Please use this identifier to cite or link to this item: http://hdl.handle.net/2445/96622
Title: PEGylated and poloxamer-modified chitosan nanoparticles incorporating a lysine-based surfactant for pH-triggered doxorubicin release
Author: Scheeren, Laís E.
Nogueira, Daniele R.
Macedo, Letícia B.
Vinardell Martínez-Hidalgo, Ma. Pilar
Mitjans Arnal, Montserrat
Infante Martínez-Pardo, Ma. Rosa
Rolim, Clarice M.B.
Keywords: Medicaments antineoplàstics
Quitosan
Nanopartícules
Agents tensioactius
Sistemes d'alliberament de medicaments
Antineoplastic agents
Chitosan
Nanoparticles
Surface active agents
Drug delivery systems
Issue Date: 28-Nov-2015
Publisher: Elsevier B.V.
Abstract: The growing demand for efficient chemotherapy in many cancers requires novel approaches in target-delivery technologies. Nanomaterials with pH-responsive behavior appear to have potential ability to selectively release the encapsulated molecules by sensing the acidic tumor microenvironment or the low pH found in endosomes. Likewise, polyethylene glycol (PEG)- and poloxamer-modified nanocarriers have been gaining attention regarding their potential to improve the effectiveness of cancer therapy. In this context, DOX-loaded pH-responsive nanoparticles (NPs) modified with PEG or poloxamer were prepared and the effects of these modifiers were evaluated on the overall characteristics of these nanostructures. Chitosan and tripolyphosphate were selected to form NPs by the interaction of oppositely charged compounds. A pH-sensitive lysine-based amphiphile (77KS) was used as a bioactive adjuvant. The strong dependence of 77KS ionization with pH makes this compound an interesting candidate to be used for the design of pH-sensitive devices. The physicochemical characterization of all NPs has been performed, and it was shown that the presence of 77KS clearly promotes a pH-triggered DOX release. Accelerated and continuous release patterns of DOX from CS-NPs under acidic conditions were observed regardless of the presence of PEG or poloxamer. Moreover, photodegradation studies have indicated that the lyophilization of NPs improved DOX stability under UVA radiation. Finally, cytotoxicity experiments have shown the ability of DOX-loaded CS-NPs to kill HeLa tumor cells. Hence, the overall results suggest that these pH-responsive CS-NPs are highly potent delivery systems to target tumor and intracellular environments, rendering them promising DOX carrier systems for cancer therapy.
Note: Versió postprint del document publicat a: http://dx.doi.org/10.1016/j.colsurfb.2015.11.049
It is part of: Colloids and Surfaces B-Biointerfaces, 2015, vol. 138, p. 117-127
Related resource: http://dx.doi.org/10.1016/j.colsurfb.2015.11.049
URI: http://hdl.handle.net/2445/96622
ISSN: 0927-7765
Appears in Collections:Articles publicats en revistes (Bioquímica i Fisiologia)

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