Reduction of xeno‐antigens in porcine pulmonary heart valves by decellularization and glycolytic enzymatic treatment

Hilfiker, Andres; Ramm, Robert; Findeisen, Katja; Goecke, Tobias; Haverich, Axel

doi:10.1111/xen.12083_13

Cited by 6 publications

(7 citation statements)

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“…The risk to include a molecule with high potential to acute response, as the recombinant protein, should carefully be evaluated, avoiding clinical disasters. Hilfiker and collaborators demonstrated the antigenicity reduction by decellularization also suggesting a humanized immunoassay do determine a quantitative antigenicity …”

Section: Discussionmentioning

confidence: 99%

Structural assessments in decellularized extracellular matrix of porcine semilunar heart valves: Evaluation of cell niches

Roderjan

Noronha

Stimamiglio

et al. 2019

Xenotransplantation

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Tissue-engineered heart valves aim to reproduce the biological properties of natural valves with anatomically correct structure and physiological performance. The closest alternative to creating an ideal heart valve substitute is to use decellularized porcine heart valves, due to their anatomy and availability. However, the immunological barrier and the structural maintenance limit the long-term physiological performance of decellularized porcine heart valves. This study investigated the extracellular matrix (ECM) structure of aortic and pulmonary porcine valves decellularized by a low concentration sodium dodecyl sulfate (SDS)-based method in order to determine the ECM scaffold (ECMS) conditions related to remodeling potential. To assess the structures of the leaflets and conduits of the heart valves, ECM components and their organization were evaluated by histology, biochemical analysis (BC), scanning electron microscopy, multiphoton microscopy, tensile test, immunofluorescence labeling (IF), and Raman microspectroscopy used to draw a profile of the cell niches. Histology and multiphoton imaging of decellularized aortic and pulmonary leaflets and conduits revealed a collagen and elastin histoarchitecture with rearrangement, loosening fibers, and glycosaminoglycan depletion confirmed by biochemistry quantification.The potential cytotoxicity of SDS residues was eliminated after 10 wash cycles. The mechanical properties of the structure of the valve indicated a functional resistance of decellularized ECM. The IF demonstrated the presence of basement membrane, suggesting a potential structure for host cell attachment. The RM analysis showed evidence of molecular interactions, suggesting conservation of the chemical composition, particularly among the protein molecular structures. The structural analyses performed in the semilunar porcine heart valves demonstrate that decellularized ECMS has structural properties that support physiological performance and potential host tissue integration. In fact, decellularized leaflet scaffolds were prone to cell interaction after human adipose-derived stromal cell seeding and culturing. Further analysis of biocompatibility, particularly the ECM-cell interaction, can elucidate the remodeling process, in preserved decellularized heart valve scaffold.

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Section: Discussionmentioning

confidence: 99%

Structural assessments in decellularized extracellular matrix of porcine semilunar heart valves: Evaluation of cell niches

Roderjan

Noronha

Stimamiglio

et al. 2019

Xenotransplantation

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“…Термоли-зин в качестве единственного агента может удалять клетки только с поверхности ткани, поэтому его применение ограничено [51]. Высокоспецифичный фермент α-галактозидаза применяется как компонент методики для децеллюляризации ксе-ногенной ткани и отвечает за удаление эпитопа α-Gal [23,52].…”

Section: биологические агентыunclassified

“…Поэтому, к сожалению, недостаточность децеллюляризации (технология предполагала гипотонический лизис клеток и об-работку ДНазой) проявилась только на клиническом этапе -больные погибали из-за быстрой дегенерации и разрыва донорской части стенки аорты вследствие острого воспаления [64]. В настоящий момент проблема ксенотрансплантации по-прежнему не решена [67,52].…”

Section: донорский материал для тканевой инженерииunclassified

Heart Valve Matrices: State of the Art and Perspectives

Петрович¹,

Сергей²,

Игорь³

et al. 2016

Vestnik SPbSU. Series 11. Medicine

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ТКАНЕВЫЕ МАТРИЦЫ КЛАПАНОВ СЕРДЦА: СОСТОЯНИЕ ПРОБЛЕМЫ И ПЕРСПЕКТИВЫ1 Санкт-Петербургский государственный университет, Российская Федерация, 199034, Санкт-Петербург, Университетская наб., 7-9 2 Клиника кардиоторакальной, сосудистой хирургии и трансплантации Медицинского университета Ганновера, Carl-Neuberg Str., 1, OE 6210, 30625, Hannover, GermanyПервые успешные протезирования аортального и митрального клапанов сердца были вы-полнены в 1960 г. соответственно D. Harken и N. Braunwald. В обоих случаях использовались механические протезы, однако спустя всего 10 лет M. Ionescu впервые имплантировал первый биологический клапан человеку. В ходе эволюции биологических клапанных протезов хирур-гами использовались свиные аортальные, ксеноперикардиальные протезы и человеческие аллографты (свежие и криосохраненные), а в последние полтора десятилетия на вооружение были взяты тканевая инженерия и направленная регенерация тканей. В настоящей статье описаны основные проблемы этой области, проведена сравнительная характеристика различ-ных методик децеллюляризации полулунных клапанов, а также перспективы использования тканевой инженерии для создания атриовентрикулярных клапанных заменителей. Библиогр. 73 назв. Ил. 1. Th e fi rst successful aortic and mitral valve replacement was performed, respectively, by D. Harken and N. Braunwald in 1960. Both used mechanical graft s, but 10 years later M. Ionescu implanted a biological valve substitute in humans. As biological valve graft s evolved, multiple sources were used: porcine aortic valves, xenopericardial substitutes, and, most recently, tissue engineered allograft s, reseeded by means of guided repopulation. Th e present work describes the major challenges of these methods, analyses diff erent decellularization approaches used for semilunar valves, and future possibilities for tissue engineering to be applied in humans, such as creation of atrioventricular valve substitutes. Refs 73. Figure 1.

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“…Indeed, carbohydrases such as α-galactosidase or peptide:N-glycosidase F (PNGase F) have been applied for the removal of the α-Gal epitope and N-glycans, respectively, from xenogeneic tissues. [33][34][35] Another carbohydrase with broader specificity, α-amylase from porcine pancreas, has been used for the production of porous foams derived from decellularized porcine left ventricle. 36 Besides carbohydrates removal, enzymes have been largely applied for tissue decellularization.…”

Section: Introductionmentioning

confidence: 99%

“…Elseways, carbohydrates removal using enzymatic treatments has been limited to enzymes with specificity against the known immunogenic carbohydrates or specific types of glycosylations. Indeed, carbohydrases such as α‐galactosidase or peptide:N‐glycosidase F (PNGase F) have been applied for the removal of the α‐Gal epitope and N‐glycans, respectively, from xenogeneic tissues 33‐35 . Another carbohydrase with broader specificity, α‐amylase from porcine pancreas, has been used for the production of porous foams derived from decellularized porcine left ventricle 36 …”

Section: Introductionmentioning

confidence: 99%

Generation of glycans depleted decellularized porcine pericardium, using digestive enzymatic supplements and enzymatic mixtures for food industry

Morticelli

Magdei

Tschalaki

et al. 2021

Xenotransplantation

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Reduction of xeno‐antigens in porcine pulmonary heart valves by decellularization and glycolytic enzymatic treatment

Cited by 6 publications

References 0 publications

Structural assessments in decellularized extracellular matrix of porcine semilunar heart valves: Evaluation of cell niches

Structural assessments in decellularized extracellular matrix of porcine semilunar heart valves: Evaluation of cell niches

Heart Valve Matrices: State of the Art and Perspectives

Generation of glycans depleted decellularized porcine pericardium, using digestive enzymatic supplements and enzymatic mixtures for food industry

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