Autologous serum improves bone formation in a primary stable silica-embedded nanohydroxyapatite bone substitute in combination with mesenchymal stem cells and rhBMP-2 in the sheep model

New therapeutic strategies are required for critical size bone defects, because the gold standard of transplanting autologous bone from an unharmed area of the body often leads to several severe side effects and disadvantages for the patient. For years, tissue engineering approaches have been seekin...

Descripción completa

Detalles Bibliográficos
Autores principales: Boos, Anja M, Weigand, Annika, Deschler, Gloria, Gerber, Thomas, Arkudas, Andreas, Kneser, Ulrich, Horch, Raymund E, Beier, Justus P
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Dove Medical Press 2014
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4242408/
https://www.ncbi.nlm.nih.gov/pubmed/25429218
http://dx.doi.org/10.2147/IJN.S66867
_version_ 1782345947415576576
author Boos, Anja M
Weigand, Annika
Deschler, Gloria
Gerber, Thomas
Arkudas, Andreas
Kneser, Ulrich
Horch, Raymund E
Beier, Justus P
author_facet Boos, Anja M
Weigand, Annika
Deschler, Gloria
Gerber, Thomas
Arkudas, Andreas
Kneser, Ulrich
Horch, Raymund E
Beier, Justus P
author_sort Boos, Anja M
collection PubMed
description New therapeutic strategies are required for critical size bone defects, because the gold standard of transplanting autologous bone from an unharmed area of the body often leads to several severe side effects and disadvantages for the patient. For years, tissue engineering approaches have been seeking a stable, axially vascularized transplantable bone replacement suitable for transplantation into the recipient bed with pre-existing insufficient conditions. For this reason, the arteriovenous loop model was developed and various bone substitutes have been vascularized. However, it has not been possible thus far to engineer a primary stable and axially vascularized transplantable bone substitute. For that purpose, a primary stable silica-embedded nanohydroxyapatite (HA) bone substitute in combination with blood, bone marrow, expanded, or directly retransplanted mesenchymal stem cells, recombinant human bone morphogenetic protein 2 (rhBMP-2), and different carrier materials (fibrin, cell culture medium, autologous serum) was tested subcutaneously for 4 or 12 weeks in the sheep model. Autologous serum lead to an early matrix change during degradation of the bone substitute and formation of new bone tissue. The best results were achieved in the group combining mesenchymal stem cells expanded with 60 μg/mL rhBMP-2 in autologous serum. Better ingrowth of fibrovascular tissue could be detected in the autologous serum group compared with the control (fibrin). Osteoclastic activity indicating an active bone remodeling process was observed after 4 weeks, particularly in the group with autologous serum and after 12 weeks in every experimental group. This study clearly demonstrates the positive effects of autologous serum in combination with mesenchymal stem cells and rhBMP-2 on bone formation in a primary stable silica-embedded nano-HA bone grafting material in the sheep model. In further experiments, the results will be transferred to the sheep arteriovenous loop model in order to engineer an axially vascularized primary stable bone replacement in clinically relevant size for free transplantation.
format Online
Article
Text
id pubmed-4242408
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher Dove Medical Press
record_format MEDLINE/PubMed
spelling pubmed-42424082014-11-26 Autologous serum improves bone formation in a primary stable silica-embedded nanohydroxyapatite bone substitute in combination with mesenchymal stem cells and rhBMP-2 in the sheep model Boos, Anja M Weigand, Annika Deschler, Gloria Gerber, Thomas Arkudas, Andreas Kneser, Ulrich Horch, Raymund E Beier, Justus P Int J Nanomedicine Original Research New therapeutic strategies are required for critical size bone defects, because the gold standard of transplanting autologous bone from an unharmed area of the body often leads to several severe side effects and disadvantages for the patient. For years, tissue engineering approaches have been seeking a stable, axially vascularized transplantable bone replacement suitable for transplantation into the recipient bed with pre-existing insufficient conditions. For this reason, the arteriovenous loop model was developed and various bone substitutes have been vascularized. However, it has not been possible thus far to engineer a primary stable and axially vascularized transplantable bone substitute. For that purpose, a primary stable silica-embedded nanohydroxyapatite (HA) bone substitute in combination with blood, bone marrow, expanded, or directly retransplanted mesenchymal stem cells, recombinant human bone morphogenetic protein 2 (rhBMP-2), and different carrier materials (fibrin, cell culture medium, autologous serum) was tested subcutaneously for 4 or 12 weeks in the sheep model. Autologous serum lead to an early matrix change during degradation of the bone substitute and formation of new bone tissue. The best results were achieved in the group combining mesenchymal stem cells expanded with 60 μg/mL rhBMP-2 in autologous serum. Better ingrowth of fibrovascular tissue could be detected in the autologous serum group compared with the control (fibrin). Osteoclastic activity indicating an active bone remodeling process was observed after 4 weeks, particularly in the group with autologous serum and after 12 weeks in every experimental group. This study clearly demonstrates the positive effects of autologous serum in combination with mesenchymal stem cells and rhBMP-2 on bone formation in a primary stable silica-embedded nano-HA bone grafting material in the sheep model. In further experiments, the results will be transferred to the sheep arteriovenous loop model in order to engineer an axially vascularized primary stable bone replacement in clinically relevant size for free transplantation. Dove Medical Press 2014-11-19 /pmc/articles/PMC4242408/ /pubmed/25429218 http://dx.doi.org/10.2147/IJN.S66867 Text en © 2014 Boos et al. This work is published by Dove Medical Press Limited, and licensed under Creative Commons Attribution – Non Commercial (unported, v3.0) License The full terms of the License are available at http://creativecommons.org/licenses/by-nc/3.0/. Non-commercial uses of the work are permitted without any further permission from Dove Medical Press Limited, provided the work is properly attributed.
spellingShingle Original Research
Boos, Anja M
Weigand, Annika
Deschler, Gloria
Gerber, Thomas
Arkudas, Andreas
Kneser, Ulrich
Horch, Raymund E
Beier, Justus P
Autologous serum improves bone formation in a primary stable silica-embedded nanohydroxyapatite bone substitute in combination with mesenchymal stem cells and rhBMP-2 in the sheep model
title Autologous serum improves bone formation in a primary stable silica-embedded nanohydroxyapatite bone substitute in combination with mesenchymal stem cells and rhBMP-2 in the sheep model
title_full Autologous serum improves bone formation in a primary stable silica-embedded nanohydroxyapatite bone substitute in combination with mesenchymal stem cells and rhBMP-2 in the sheep model
title_fullStr Autologous serum improves bone formation in a primary stable silica-embedded nanohydroxyapatite bone substitute in combination with mesenchymal stem cells and rhBMP-2 in the sheep model
title_full_unstemmed Autologous serum improves bone formation in a primary stable silica-embedded nanohydroxyapatite bone substitute in combination with mesenchymal stem cells and rhBMP-2 in the sheep model
title_short Autologous serum improves bone formation in a primary stable silica-embedded nanohydroxyapatite bone substitute in combination with mesenchymal stem cells and rhBMP-2 in the sheep model
title_sort autologous serum improves bone formation in a primary stable silica-embedded nanohydroxyapatite bone substitute in combination with mesenchymal stem cells and rhbmp-2 in the sheep model
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4242408/
https://www.ncbi.nlm.nih.gov/pubmed/25429218
http://dx.doi.org/10.2147/IJN.S66867
work_keys_str_mv AT boosanjam autologousserumimprovesboneformationinaprimarystablesilicaembeddednanohydroxyapatitebonesubstituteincombinationwithmesenchymalstemcellsandrhbmp2inthesheepmodel
AT weigandannika autologousserumimprovesboneformationinaprimarystablesilicaembeddednanohydroxyapatitebonesubstituteincombinationwithmesenchymalstemcellsandrhbmp2inthesheepmodel
AT deschlergloria autologousserumimprovesboneformationinaprimarystablesilicaembeddednanohydroxyapatitebonesubstituteincombinationwithmesenchymalstemcellsandrhbmp2inthesheepmodel
AT gerberthomas autologousserumimprovesboneformationinaprimarystablesilicaembeddednanohydroxyapatitebonesubstituteincombinationwithmesenchymalstemcellsandrhbmp2inthesheepmodel
AT arkudasandreas autologousserumimprovesboneformationinaprimarystablesilicaembeddednanohydroxyapatitebonesubstituteincombinationwithmesenchymalstemcellsandrhbmp2inthesheepmodel
AT kneserulrich autologousserumimprovesboneformationinaprimarystablesilicaembeddednanohydroxyapatitebonesubstituteincombinationwithmesenchymalstemcellsandrhbmp2inthesheepmodel
AT horchraymunde autologousserumimprovesboneformationinaprimarystablesilicaembeddednanohydroxyapatitebonesubstituteincombinationwithmesenchymalstemcellsandrhbmp2inthesheepmodel
AT beierjustusp autologousserumimprovesboneformationinaprimarystablesilicaembeddednanohydroxyapatitebonesubstituteincombinationwithmesenchymalstemcellsandrhbmp2inthesheepmodel

Ejemplares similares