Toward acellular xenogeneic heart valve prostheses: Histological and biomechanical characterization of decellularized and enzymatically deglycosylated porcine pulmonary heart valve matrices
Katja Findeisen
1
,
Lucrezia Morticelli
1
,
Tobias Goecke
1
,
Louisa Kolbeck
1
,
Robert Ramm
1
,
Hans Klaus Höffler
2
,
Gudrun Brandes
3
,
Sotirios A. Korossis
2
,
Axel Haverich
1, 2
,
Andres Hilfiker
1, 2
Publication type: Journal Article
Publication date: 2020-06-18
scimago Q2
wos Q1
SJR: 0.908
CiteScore: 6.4
Impact factor: 4.1
ISSN: 0908665X, 13993089
PubMed ID:
32557876
Immunology
Transplantation
Abstract
The use of decellularized xenogeneic heart valves might offer a solution to overcome the issue of human valve shortage. The aim of this study was to revise decellularization protocols in combination with enzymatic deglycosylation, in order to reduce the immunogenicity of porcine pulmonary heart valves, in means of cells, carbohydrates, and, primarily, Galα1-3Gal (α-Gal) epitope removal. In particular, the valves were decellularized with sodium dodecylsulfate/sodium deoxycholate (SDS/SD), Triton X-100 + SDS (Tx + SDS), or Trypsin + Triton X-100 (Tryp + Tx) followed by enzymatic digestion with PNGaseF, Endoglycosidase H, or O-glycosidase combined with Neuraminidase. Results showed that decellularization alone reduced carbohydrate structures only to a limited extent, and it did not result in an α-Gal free scaffold. Nevertheless, decellularization with Tryp + Tx represented the most effective decellularization protocol in means of carbohydrates reduction. Overall, carbohydrates and α-Gal removal could strongly be improved by applying PNGaseF, in particular in combination with Tryp + Tx treatment, contrary to Endoglycosidase H and O-glycosidase treatments. Furthermore, decellularization with PNGaseF did not affect biomechanical stability, in comparison with decellularization alone, as shown by burst pressure and uniaxial tensile tests. In conclusion, valves decellularized with Tryp + Tx and PNGaseF resulted in prostheses with potentially reduced immunogenicity and maintained mechanical stability.
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Findeisen K. et al. Toward acellular xenogeneic heart valve prostheses: Histological and biomechanical characterization of decellularized and enzymatically deglycosylated porcine pulmonary heart valve matrices // Xenotransplantation. 2020. Vol. 27. No. 5.
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Findeisen K., Morticelli L., Goecke T., Kolbeck L., Ramm R., Höffler H. K., Brandes G., Korossis S. A., Haverich A., Hilfiker A. Toward acellular xenogeneic heart valve prostheses: Histological and biomechanical characterization of decellularized and enzymatically deglycosylated porcine pulmonary heart valve matrices // Xenotransplantation. 2020. Vol. 27. No. 5.
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TY - JOUR
DO - 10.1111/xen.12617
UR - https://doi.org/10.1111/xen.12617
TI - Toward acellular xenogeneic heart valve prostheses: Histological and biomechanical characterization of decellularized and enzymatically deglycosylated porcine pulmonary heart valve matrices
T2 - Xenotransplantation
AU - Findeisen, Katja
AU - Morticelli, Lucrezia
AU - Goecke, Tobias
AU - Kolbeck, Louisa
AU - Ramm, Robert
AU - Höffler, Hans Klaus
AU - Brandes, Gudrun
AU - Korossis, Sotirios A.
AU - Haverich, Axel
AU - Hilfiker, Andres
PY - 2020
DA - 2020/06/18
PB - Wiley
IS - 5
VL - 27
PMID - 32557876
SN - 0908-665X
SN - 1399-3089
ER -
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@article{2020_Findeisen,
author = {Katja Findeisen and Lucrezia Morticelli and Tobias Goecke and Louisa Kolbeck and Robert Ramm and Hans Klaus Höffler and Gudrun Brandes and Sotirios A. Korossis and Axel Haverich and Andres Hilfiker},
title = {Toward acellular xenogeneic heart valve prostheses: Histological and biomechanical characterization of decellularized and enzymatically deglycosylated porcine pulmonary heart valve matrices},
journal = {Xenotransplantation},
year = {2020},
volume = {27},
publisher = {Wiley},
month = {jun},
url = {https://doi.org/10.1111/xen.12617},
number = {5},
doi = {10.1111/xen.12617}
}