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TGF-β signaling and Creb5 cooperatively regulate Fgf18 to control pharyngeal muscle development

The communication between myogenic cells and their surrounding connective tissues is indispensable for muscle morphogenesis. During late embryonic development in mice, myogenic progenitors migrate to discrete sites to form individual muscles. The detailed mechanism of this process remains unclear. U...

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Autores principales: Feng, Jifan, Han, Xia, Yuan, Yuan, Cho, Courtney Kyeong, Janečková, Eva, Guo, Tingwei, Pareek, Siddhika, Rahman, Md Shaifur, Zheng, Banghong, Bi, Jing, Jing, Junjun, Zhang, Mingyi, Xu, Jian, Ho, Thach-Vu, Chai, Yang
Formato: Online Artículo Texto
Lenguaje:English
Publicado: eLife Sciences Publications, Ltd 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9771365/
https://www.ncbi.nlm.nih.gov/pubmed/36542062
http://dx.doi.org/10.7554/eLife.80405
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author Feng, Jifan
Han, Xia
Yuan, Yuan
Cho, Courtney Kyeong
Janečková, Eva
Guo, Tingwei
Pareek, Siddhika
Rahman, Md Shaifur
Zheng, Banghong
Bi, Jing
Jing, Junjun
Zhang, Mingyi
Xu, Jian
Ho, Thach-Vu
Chai, Yang
author_facet Feng, Jifan
Han, Xia
Yuan, Yuan
Cho, Courtney Kyeong
Janečková, Eva
Guo, Tingwei
Pareek, Siddhika
Rahman, Md Shaifur
Zheng, Banghong
Bi, Jing
Jing, Junjun
Zhang, Mingyi
Xu, Jian
Ho, Thach-Vu
Chai, Yang
author_sort Feng, Jifan
collection PubMed
description The communication between myogenic cells and their surrounding connective tissues is indispensable for muscle morphogenesis. During late embryonic development in mice, myogenic progenitors migrate to discrete sites to form individual muscles. The detailed mechanism of this process remains unclear. Using mouse levator veli palatini (LVP) development as a model, we systematically investigated how a distinct connective tissue subpopulation, perimysial fibroblasts, communicates with myogenic cells to regulate mouse pharyngeal myogenesis. Using single-cell RNAseq data analysis, we identified that TGF-β signaling is a key regulator for the perimysial fibroblasts. Loss of TGF-β signaling in the neural crest-derived palatal mesenchyme leads to defects in perimysial fibroblasts and muscle malformation in the soft palate in Osr2(Cre);Tgfbr1(fl/fl) mice. In particular, Creb5, a transcription factor expressed in the perimysial fibroblasts, cooperates with TGF-β signaling to activate expression of Fgf18. Moreover, Fgf18 supports pharyngeal muscle development in vivo and exogenous Fgf18 can partially rescue myogenic cell numbers in Osr2(Cre);Tgfbr1(fl/fl) samples, illustrating that TGF-β-regulated Fgf18 signaling is required for LVP development. Collectively, our findings reveal the mechanism by which TGF-β signaling achieves its functional specificity in defining the perimysial-to-myogenic signals for pharyngeal myogenesis.
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spelling pubmed-97713652022-12-22 TGF-β signaling and Creb5 cooperatively regulate Fgf18 to control pharyngeal muscle development Feng, Jifan Han, Xia Yuan, Yuan Cho, Courtney Kyeong Janečková, Eva Guo, Tingwei Pareek, Siddhika Rahman, Md Shaifur Zheng, Banghong Bi, Jing Jing, Junjun Zhang, Mingyi Xu, Jian Ho, Thach-Vu Chai, Yang eLife Developmental Biology The communication between myogenic cells and their surrounding connective tissues is indispensable for muscle morphogenesis. During late embryonic development in mice, myogenic progenitors migrate to discrete sites to form individual muscles. The detailed mechanism of this process remains unclear. Using mouse levator veli palatini (LVP) development as a model, we systematically investigated how a distinct connective tissue subpopulation, perimysial fibroblasts, communicates with myogenic cells to regulate mouse pharyngeal myogenesis. Using single-cell RNAseq data analysis, we identified that TGF-β signaling is a key regulator for the perimysial fibroblasts. Loss of TGF-β signaling in the neural crest-derived palatal mesenchyme leads to defects in perimysial fibroblasts and muscle malformation in the soft palate in Osr2(Cre);Tgfbr1(fl/fl) mice. In particular, Creb5, a transcription factor expressed in the perimysial fibroblasts, cooperates with TGF-β signaling to activate expression of Fgf18. Moreover, Fgf18 supports pharyngeal muscle development in vivo and exogenous Fgf18 can partially rescue myogenic cell numbers in Osr2(Cre);Tgfbr1(fl/fl) samples, illustrating that TGF-β-regulated Fgf18 signaling is required for LVP development. Collectively, our findings reveal the mechanism by which TGF-β signaling achieves its functional specificity in defining the perimysial-to-myogenic signals for pharyngeal myogenesis. eLife Sciences Publications, Ltd 2022-12-21 /pmc/articles/PMC9771365/ /pubmed/36542062 http://dx.doi.org/10.7554/eLife.80405 Text en © 2022, Feng et al https://creativecommons.org/licenses/by/4.0/This article is distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use and redistribution provided that the original author and source are credited.
spellingShingle Developmental Biology
Feng, Jifan
Han, Xia
Yuan, Yuan
Cho, Courtney Kyeong
Janečková, Eva
Guo, Tingwei
Pareek, Siddhika
Rahman, Md Shaifur
Zheng, Banghong
Bi, Jing
Jing, Junjun
Zhang, Mingyi
Xu, Jian
Ho, Thach-Vu
Chai, Yang
TGF-β signaling and Creb5 cooperatively regulate Fgf18 to control pharyngeal muscle development
title TGF-β signaling and Creb5 cooperatively regulate Fgf18 to control pharyngeal muscle development
title_full TGF-β signaling and Creb5 cooperatively regulate Fgf18 to control pharyngeal muscle development
title_fullStr TGF-β signaling and Creb5 cooperatively regulate Fgf18 to control pharyngeal muscle development
title_full_unstemmed TGF-β signaling and Creb5 cooperatively regulate Fgf18 to control pharyngeal muscle development
title_short TGF-β signaling and Creb5 cooperatively regulate Fgf18 to control pharyngeal muscle development
title_sort tgf-β signaling and creb5 cooperatively regulate fgf18 to control pharyngeal muscle development
topic Developmental Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9771365/
https://www.ncbi.nlm.nih.gov/pubmed/36542062
http://dx.doi.org/10.7554/eLife.80405
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