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Repair of critical sized cranial defects with BMP9-transduced calvarial cells delivered in a thermoresponsive scaffold

Large skeletal defects caused by trauma, congenital malformations, and post-oncologic resections of the calvarium present major challenges to the reconstructive surgeon. We previously identified BMP-9 as the most osteogenic BMP in vitro and in vivo. Here we sought to investigate the bone regenerativ...

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Autores principales: Dumanian, Zari P., Tollemar, Viktor, Ye, Jixing, Lu, Minpeng, Zhu, Yunxiao, Liao, Junyi, Ameer, Guillermo A., He, Tong-Chuan, Reid, Russell R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5332017/
https://www.ncbi.nlm.nih.gov/pubmed/28249039
http://dx.doi.org/10.1371/journal.pone.0172327
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author Dumanian, Zari P.
Tollemar, Viktor
Ye, Jixing
Lu, Minpeng
Zhu, Yunxiao
Liao, Junyi
Ameer, Guillermo A.
He, Tong-Chuan
Reid, Russell R.
author_facet Dumanian, Zari P.
Tollemar, Viktor
Ye, Jixing
Lu, Minpeng
Zhu, Yunxiao
Liao, Junyi
Ameer, Guillermo A.
He, Tong-Chuan
Reid, Russell R.
author_sort Dumanian, Zari P.
collection PubMed
description Large skeletal defects caused by trauma, congenital malformations, and post-oncologic resections of the calvarium present major challenges to the reconstructive surgeon. We previously identified BMP-9 as the most osteogenic BMP in vitro and in vivo. Here we sought to investigate the bone regenerative capacity of murine-derived calvarial mesenchymal progenitor cells (iCALs) transduced by BMP-9 in the context of healing critical-sized calvarial defects. To accomplish this, the transduced cells were delivered to the defect site within a thermoresponsive biodegradable scaffold consisting of poly(polyethylene glycol citrate-co-N-isopropylacrylamide mixed with gelatin (PPCN-g). A total of three treatment arms were evaluated: PPCN-g alone, PPCN-g seeded with iCALs expressing GFP, and PPCN-g seeded with iCALs expressing BMP-9. Defects treated only with PPCN-g scaffold did not statistically change in size when evaluated at eight weeks postoperatively (p = 0.72). Conversely, both animal groups treated with iCALs showed significant reductions in defect size after 12 weeks of follow-up (BMP9-treated: p = 0.0025; GFP-treated: p = 0.0042). However, H&E and trichrome staining revealed more complete osseointegration and mature bone formation only in the BMP9-treated group. These results suggest that BMP9-transduced iCALs seeded in a PPCN-g thermoresponsive scaffold is capable of inducing bone formation in vivo and is an effective means of creating tissue engineered bone for critical sized defects.
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spelling pubmed-53320172017-03-10 Repair of critical sized cranial defects with BMP9-transduced calvarial cells delivered in a thermoresponsive scaffold Dumanian, Zari P. Tollemar, Viktor Ye, Jixing Lu, Minpeng Zhu, Yunxiao Liao, Junyi Ameer, Guillermo A. He, Tong-Chuan Reid, Russell R. PLoS One Research Article Large skeletal defects caused by trauma, congenital malformations, and post-oncologic resections of the calvarium present major challenges to the reconstructive surgeon. We previously identified BMP-9 as the most osteogenic BMP in vitro and in vivo. Here we sought to investigate the bone regenerative capacity of murine-derived calvarial mesenchymal progenitor cells (iCALs) transduced by BMP-9 in the context of healing critical-sized calvarial defects. To accomplish this, the transduced cells were delivered to the defect site within a thermoresponsive biodegradable scaffold consisting of poly(polyethylene glycol citrate-co-N-isopropylacrylamide mixed with gelatin (PPCN-g). A total of three treatment arms were evaluated: PPCN-g alone, PPCN-g seeded with iCALs expressing GFP, and PPCN-g seeded with iCALs expressing BMP-9. Defects treated only with PPCN-g scaffold did not statistically change in size when evaluated at eight weeks postoperatively (p = 0.72). Conversely, both animal groups treated with iCALs showed significant reductions in defect size after 12 weeks of follow-up (BMP9-treated: p = 0.0025; GFP-treated: p = 0.0042). However, H&E and trichrome staining revealed more complete osseointegration and mature bone formation only in the BMP9-treated group. These results suggest that BMP9-transduced iCALs seeded in a PPCN-g thermoresponsive scaffold is capable of inducing bone formation in vivo and is an effective means of creating tissue engineered bone for critical sized defects. Public Library of Science 2017-03-01 /pmc/articles/PMC5332017/ /pubmed/28249039 http://dx.doi.org/10.1371/journal.pone.0172327 Text en © 2017 Dumanian 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 (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Dumanian, Zari P.
Tollemar, Viktor
Ye, Jixing
Lu, Minpeng
Zhu, Yunxiao
Liao, Junyi
Ameer, Guillermo A.
He, Tong-Chuan
Reid, Russell R.
Repair of critical sized cranial defects with BMP9-transduced calvarial cells delivered in a thermoresponsive scaffold
title Repair of critical sized cranial defects with BMP9-transduced calvarial cells delivered in a thermoresponsive scaffold
title_full Repair of critical sized cranial defects with BMP9-transduced calvarial cells delivered in a thermoresponsive scaffold
title_fullStr Repair of critical sized cranial defects with BMP9-transduced calvarial cells delivered in a thermoresponsive scaffold
title_full_unstemmed Repair of critical sized cranial defects with BMP9-transduced calvarial cells delivered in a thermoresponsive scaffold
title_short Repair of critical sized cranial defects with BMP9-transduced calvarial cells delivered in a thermoresponsive scaffold
title_sort repair of critical sized cranial defects with bmp9-transduced calvarial cells delivered in a thermoresponsive scaffold
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5332017/
https://www.ncbi.nlm.nih.gov/pubmed/28249039
http://dx.doi.org/10.1371/journal.pone.0172327
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