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The Role of Biodegradable Poly-(L-lactide)-Based Polymers in Blood Cell Activation and Platelet-Monocyte Interaction

The main purpose of new stent technologies is to overcome unfavorable material-related incompatibilities by producing bio- and hemo-compatible polymers with anti-inflammatory and anti-thrombogenic properties. In this context, wettability is an important surface property, which has a major impact on...

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Autores principales: Strohbach, Anne, Maess, Friedemann, Wulf, Katharina, Petersen, Svea, Grabow, Niels, Schmitz, Klaus-Peter, Felix, Stephan B., Busch, Raila
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8231768/
https://www.ncbi.nlm.nih.gov/pubmed/34199303
http://dx.doi.org/10.3390/ijms22126340
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author Strohbach, Anne
Maess, Friedemann
Wulf, Katharina
Petersen, Svea
Grabow, Niels
Schmitz, Klaus-Peter
Felix, Stephan B.
Busch, Raila
author_facet Strohbach, Anne
Maess, Friedemann
Wulf, Katharina
Petersen, Svea
Grabow, Niels
Schmitz, Klaus-Peter
Felix, Stephan B.
Busch, Raila
author_sort Strohbach, Anne
collection PubMed
description The main purpose of new stent technologies is to overcome unfavorable material-related incompatibilities by producing bio- and hemo-compatible polymers with anti-inflammatory and anti-thrombogenic properties. In this context, wettability is an important surface property, which has a major impact on the biological response of blood cells. However, the influence of local hemodynamic changes also influences blood cell activation. Therefore, we investigated biodegradable polymers with different wettability to identify possible aspects for a better prediction of blood compatibility. We applied shear rates of 100 s(−1) and 1500 s(−1) and assessed platelet and monocyte activation as well as the formation of CD62P+ monocyte-bound platelets via flow cytometry. Aggregation of circulating platelets induced by collagen was assessed by light transmission aggregometry. Via live cell imaging, leukocytes were tracked on biomaterial surfaces to assess their average velocity. Monocyte adhesion on biomaterials was determined by fluorescence microscopy. In response to low shear rates of 100 s(−1), activation of circulating platelets and monocytes as well as the formation of CD62P+ monocyte-bound platelets corresponded to the wettability of the underlying material with the most favorable conditions on more hydrophilic surfaces. Under high shear rates, however, blood compatibility cannot only be predicted by the concept of wettability. We assume that the mechanisms of blood cell-polymer interactions do not allow for a rule-of-thumb prediction of the blood compatibility of a material, which makes extensive in vitro testing mandatory.
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spelling pubmed-82317682021-06-26 The Role of Biodegradable Poly-(L-lactide)-Based Polymers in Blood Cell Activation and Platelet-Monocyte Interaction Strohbach, Anne Maess, Friedemann Wulf, Katharina Petersen, Svea Grabow, Niels Schmitz, Klaus-Peter Felix, Stephan B. Busch, Raila Int J Mol Sci Article The main purpose of new stent technologies is to overcome unfavorable material-related incompatibilities by producing bio- and hemo-compatible polymers with anti-inflammatory and anti-thrombogenic properties. In this context, wettability is an important surface property, which has a major impact on the biological response of blood cells. However, the influence of local hemodynamic changes also influences blood cell activation. Therefore, we investigated biodegradable polymers with different wettability to identify possible aspects for a better prediction of blood compatibility. We applied shear rates of 100 s(−1) and 1500 s(−1) and assessed platelet and monocyte activation as well as the formation of CD62P+ monocyte-bound platelets via flow cytometry. Aggregation of circulating platelets induced by collagen was assessed by light transmission aggregometry. Via live cell imaging, leukocytes were tracked on biomaterial surfaces to assess their average velocity. Monocyte adhesion on biomaterials was determined by fluorescence microscopy. In response to low shear rates of 100 s(−1), activation of circulating platelets and monocytes as well as the formation of CD62P+ monocyte-bound platelets corresponded to the wettability of the underlying material with the most favorable conditions on more hydrophilic surfaces. Under high shear rates, however, blood compatibility cannot only be predicted by the concept of wettability. We assume that the mechanisms of blood cell-polymer interactions do not allow for a rule-of-thumb prediction of the blood compatibility of a material, which makes extensive in vitro testing mandatory. MDPI 2021-06-13 /pmc/articles/PMC8231768/ /pubmed/34199303 http://dx.doi.org/10.3390/ijms22126340 Text en © 2021 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
Strohbach, Anne
Maess, Friedemann
Wulf, Katharina
Petersen, Svea
Grabow, Niels
Schmitz, Klaus-Peter
Felix, Stephan B.
Busch, Raila
The Role of Biodegradable Poly-(L-lactide)-Based Polymers in Blood Cell Activation and Platelet-Monocyte Interaction
title The Role of Biodegradable Poly-(L-lactide)-Based Polymers in Blood Cell Activation and Platelet-Monocyte Interaction
title_full The Role of Biodegradable Poly-(L-lactide)-Based Polymers in Blood Cell Activation and Platelet-Monocyte Interaction
title_fullStr The Role of Biodegradable Poly-(L-lactide)-Based Polymers in Blood Cell Activation and Platelet-Monocyte Interaction
title_full_unstemmed The Role of Biodegradable Poly-(L-lactide)-Based Polymers in Blood Cell Activation and Platelet-Monocyte Interaction
title_short The Role of Biodegradable Poly-(L-lactide)-Based Polymers in Blood Cell Activation and Platelet-Monocyte Interaction
title_sort role of biodegradable poly-(l-lactide)-based polymers in blood cell activation and platelet-monocyte interaction
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8231768/
https://www.ncbi.nlm.nih.gov/pubmed/34199303
http://dx.doi.org/10.3390/ijms22126340
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