Please use this identifier to cite or link to this item: doi:10.22028/D291-40652
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Title: Cytocompatibility Evaluation of PEG-Methylsulfone Hydrogels
Author(s): Trujillo, Sara
Kasper, Jennifer
de Miguel-Jiménez, Adrián
Abt, Britta
Bauer, Alina
Mekontso, Joëlle
Pearson, Samuel
del Campo Bécares, Aránzazu
Language: English
Title: ACS omega
Volume: 8
Issue: 35
Pages: 32043–32052
Publisher/Platform: ACS
Year of Publication: 2023
DDC notations: 540 Chemistry
Publikation type: Journal Article
Abstract: Methylsulfone derivatized poly(ethylene) glycol (PEG) macromers can be biofunctionalized with thiolated ligands and cross-linked with thiol-based cross-linkers to obtain bioactive PEG hydrogels for in situ cell encapsulation. Methylsulfonyl-thiol (MS-SH) reactions present several advantages for this purpose when compared to other thiol-based cross-linking systems. They proceed with adequate and tunable kinetics for encapsulation, they reach a high conversion degree with good selectivity, and they generate stable reaction products. Our previous work demonstrated the cytocompatibility of cross-linked PEG-MS/thiol hydrogels in contact with fibroblasts. However, the cytocompatibility of the in situ MS-SH cross-linking reaction itself, which generates methylsulfinic acid as byproduct at the cross-linked site, remains to be evaluated. These studies are necessary to evaluate the potential of these systems for in vivo applications. Here we perform an extensive cytocompatibility study of PEG hydrogels during in situ cross-linking by the methylsulfonyl-thiol reaction. We compare these results with maleimide-thiol cross-linked PEGs which are well established for cell culture and in vivo experiments and do not involve the release of a byproduct. We show that fibroblasts and endothelial cells remain viable after in situ polymerization of methylsulfonyl-thiol gels on the top of the cell layers. Cell viability seems better than after in situ cross-linking hydrogels with maleimide-thiol chemistry. The endothelial cell proinflammatory phenotype is low and similar to the one obtained by the maleimide-thiol reaction. Finally, no activation of monocytes is observed. All in all, these results demonstrate that the methylsulfonyl-thiol chemistry is cytocompatible and does not trigger high pro-inflammatory responses in endothelial cells and monocytes. These results make methylsulfonyl-thiol chemistries eligible for in vivo testing and eventually clinical application in the future.
DOI of the first publication: 10.1021/acsomega.3c03952
URL of the first publication: https://pubs.acs.org/doi/10.1021/acsomega.3c03952
Link to this record: urn:nbn:de:bsz:291--ds-406520
hdl:20.500.11880/36543
http://dx.doi.org/10.22028/D291-40652
ISSN: 2470-1343
Date of registration: 2-Oct-2023
Faculty: NT - Naturwissenschaftlich- Technische Fakultät
Department: NT - Chemie
Professorship: NT - Prof. Dr. Aránzazu del Campo
Collections:SciDok - Der Wissenschaftsserver der Universität des Saarlandes

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