Hyaluronic acid-recombinant gelatin gels as a scaffold for soft tissue regeneration

An array of different types of hyaluronic acid (HA)- and collagen-based products is available for filling soft-tissue defects. A major drawback of the current soft-tissue fillers is their inability to induce cell infiltration and new tissue formation. Our aim is to develop novel biodegradable inject...

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Main Authors: A Tuin, J Zandstra, SG Kluijtmans, JB Bouwstra, MC Harmsen, MJA Van Luyn
Format: Article
Language:English
Published: AO Research Institute Davos 2012-10-01
Series:European Cells & Materials
Subjects:
Online Access:http://www.ecmjournal.org/journal/papers/vol024/pdf/v024a23.pdf
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spelling doaj-9c2ea5826e784aacb1447c8e2cb61c342020-11-24T23:28:45Zeng AO Research Institute DavosEuropean Cells & Materials1473-22622012-10-0124320330Hyaluronic acid-recombinant gelatin gels as a scaffold for soft tissue regenerationA TuinJ ZandstraSG KluijtmansJB BouwstraMC HarmsenMJA Van LuynAn array of different types of hyaluronic acid (HA)- and collagen-based products is available for filling soft-tissue defects. A major drawback of the current soft-tissue fillers is their inability to induce cell infiltration and new tissue formation. Our aim is to develop novel biodegradable injectable gels which induce soft tissue regeneration, initially resulting in integration and finally replacement of the gel with new autologous tissue. Two reference gels of pure HA, monophasic HA-1 and micronised HA-2, were used. Furthermore, both gels were mixed with recombinant gelatin (RG) resulting in HA-1+RG and HA-2+RG. All gels were subcutaneously injected on the back of rats and explanted after 4 weeks. Addition of RG to HA-1 resulted in stroma formation (neovascularisation and ECM deposition) which was restricted to the outer rim of the HA-1+RG gel. In contrast, addition of RG to HA-2 induced stroma formation throughout the gel. The RG component of the gel was degraded by macrophages and giant cells and subsequently replaced by new vascularised tissue. Immunohistochemical staining showed that the extracellular matrix components collagen I and III were deposited throughout the gel. In conclusion, this study shows the proof of principle that addition of RG to HA-2 results in a novel injectable gel capable of inducing soft tissue regeneration. In this gel HA has a scaffold function whereas the RG component induces new tissue formation, resulting in proper vascularisation and integration of the HA-2+RG gel with the autologous tissue.http://www.ecmjournal.org/journal/papers/vol024/pdf/v024a23.pdfTissue regenerationhydrogelscaffoldhyaluronic acidrecombinant gelatin
collection DOAJ
language English
format Article
sources DOAJ
author A Tuin
J Zandstra
SG Kluijtmans
JB Bouwstra
MC Harmsen
MJA Van Luyn
spellingShingle A Tuin
J Zandstra
SG Kluijtmans
JB Bouwstra
MC Harmsen
MJA Van Luyn
Hyaluronic acid-recombinant gelatin gels as a scaffold for soft tissue regeneration
European Cells & Materials
Tissue regeneration
hydrogel
scaffold
hyaluronic acid
recombinant gelatin
author_facet A Tuin
J Zandstra
SG Kluijtmans
JB Bouwstra
MC Harmsen
MJA Van Luyn
author_sort A Tuin
title Hyaluronic acid-recombinant gelatin gels as a scaffold for soft tissue regeneration
title_short Hyaluronic acid-recombinant gelatin gels as a scaffold for soft tissue regeneration
title_full Hyaluronic acid-recombinant gelatin gels as a scaffold for soft tissue regeneration
title_fullStr Hyaluronic acid-recombinant gelatin gels as a scaffold for soft tissue regeneration
title_full_unstemmed Hyaluronic acid-recombinant gelatin gels as a scaffold for soft tissue regeneration
title_sort hyaluronic acid-recombinant gelatin gels as a scaffold for soft tissue regeneration
publisher AO Research Institute Davos
series European Cells & Materials
issn 1473-2262
publishDate 2012-10-01
description An array of different types of hyaluronic acid (HA)- and collagen-based products is available for filling soft-tissue defects. A major drawback of the current soft-tissue fillers is their inability to induce cell infiltration and new tissue formation. Our aim is to develop novel biodegradable injectable gels which induce soft tissue regeneration, initially resulting in integration and finally replacement of the gel with new autologous tissue. Two reference gels of pure HA, monophasic HA-1 and micronised HA-2, were used. Furthermore, both gels were mixed with recombinant gelatin (RG) resulting in HA-1+RG and HA-2+RG. All gels were subcutaneously injected on the back of rats and explanted after 4 weeks. Addition of RG to HA-1 resulted in stroma formation (neovascularisation and ECM deposition) which was restricted to the outer rim of the HA-1+RG gel. In contrast, addition of RG to HA-2 induced stroma formation throughout the gel. The RG component of the gel was degraded by macrophages and giant cells and subsequently replaced by new vascularised tissue. Immunohistochemical staining showed that the extracellular matrix components collagen I and III were deposited throughout the gel. In conclusion, this study shows the proof of principle that addition of RG to HA-2 results in a novel injectable gel capable of inducing soft tissue regeneration. In this gel HA has a scaffold function whereas the RG component induces new tissue formation, resulting in proper vascularisation and integration of the HA-2+RG gel with the autologous tissue.
topic Tissue regeneration
hydrogel
scaffold
hyaluronic acid
recombinant gelatin
url http://www.ecmjournal.org/journal/papers/vol024/pdf/v024a23.pdf
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