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Preliminary Investigation of the Dissolution Behavior, Cytocompatibility, Effects of Fibrinogen Conformation and Platelet Adhesion for Radiopaque Embolic Particles

Experimental embolic particles based on a novel zinc-silicate glass system have been biologically evaluated for potential consideration in transcatheter arterial embolization procedures. In addition to controlling the cytotoxicity and haemocompatibility for such embolic particles, its glass structur...

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Autores principales: Kehoe, Sharon, Tremblay, Marie-Laurence, Coughlan, Aisling, Towler, Mark R., Rainey, Jan K., Abraham, Robert J., Boyd, Daniel
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4030908/
https://www.ncbi.nlm.nih.gov/pubmed/24956083
http://dx.doi.org/10.3390/jfb4030089
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author Kehoe, Sharon
Tremblay, Marie-Laurence
Coughlan, Aisling
Towler, Mark R.
Rainey, Jan K.
Abraham, Robert J.
Boyd, Daniel
author_facet Kehoe, Sharon
Tremblay, Marie-Laurence
Coughlan, Aisling
Towler, Mark R.
Rainey, Jan K.
Abraham, Robert J.
Boyd, Daniel
author_sort Kehoe, Sharon
collection PubMed
description Experimental embolic particles based on a novel zinc-silicate glass system have been biologically evaluated for potential consideration in transcatheter arterial embolization procedures. In addition to controlling the cytotoxicity and haemocompatibility for such embolic particles, its glass structure may mediate specific responses via dissolution in the physiological environment. In a 120 h in-vitro dissolution study, ion release levels for silicon (Si(4+)), sodium (Na(+)), calcium (Ca(2+)), zinc (Zn(2+)), titanium (Ti(4+)), lanthanum (La(3+)), strontium (Sr(2+)), and magnesium (Mg(2+)), were found to range from 0.04 to 5.41 ppm, 0.27–2.28 ppm, 2.32–8.47 ppm, 0.16–0.20 ppm, 0.12–2.15 ppm, 0.16–0.49 ppm and 0.01–0.12 ppm, respectively for the series of glass compositions evaluated. Initial release of Zn(2+) (1.93–10.40 ppm) was only evident after 120 h. All compositions showed levels of cell viabilities ranging from 61.31 ± 4.33% to 153.7 ± 1.25% at 25%–100% serial extract dilutions. The conformational state of fibrinogen, known to induce thrombi, indicated that no changes were induced with respect of the materials dissolution by-products. Furthermore, the best-in-class experimental composition showed equivalency to contour PVA in terms of inducing platelet adhesion. The data generated here provides requisite evidence to continue to in-vivo pre-clinical evaluation using the best-in-class experimental composition evaluated.
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spelling pubmed-40309082014-06-12 Preliminary Investigation of the Dissolution Behavior, Cytocompatibility, Effects of Fibrinogen Conformation and Platelet Adhesion for Radiopaque Embolic Particles Kehoe, Sharon Tremblay, Marie-Laurence Coughlan, Aisling Towler, Mark R. Rainey, Jan K. Abraham, Robert J. Boyd, Daniel J Funct Biomater Article Experimental embolic particles based on a novel zinc-silicate glass system have been biologically evaluated for potential consideration in transcatheter arterial embolization procedures. In addition to controlling the cytotoxicity and haemocompatibility for such embolic particles, its glass structure may mediate specific responses via dissolution in the physiological environment. In a 120 h in-vitro dissolution study, ion release levels for silicon (Si(4+)), sodium (Na(+)), calcium (Ca(2+)), zinc (Zn(2+)), titanium (Ti(4+)), lanthanum (La(3+)), strontium (Sr(2+)), and magnesium (Mg(2+)), were found to range from 0.04 to 5.41 ppm, 0.27–2.28 ppm, 2.32–8.47 ppm, 0.16–0.20 ppm, 0.12–2.15 ppm, 0.16–0.49 ppm and 0.01–0.12 ppm, respectively for the series of glass compositions evaluated. Initial release of Zn(2+) (1.93–10.40 ppm) was only evident after 120 h. All compositions showed levels of cell viabilities ranging from 61.31 ± 4.33% to 153.7 ± 1.25% at 25%–100% serial extract dilutions. The conformational state of fibrinogen, known to induce thrombi, indicated that no changes were induced with respect of the materials dissolution by-products. Furthermore, the best-in-class experimental composition showed equivalency to contour PVA in terms of inducing platelet adhesion. The data generated here provides requisite evidence to continue to in-vivo pre-clinical evaluation using the best-in-class experimental composition evaluated. MDPI 2013-07-10 /pmc/articles/PMC4030908/ /pubmed/24956083 http://dx.doi.org/10.3390/jfb4030089 Text en © 2013 by the authors; licensee MDPI, Basel, Switzerland. http://creativecommons.org/licenses/by/3.0/ This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution license (http://creativecommons.org/licenses/by/3.0/).
spellingShingle Article
Kehoe, Sharon
Tremblay, Marie-Laurence
Coughlan, Aisling
Towler, Mark R.
Rainey, Jan K.
Abraham, Robert J.
Boyd, Daniel
Preliminary Investigation of the Dissolution Behavior, Cytocompatibility, Effects of Fibrinogen Conformation and Platelet Adhesion for Radiopaque Embolic Particles
title Preliminary Investigation of the Dissolution Behavior, Cytocompatibility, Effects of Fibrinogen Conformation and Platelet Adhesion for Radiopaque Embolic Particles
title_full Preliminary Investigation of the Dissolution Behavior, Cytocompatibility, Effects of Fibrinogen Conformation and Platelet Adhesion for Radiopaque Embolic Particles
title_fullStr Preliminary Investigation of the Dissolution Behavior, Cytocompatibility, Effects of Fibrinogen Conformation and Platelet Adhesion for Radiopaque Embolic Particles
title_full_unstemmed Preliminary Investigation of the Dissolution Behavior, Cytocompatibility, Effects of Fibrinogen Conformation and Platelet Adhesion for Radiopaque Embolic Particles
title_short Preliminary Investigation of the Dissolution Behavior, Cytocompatibility, Effects of Fibrinogen Conformation and Platelet Adhesion for Radiopaque Embolic Particles
title_sort preliminary investigation of the dissolution behavior, cytocompatibility, effects of fibrinogen conformation and platelet adhesion for radiopaque embolic particles
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4030908/
https://www.ncbi.nlm.nih.gov/pubmed/24956083
http://dx.doi.org/10.3390/jfb4030089
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