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dc.contributor.authorUmerska, A.*
dc.contributor.authorPaluch, Krzysztof J.*
dc.contributor.authorSantos Martinez, M.-J.*
dc.contributor.authorCorrigan, O.I.*
dc.contributor.authorMedina, C.*
dc.contributor.authorTajber, L.*
dc.date.accessioned2017-12-11T13:24:15Z
dc.date.available2017-12-11T13:24:15Z
dc.date.issued2014
dc.identifier.citationUmerska A, Paluch KJ, Santos Martinez M-J et al (2014) Self-assembled hyaluronate/protamine polyelectrolyte nanoplexes: Synthesis, stability, biocompatibility and potential use as peptide carriers. Journal of Biomedical Nanotechnology. 10(12): 3658-3673.
dc.identifier.urihttp://hdl.handle.net/10454/14147
dc.descriptionNo
dc.description.abstractThis work investigates a new type of polyelectrolyte complex nanocarrier composed of hyaluronic acid (HA) and protamine (PROT). Small (approximately 60 nm) and negatively charged nanoparticles (NPs) with a polydispersity index of less than 0.2 were obtained with properties that were dependent on the mixing ratio, concentration of polyelectrolytes and molecular weight of HA. Salmon calcitonin (sCT) was efficiently (up to 100%) associated with the NPs, and the drug loading (9.6-39% w/w) was notably high, possibly due to an interaction between HA and sCT. The NPs released ~70-80% of the sCT after 24 hours, with the estimated total amount of released sCT depending on the amount of HA and PROT present in the NPs. The isoelectric point of the NPs was close to pH 2, and the negative surface charge was maintained above this pH. The HA/PROT nanoplexes protected the sCT from enzymatic degradation and showed low toxicity to intestinal epithelial cells, and thus may be a promising oral delivery system for peptides.
dc.language.isoen
dc.subjectHyaluronic acid
dc.subjectProtamine
dc.subjectCalcitonin
dc.subjectNanoparticles
dc.subjectPolyelectrolyte complex
dc.subjectCaco 2 -cells
dc.titleSelf-assembled hyaluronate/protamine polyelectrolyte nanoplexes: Synthesis, stability, biocompatibility and potential use as peptide carriers
dc.status.refereedYes
dc.typeArticle
dc.type.versionNo full-text in the repository
dc.openaccess.statusclosedAccess
dc.date.accepted26/11/2013


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