecommons.org/licenses/by/3.0This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/3.0), which permits unrestricted use, distribution and reproduction in any medium provided that the original work is properly attributed.
spellingShingle Research Article
Li, Jingjing
Miao, Lianjie
Zhao, Chen
Shaikh Qureshi, Wasay Mohiuddin
Shieh, David
Guo, Hua
Lu, Yangyang
Hu, Saiyang
Huang, Alice
Zhang, Lu
Cai, Chen-leng
Wan, Leo Q.
Xin, Hongbo
Vincent, Peter
Singer, Harold A.
Zheng, Yi
Cleaver, Ondine
Fan, Zhen-Chuan
Wu, Mingfu
CDC42 is required for epicardial and pro-epicardial development by mediating FGF receptor trafficking to the plasma membrane
title CDC42 is required for epicardial and pro-epicardial development by mediating FGF receptor trafficking to the plasma membrane
title_full CDC42 is required for epicardial and pro-epicardial development by mediating FGF receptor trafficking to the plasma membrane
title_fullStr CDC42 is required for epicardial and pro-epicardial development by mediating FGF receptor trafficking to the plasma membrane
title_full_unstemmed CDC42 is required for epicardial and pro-epicardial development by mediating FGF receptor trafficking to the plasma membrane
title_short CDC42 is required for epicardial and pro-epicardial development by mediating FGF receptor trafficking to the plasma membrane
title_sort cdc42 is required for epicardial and pro-epicardial development by mediating fgf receptor trafficking to the plasma membrane
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5450847/
https://www.ncbi.nlm.nih.gov/pubmed/28465335
http://dx.doi.org/10.1242/dev.147173
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