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Histologic Assessment of Drug-Eluting Grafts Related to Implantation Site

Drug-eluting vascular prostheses represent a new direction in vascular surgery to reduce early thrombosis and late intimal hyperplasia for small calibre grafts. Subcutaneous implantation in rats is a rapid and cost-effective screening model to assess the drug-elution effect and could, to some extent...

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Autores principales: Tille, Jean-Christophe, de Valence, Sarra, Mandracchia, Delia, Nottelet, Benjamin, Innocente, Francesco, Gurny, Robert, Möller, Michael, Walpoth, Beat H.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5831816/
https://www.ncbi.nlm.nih.gov/pubmed/29615579
http://dx.doi.org/10.3390/jdb4010011
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author Tille, Jean-Christophe
de Valence, Sarra
Mandracchia, Delia
Nottelet, Benjamin
Innocente, Francesco
Gurny, Robert
Möller, Michael
Walpoth, Beat H.
author_facet Tille, Jean-Christophe
de Valence, Sarra
Mandracchia, Delia
Nottelet, Benjamin
Innocente, Francesco
Gurny, Robert
Möller, Michael
Walpoth, Beat H.
author_sort Tille, Jean-Christophe
collection PubMed
description Drug-eluting vascular prostheses represent a new direction in vascular surgery to reduce early thrombosis and late intimal hyperplasia for small calibre grafts. Subcutaneous implantation in rats is a rapid and cost-effective screening model to assess the drug-elution effect and could, to some extent, be useful to forecast results for vascular prostheses. We compared biological and histological responses to scaffolds in different implantation sites. Polycaprolactone (PCL), paclitaxel-loaded PCL (PCL-PTX) and dexamethasone-loaded PCL (PCL-DXM) electrospun scaffolds were implanted subcutaneously and in an infrarenal abdominal aortic model in rats for up to 12 weeks. At the conclusion of the study, a histological analysis was performed. Cellular graft invasion revealed differences in the progression of cellular infiltration between PCL-PTX and PCL/PCL-DXM groups in both models. Cell infiltration increased over time in the aortic model compared to the subcutaneous model for all groups. Cell counting revealed major differences in fibroblast, macrophage and giant cell graft colonisation in all groups and models over time. Macrophages and giant cells increased in the PCL aortic model; whereas in the subcutaneous model these cell types increased only after three weeks or even decreased in the drug-eluting PCL groups. Other major findings were observed only in the aortic replacement such as extracellular matrix deposition and neo-angiogenesis. The subcutaneous implant model can be used for screening, especially when drug-eluting effects are studied. However, major histological differences were observed in cell type reaction and depth of cell penetration compared to the aortic model. Our results demonstrate that the implantation site is a critical determinant of the biological response.
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spelling pubmed-58318162018-03-30 Histologic Assessment of Drug-Eluting Grafts Related to Implantation Site Tille, Jean-Christophe de Valence, Sarra Mandracchia, Delia Nottelet, Benjamin Innocente, Francesco Gurny, Robert Möller, Michael Walpoth, Beat H. J Dev Biol Article Drug-eluting vascular prostheses represent a new direction in vascular surgery to reduce early thrombosis and late intimal hyperplasia for small calibre grafts. Subcutaneous implantation in rats is a rapid and cost-effective screening model to assess the drug-elution effect and could, to some extent, be useful to forecast results for vascular prostheses. We compared biological and histological responses to scaffolds in different implantation sites. Polycaprolactone (PCL), paclitaxel-loaded PCL (PCL-PTX) and dexamethasone-loaded PCL (PCL-DXM) electrospun scaffolds were implanted subcutaneously and in an infrarenal abdominal aortic model in rats for up to 12 weeks. At the conclusion of the study, a histological analysis was performed. Cellular graft invasion revealed differences in the progression of cellular infiltration between PCL-PTX and PCL/PCL-DXM groups in both models. Cell infiltration increased over time in the aortic model compared to the subcutaneous model for all groups. Cell counting revealed major differences in fibroblast, macrophage and giant cell graft colonisation in all groups and models over time. Macrophages and giant cells increased in the PCL aortic model; whereas in the subcutaneous model these cell types increased only after three weeks or even decreased in the drug-eluting PCL groups. Other major findings were observed only in the aortic replacement such as extracellular matrix deposition and neo-angiogenesis. The subcutaneous implant model can be used for screening, especially when drug-eluting effects are studied. However, major histological differences were observed in cell type reaction and depth of cell penetration compared to the aortic model. Our results demonstrate that the implantation site is a critical determinant of the biological response. MDPI 2016-02-20 /pmc/articles/PMC5831816/ /pubmed/29615579 http://dx.doi.org/10.3390/jdb4010011 Text en © 2016 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons by Attribution (CC-BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Tille, Jean-Christophe
de Valence, Sarra
Mandracchia, Delia
Nottelet, Benjamin
Innocente, Francesco
Gurny, Robert
Möller, Michael
Walpoth, Beat H.
Histologic Assessment of Drug-Eluting Grafts Related to Implantation Site
title Histologic Assessment of Drug-Eluting Grafts Related to Implantation Site
title_full Histologic Assessment of Drug-Eluting Grafts Related to Implantation Site
title_fullStr Histologic Assessment of Drug-Eluting Grafts Related to Implantation Site
title_full_unstemmed Histologic Assessment of Drug-Eluting Grafts Related to Implantation Site
title_short Histologic Assessment of Drug-Eluting Grafts Related to Implantation Site
title_sort histologic assessment of drug-eluting grafts related to implantation site
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5831816/
https://www.ncbi.nlm.nih.gov/pubmed/29615579
http://dx.doi.org/10.3390/jdb4010011
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