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Layer-by-layer assembly of mucin and chitosan - Influence of surface properties, concentration and type of mucin
Malmö högskola, Faculty of Health and Society (HS).
Malmö högskola, Faculty of Odontology (OD).ORCID iD: 0000-0001-8495-5186
Malmö högskola, Faculty of Health and Society (HS).ORCID iD: 0000-0003-0392-3540
Malmö högskola, Faculty of Health and Society (HS).
2006 (English)In: Journal of Colloid and Interface Science, ISSN 0021-9797, E-ISSN 1095-7103, Vol. 299, no 2, p. 608-616Article in journal (Refereed) Published
Abstract [en]

Bovine submaxillary mucin (BSM) and chitosan were used to build layer-by-layer structures on solid substrates. The build-up was monitored using in situ ellipsometry to obtain time resolved values of the thickness and adsorbed amount. Additionally surface morphology during build-up was studied by atomic force microscopy (AFM). It was found that the adsorbed amount of the film increases approximately linearly with each deposition cycle on hydrophobized silica whereas construction on silica was found not to be possible at the experimental conditions used. We conclude that sufficient amount of the first mucin layer is crucial for the subsequent multilayer formation. The complex build-up kinetics on hydrophobized silica is characterized by adsorption and redissolution processes and the overall growth is the sum of both processes. AFM imaging on hydrophobized silica also confirmed the presence of redissolution processes and chitosan addition led to a reduction both in the number of surface aggregates and in the roughness of the surface. The present work also shows that by adjusting the relative concentrations of the polyelectrolytes it is possible to change the growth rate considerably. The final structures after deposition of 8 bilayers were found to have a high content of water and film stability test revealed that a substantial amount dissolves when increasing electrolyte concentration or pH of the ambient solution. Human mucin from saliva (MUC5B) was also used to create multilayers with chitosan on hydrophobized silica and it was revealed that no redissolution appears to be present in this system.

Place, publisher, year, edition, pages
Academic Press, 2006. Vol. 299, no 2, p. 608-616
Keywords [en]
mucin, chitosan, multilayer
National Category
Physical Chemistry
Identifiers
URN: urn:nbn:se:mau:diva-5043DOI: 10.1016/j.jcis.2006.02.027ISI: 000238294800015PubMedID: 16564534Scopus ID: 2-s2.0-33646928130Local ID: 3151OAI: oai:DiVA.org:mau-5043DiVA, id: diva2:1401878
Available from: 2020-02-28 Created: 2020-02-28 Last updated: 2025-09-01Bibliographically approved
In thesis
1. Interactions of Mucins with Biopolymers and Drug Delivery Particles
Open this publication in new window or tab >>Interactions of Mucins with Biopolymers and Drug Delivery Particles
2008 (English)Doctoral thesis, comprehensive summary (Other academic)
Abstract [en]

The main components in the mucous gels apart from water are mucins, which are proteins with high molecular weights and an abundance of negatively charged oligosaccharide side chains. The aim of the investigations was to characterize interactions between mucins and other proteins that are present in the mucous gel, and also between mucins and components used in pharmaceutical formulations. More specifically, the main objectives were (I) to investigate the possibility to assemble multilayer films with mucins and oppositely charged polymers or proteins on solid substrates; (II) to evaluate mucoadhesive proper-ties of drug delivery particles by examination of their interactions with mucins. The construction of multilayer films was performed on silica and hydrophobized silica surfaces by alternate adsorption, and the adsorbed amount and thickness of the films were measured in situ by time resolved ellipsometry. It was demonstrated that films could be assembled using mucins in combination with both chitosan and lactoperoxidase. The build-up was characterized by adsorption and redissolution processes, and the extent of redissolution could be explained by taking the charge densities and concentrations of the components into account. It was also demonstrated that the nature of the substrate can be crucial for the possibilities to assemble multilayer films, and from the results it may be concluded that a high amount of mucin in the first step is important for successful layer-by-layer assembly. Furthermore, it was demonstrated that lactoperoxidase is catalytically active when adsorbed to mucin layers, and it may thereby exert its antimicrobial action. The evaluation of mucoadhesive properties of drug delivery particles was performed with lipid nanoparticles stabilized by a poly(ethylene oxide) based polymer and with particles modified by chitosan. Both types of model particles (unmodified and chitosan modified) were investigated by measuring their adsorption to mucin-coated silica surfaces by ellipsometry. It was shown that the binding of unmodified particles to mucin-coated silica surfaces was weak and pH-dependent. Based on the pH and electrolyte dependence of the adsorption, it was proposed that the interaction is mediated by hydrogen bonding between protonated carboxyl groups in the mucin molecule and oxygen atoms in poly(ethylene oxide). Chitosan modified particles, on the other hand, showed a substantial and strong binding to mucin-coated surfaces, which can probably be attributed to interactions between amino groups in chitosan and negatively charged groups in the mucin layer. The findings from the present investigations are in agreement with previous reports on the interaction of mucins with poly(ethylene oxide) and chitosan. It can therefore be concluded that the methodology applied is useful for evaluating mucoadhesive properties of nanoparticles.

Place, publisher, year, edition, pages
Malmö University, 2008
Series
Malmö University Health and Society Dissertations, ISSN 1653-5383
Keywords
mucin, chitosan, lactoperoxidase, multilayer, mucoadhesion, nanoparticles, ellipsometry
National Category
Physical Chemistry
Identifiers
urn:nbn:se:mau:diva-7339 (URN)5930 (Local ID)978-91-7104-212-5 (ISBN)5930 (Archive number)5930 (OAI)
Note

Note: The papers are not included in the fulltext online.

Paper III and V in dissertation as manuscript, paper IV as accepted manuscript.

Available from: 2020-02-28 Created: 2020-02-28 Last updated: 2024-03-05Bibliographically approved

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Svensson, OlofLindh, LiselottCárdenas, MaritéArnebrant, Thomas

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