A Glutaraldehyde-Free Crosslinking Method for the Treatment of Collagen-Based Biomaterials for Clinical Application

Biological bioprostheses such as grafts, patches, and heart valves are often derived from biological tissue like the pericardium. These bioprostheses can be of xenogenic, allogeneic, or autologous origin. Irrespective of their origin, all types are pre-treated via crosslinking to render the tissue n...

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Autores principales: Steitz, Marvin, Zouhair, Sabra, Khan, Mahamuda Badhon, Breitenstein-Attach, Alexander, Fritsch, Katharina, Tuladhar, Sugat Ratna, Wulsten, Dag, Wolkers, Willem-Frederik, Sun, Xiaolin, Hao, Yimeng, Emeis, Jasper, Lange, Hans-E., Berger, Felix, Schmitt, Boris
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10669889/
https://www.ncbi.nlm.nih.gov/pubmed/38002371
http://dx.doi.org/10.3390/bioengineering10111247
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author Steitz, Marvin
Zouhair, Sabra
Khan, Mahamuda Badhon
Breitenstein-Attach, Alexander
Fritsch, Katharina
Tuladhar, Sugat Ratna
Wulsten, Dag
Wolkers, Willem-Frederik
Sun, Xiaolin
Hao, Yimeng
Emeis, Jasper
Lange, Hans-E.
Berger, Felix
Schmitt, Boris
author_facet Steitz, Marvin
Zouhair, Sabra
Khan, Mahamuda Badhon
Breitenstein-Attach, Alexander
Fritsch, Katharina
Tuladhar, Sugat Ratna
Wulsten, Dag
Wolkers, Willem-Frederik
Sun, Xiaolin
Hao, Yimeng
Emeis, Jasper
Lange, Hans-E.
Berger, Felix
Schmitt, Boris
author_sort Steitz, Marvin
collection PubMed
description Biological bioprostheses such as grafts, patches, and heart valves are often derived from biological tissue like the pericardium. These bioprostheses can be of xenogenic, allogeneic, or autologous origin. Irrespective of their origin, all types are pre-treated via crosslinking to render the tissue non-antigenic and mechanically strong or to minimize degradation. The most widely used crosslinking agent is glutaraldehyde. However, glutaraldehyde-treated tissue is prone to calcification, inflammatory degradation, and mechanical injury, and it is incapable of matrix regeneration, leading to structural degeneration over time. In this work, we are investigating an alternative crosslinking method for an intraoperative application. The treated tissue‘s crosslinking degree was evaluated by differential scanning calorimetry. To confirm the findings, a collagenase assay was conducted. Uniaxial tensile testing was used to assess the tissue’s mechanical properties. To support the findings, the treated tissue was visualized using two-photon microscopy. Additionally, fourier transform infrared spectroscopy was performed to study the overall protein secondary structure. Finally, a crosslinking procedure was identified for intraoperative processing. The samples showed a significant increase in thermal and enzymatic stability after treatment compared to the control, with a difference of up to 22.2 °C and 100%, respectively. Also, the tissue showed similar biomechanics to glutaraldehyde-treated tissue, showing greater extensibility, a higher failure strain, and a lower ultimate tensile strength than the control. The significant difference in the structure band ratio after treatment is proof of the introduction of additional crosslinks compared to the untreated control with regard to differences in the amide-I region. The microscopic images support these findings, showing an alteration of the fiber orientation after treatment. For collagen-based biomaterials, such as pericardial tissue, the novel phenolic crosslinking agent proved to be an equivalent alternative to glutaraldehyde regarding tissue characteristics. Although long-term studies must be performed to investigate superiority in terms of longevity and calcification, our novel crosslinking agent can be applied in concentrations of 1.5% or 2.0% for the treatment of biomaterials.
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spelling pubmed-106698892023-10-25 A Glutaraldehyde-Free Crosslinking Method for the Treatment of Collagen-Based Biomaterials for Clinical Application Steitz, Marvin Zouhair, Sabra Khan, Mahamuda Badhon Breitenstein-Attach, Alexander Fritsch, Katharina Tuladhar, Sugat Ratna Wulsten, Dag Wolkers, Willem-Frederik Sun, Xiaolin Hao, Yimeng Emeis, Jasper Lange, Hans-E. Berger, Felix Schmitt, Boris Bioengineering (Basel) Article Biological bioprostheses such as grafts, patches, and heart valves are often derived from biological tissue like the pericardium. These bioprostheses can be of xenogenic, allogeneic, or autologous origin. Irrespective of their origin, all types are pre-treated via crosslinking to render the tissue non-antigenic and mechanically strong or to minimize degradation. The most widely used crosslinking agent is glutaraldehyde. However, glutaraldehyde-treated tissue is prone to calcification, inflammatory degradation, and mechanical injury, and it is incapable of matrix regeneration, leading to structural degeneration over time. In this work, we are investigating an alternative crosslinking method for an intraoperative application. The treated tissue‘s crosslinking degree was evaluated by differential scanning calorimetry. To confirm the findings, a collagenase assay was conducted. Uniaxial tensile testing was used to assess the tissue’s mechanical properties. To support the findings, the treated tissue was visualized using two-photon microscopy. Additionally, fourier transform infrared spectroscopy was performed to study the overall protein secondary structure. Finally, a crosslinking procedure was identified for intraoperative processing. The samples showed a significant increase in thermal and enzymatic stability after treatment compared to the control, with a difference of up to 22.2 °C and 100%, respectively. Also, the tissue showed similar biomechanics to glutaraldehyde-treated tissue, showing greater extensibility, a higher failure strain, and a lower ultimate tensile strength than the control. The significant difference in the structure band ratio after treatment is proof of the introduction of additional crosslinks compared to the untreated control with regard to differences in the amide-I region. The microscopic images support these findings, showing an alteration of the fiber orientation after treatment. For collagen-based biomaterials, such as pericardial tissue, the novel phenolic crosslinking agent proved to be an equivalent alternative to glutaraldehyde regarding tissue characteristics. Although long-term studies must be performed to investigate superiority in terms of longevity and calcification, our novel crosslinking agent can be applied in concentrations of 1.5% or 2.0% for the treatment of biomaterials. MDPI 2023-10-25 /pmc/articles/PMC10669889/ /pubmed/38002371 http://dx.doi.org/10.3390/bioengineering10111247 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Steitz, Marvin
Zouhair, Sabra
Khan, Mahamuda Badhon
Breitenstein-Attach, Alexander
Fritsch, Katharina
Tuladhar, Sugat Ratna
Wulsten, Dag
Wolkers, Willem-Frederik
Sun, Xiaolin
Hao, Yimeng
Emeis, Jasper
Lange, Hans-E.
Berger, Felix
Schmitt, Boris
A Glutaraldehyde-Free Crosslinking Method for the Treatment of Collagen-Based Biomaterials for Clinical Application
title A Glutaraldehyde-Free Crosslinking Method for the Treatment of Collagen-Based Biomaterials for Clinical Application
title_full A Glutaraldehyde-Free Crosslinking Method for the Treatment of Collagen-Based Biomaterials for Clinical Application
title_fullStr A Glutaraldehyde-Free Crosslinking Method for the Treatment of Collagen-Based Biomaterials for Clinical Application
title_full_unstemmed A Glutaraldehyde-Free Crosslinking Method for the Treatment of Collagen-Based Biomaterials for Clinical Application
title_short A Glutaraldehyde-Free Crosslinking Method for the Treatment of Collagen-Based Biomaterials for Clinical Application
title_sort glutaraldehyde-free crosslinking method for the treatment of collagen-based biomaterials for clinical application
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10669889/
https://www.ncbi.nlm.nih.gov/pubmed/38002371
http://dx.doi.org/10.3390/bioengineering10111247
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