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Bio-Engineered Scaffolds Derived from Decellularized Human Esophagus for Functional Organ Reconstruction

Esophageal reconstruction through bio-engineered allografts that highly resemble the peculiar properties of the tissue extracellular matrix (ECM) is a prospective strategy to overcome the limitations of current surgical approaches. In this work, human esophagus was decellularized for the first time...

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Autores principales: Barbon, Silvia, Biccari, Andrea, Stocco, Elena, Capovilla, Giovanni, D’Angelo, Edoardo, Todesco, Martina, Sandrin, Deborah, Bagno, Andrea, Romanato, Filippo, Macchi, Veronica, De Caro, Raffaele, Agostini, Marco, Merigliano, Stefano, Valmasoni, Michele, Porzionato, Andrea
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9563623/
https://www.ncbi.nlm.nih.gov/pubmed/36230907
http://dx.doi.org/10.3390/cells11192945
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author Barbon, Silvia
Biccari, Andrea
Stocco, Elena
Capovilla, Giovanni
D’Angelo, Edoardo
Todesco, Martina
Sandrin, Deborah
Bagno, Andrea
Romanato, Filippo
Macchi, Veronica
De Caro, Raffaele
Agostini, Marco
Merigliano, Stefano
Valmasoni, Michele
Porzionato, Andrea
author_facet Barbon, Silvia
Biccari, Andrea
Stocco, Elena
Capovilla, Giovanni
D’Angelo, Edoardo
Todesco, Martina
Sandrin, Deborah
Bagno, Andrea
Romanato, Filippo
Macchi, Veronica
De Caro, Raffaele
Agostini, Marco
Merigliano, Stefano
Valmasoni, Michele
Porzionato, Andrea
author_sort Barbon, Silvia
collection PubMed
description Esophageal reconstruction through bio-engineered allografts that highly resemble the peculiar properties of the tissue extracellular matrix (ECM) is a prospective strategy to overcome the limitations of current surgical approaches. In this work, human esophagus was decellularized for the first time in the literature by comparing three detergent-enzymatic protocols. After decellularization, residual DNA quantification and histological analyses showed that all protocols efficiently removed cells, DNA (<50 ng/mg of tissue) and muscle fibers, preserving collagen/elastin components. The glycosaminoglycan fraction was maintained (70–98%) in the decellularized versus native tissues, while immunohistochemistry showed unchanged expression of specific ECM markers (collagen IV, laminin). The proteomic signature of acellular esophagi corroborated the retention of structural collagens, basement membrane and matrix–cell interaction proteins. Conversely, decellularization led to the loss of HLA-DR expression, producing non-immunogenic allografts. According to hydroxyproline quantification, matrix collagen was preserved (2–6 µg/mg of tissue) after decellularization, while Second-Harmonic Generation imaging highlighted a decrease in collagen intensity. Based on uniaxial tensile tests, decellularization affected tissue stiffness, but sample integrity/manipulability was still maintained. Finally, the cytotoxicity test revealed that no harmful remnants/contaminants were present on acellular esophageal matrices, suggesting allograft biosafety. Despite the different outcomes showed by the three decellularization methods (regarding, for example, tissue manipulability, DNA removal, and glycosaminoglycans/hydroxyproline contents) the ultimate validation should be provided by future repopulation tests and in vivo orthotopic implant of esophageal scaffolds.
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spelling pubmed-95636232022-10-15 Bio-Engineered Scaffolds Derived from Decellularized Human Esophagus for Functional Organ Reconstruction Barbon, Silvia Biccari, Andrea Stocco, Elena Capovilla, Giovanni D’Angelo, Edoardo Todesco, Martina Sandrin, Deborah Bagno, Andrea Romanato, Filippo Macchi, Veronica De Caro, Raffaele Agostini, Marco Merigliano, Stefano Valmasoni, Michele Porzionato, Andrea Cells Article Esophageal reconstruction through bio-engineered allografts that highly resemble the peculiar properties of the tissue extracellular matrix (ECM) is a prospective strategy to overcome the limitations of current surgical approaches. In this work, human esophagus was decellularized for the first time in the literature by comparing three detergent-enzymatic protocols. After decellularization, residual DNA quantification and histological analyses showed that all protocols efficiently removed cells, DNA (<50 ng/mg of tissue) and muscle fibers, preserving collagen/elastin components. The glycosaminoglycan fraction was maintained (70–98%) in the decellularized versus native tissues, while immunohistochemistry showed unchanged expression of specific ECM markers (collagen IV, laminin). The proteomic signature of acellular esophagi corroborated the retention of structural collagens, basement membrane and matrix–cell interaction proteins. Conversely, decellularization led to the loss of HLA-DR expression, producing non-immunogenic allografts. According to hydroxyproline quantification, matrix collagen was preserved (2–6 µg/mg of tissue) after decellularization, while Second-Harmonic Generation imaging highlighted a decrease in collagen intensity. Based on uniaxial tensile tests, decellularization affected tissue stiffness, but sample integrity/manipulability was still maintained. Finally, the cytotoxicity test revealed that no harmful remnants/contaminants were present on acellular esophageal matrices, suggesting allograft biosafety. Despite the different outcomes showed by the three decellularization methods (regarding, for example, tissue manipulability, DNA removal, and glycosaminoglycans/hydroxyproline contents) the ultimate validation should be provided by future repopulation tests and in vivo orthotopic implant of esophageal scaffolds. MDPI 2022-09-20 /pmc/articles/PMC9563623/ /pubmed/36230907 http://dx.doi.org/10.3390/cells11192945 Text en © 2022 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
Barbon, Silvia
Biccari, Andrea
Stocco, Elena
Capovilla, Giovanni
D’Angelo, Edoardo
Todesco, Martina
Sandrin, Deborah
Bagno, Andrea
Romanato, Filippo
Macchi, Veronica
De Caro, Raffaele
Agostini, Marco
Merigliano, Stefano
Valmasoni, Michele
Porzionato, Andrea
Bio-Engineered Scaffolds Derived from Decellularized Human Esophagus for Functional Organ Reconstruction
title Bio-Engineered Scaffolds Derived from Decellularized Human Esophagus for Functional Organ Reconstruction
title_full Bio-Engineered Scaffolds Derived from Decellularized Human Esophagus for Functional Organ Reconstruction
title_fullStr Bio-Engineered Scaffolds Derived from Decellularized Human Esophagus for Functional Organ Reconstruction
title_full_unstemmed Bio-Engineered Scaffolds Derived from Decellularized Human Esophagus for Functional Organ Reconstruction
title_short Bio-Engineered Scaffolds Derived from Decellularized Human Esophagus for Functional Organ Reconstruction
title_sort bio-engineered scaffolds derived from decellularized human esophagus for functional organ reconstruction
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9563623/
https://www.ncbi.nlm.nih.gov/pubmed/36230907
http://dx.doi.org/10.3390/cells11192945
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