TGFβ1-Induced Baf60c Regulates both Smooth Muscle Cell Commitment and Quiescence

Smooth muscle cells (SMCs) play critical roles in a number of diseases; however, the molecular mechanism underlying their development is unclear. Although the role of TGFβ1 signaling in SMC development is well established, the downstream molecular signals are not fully understood. We used several ra...

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Autores principales: Sohni, Abhishek, Mulas, Francesca, Ferrazzi, Fulvia, Luttun, Aernout, Bellazzi, Riccardo, Huylebroeck, Danny, Ekker, Stephen C., Verfaillie, Catherine M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3482188/
https://www.ncbi.nlm.nih.gov/pubmed/23110084
http://dx.doi.org/10.1371/journal.pone.0047629
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author Sohni, Abhishek
Mulas, Francesca
Ferrazzi, Fulvia
Luttun, Aernout
Bellazzi, Riccardo
Huylebroeck, Danny
Ekker, Stephen C.
Verfaillie, Catherine M.
author_facet Sohni, Abhishek
Mulas, Francesca
Ferrazzi, Fulvia
Luttun, Aernout
Bellazzi, Riccardo
Huylebroeck, Danny
Ekker, Stephen C.
Verfaillie, Catherine M.
author_sort Sohni, Abhishek
collection PubMed
description Smooth muscle cells (SMCs) play critical roles in a number of diseases; however, the molecular mechanism underlying their development is unclear. Although the role of TGFβ1 signaling in SMC development is well established, the downstream molecular signals are not fully understood. We used several rat multipotent adult progenitor cell ((r)MAPC) lines that express levels of Oct4 mRNA similar to hypoblast stem cells (HypoSC), and can differentiate robustly to mesodermal and endodermal cell types. TGFβ1 alone, or with PDGF-BB, induces differentiation of rMAPCs to SMCs, which expressed structural SMC proteins, including α-smooth muscle actin (αSMA), and contribute to the SMC coat of blood vessels in vivo. A genome-wide time-course transcriptome analysis revealed that transcripts of Baf60c, part of the SWI/SNF actin binding chromatin remodeling complex D-3 (SMARCD3/BAF60c), were significantly induced during MAPC-SMC differentiation. We demonstrated that BAF60c is a necessary co-regulator of TGFβ1 mediated induction of SMC genes. Knock-down of Baf60c decreased SMC gene expression in rMAPCs whereas ectopic expression of Baf60c was sufficient to commit rMAPCs to SMCs in the absence of exogenous cytokines. TGFβ1 activates Baf60c via the direct binding of SMAD2/3 complexes to the Baf60c promoter region. Chromatin- and co-immunoprecipitation studies demonstrated that regulation of SMC genes by BAF60c is mediated via interaction with SRF binding CArG box-containing promoter elements in SMC genes. We noted that compared with TGFβ1, Baf60c overexpression in rMAPC yielded SMC with a more immature phenotype. Similarly, Baf60c induced an immature phenotype in rat aortic SMCs marked by increased cell proliferation and decreased contractile marker expression. Thus, Baf60c is important for TGFβ-mediated commitment of primitive stem cells (rMAPCs) to SMCs and is associated with induction of a proliferative state of quiescent SMCs. The MAPC-SMC differentiation system may be useful for identification of additional critical (co-)regulators of SMC development.
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spelling pubmed-34821882012-10-29 TGFβ1-Induced Baf60c Regulates both Smooth Muscle Cell Commitment and Quiescence Sohni, Abhishek Mulas, Francesca Ferrazzi, Fulvia Luttun, Aernout Bellazzi, Riccardo Huylebroeck, Danny Ekker, Stephen C. Verfaillie, Catherine M. PLoS One Research Article Smooth muscle cells (SMCs) play critical roles in a number of diseases; however, the molecular mechanism underlying their development is unclear. Although the role of TGFβ1 signaling in SMC development is well established, the downstream molecular signals are not fully understood. We used several rat multipotent adult progenitor cell ((r)MAPC) lines that express levels of Oct4 mRNA similar to hypoblast stem cells (HypoSC), and can differentiate robustly to mesodermal and endodermal cell types. TGFβ1 alone, or with PDGF-BB, induces differentiation of rMAPCs to SMCs, which expressed structural SMC proteins, including α-smooth muscle actin (αSMA), and contribute to the SMC coat of blood vessels in vivo. A genome-wide time-course transcriptome analysis revealed that transcripts of Baf60c, part of the SWI/SNF actin binding chromatin remodeling complex D-3 (SMARCD3/BAF60c), were significantly induced during MAPC-SMC differentiation. We demonstrated that BAF60c is a necessary co-regulator of TGFβ1 mediated induction of SMC genes. Knock-down of Baf60c decreased SMC gene expression in rMAPCs whereas ectopic expression of Baf60c was sufficient to commit rMAPCs to SMCs in the absence of exogenous cytokines. TGFβ1 activates Baf60c via the direct binding of SMAD2/3 complexes to the Baf60c promoter region. Chromatin- and co-immunoprecipitation studies demonstrated that regulation of SMC genes by BAF60c is mediated via interaction with SRF binding CArG box-containing promoter elements in SMC genes. We noted that compared with TGFβ1, Baf60c overexpression in rMAPC yielded SMC with a more immature phenotype. Similarly, Baf60c induced an immature phenotype in rat aortic SMCs marked by increased cell proliferation and decreased contractile marker expression. Thus, Baf60c is important for TGFβ-mediated commitment of primitive stem cells (rMAPCs) to SMCs and is associated with induction of a proliferative state of quiescent SMCs. The MAPC-SMC differentiation system may be useful for identification of additional critical (co-)regulators of SMC development. Public Library of Science 2012-10-26 /pmc/articles/PMC3482188/ /pubmed/23110084 http://dx.doi.org/10.1371/journal.pone.0047629 Text en © 2012 Sohni 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
Sohni, Abhishek
Mulas, Francesca
Ferrazzi, Fulvia
Luttun, Aernout
Bellazzi, Riccardo
Huylebroeck, Danny
Ekker, Stephen C.
Verfaillie, Catherine M.
TGFβ1-Induced Baf60c Regulates both Smooth Muscle Cell Commitment and Quiescence
title TGFβ1-Induced Baf60c Regulates both Smooth Muscle Cell Commitment and Quiescence
title_full TGFβ1-Induced Baf60c Regulates both Smooth Muscle Cell Commitment and Quiescence
title_fullStr TGFβ1-Induced Baf60c Regulates both Smooth Muscle Cell Commitment and Quiescence
title_full_unstemmed TGFβ1-Induced Baf60c Regulates both Smooth Muscle Cell Commitment and Quiescence
title_short TGFβ1-Induced Baf60c Regulates both Smooth Muscle Cell Commitment and Quiescence
title_sort tgfβ1-induced baf60c regulates both smooth muscle cell commitment and quiescence
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3482188/
https://www.ncbi.nlm.nih.gov/pubmed/23110084
http://dx.doi.org/10.1371/journal.pone.0047629
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