4.7 Article

Folate-Conjugated Polymer Micelles with pH-Triggered Drug Release Properties

Journal

MACROMOLECULAR RAPID COMMUNICATIONS
Volume 31, Issue 13, Pages 1163-1169

Publisher

WILEY-V C H VERLAG GMBH
DOI: 10.1002/marc.200900876

Keywords

block copolymers; doxorubicin; folate; micelles; stimuli-sensitive polymers

Funding

  1. National University of Singapore (NUS) [R-279-000-282-112]

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Folate has been applied as a targeting moiety for various anticancer drug-delivery agents to avoid non-specific attack of normal tissues as well as to increase cellular uptake at the target tumor cells. Polymer micelles made of poly[(D,L-lactide)-co-glycoliden-poly(ethylene glycol)folate (PLGA-PEG-FOL) was fabricated as a tumor targeting carrier for encapsulating the anticancer drug doxorubicin. To accelerate the drug release in the endosome after folate-mediated cellular uptake, pH-sensitive poly(beta-amino ester)-PEG-FOL (PAE-PEG-FOL) was added together with PLGA-PEG-FOL to form mixed micelles. The results showed that the drug release can be triggered at different pH due to the ionization of PAE. The IC50 of PLGA-PEG-FOL micelles is 0.46 x 10(-6) M. With 20% PAE in the mixed micelles (20:80 mixed micelles), the IC50 decreases to 0.34 x 10(-6) M, which is comparable to that of pure PAE-PEG-FOL micelles at pH 7.4. As a result of the pH sensitivity, the PAE-PEG-FOL micelles are not stable at pH 6.5 or lower, and the drug may be released from the micelles into the extracellular environment before uptake by the cells. The 20:80 mixed micelles are relatively stable at this condition. As a result, the micelles retain more drug in the micelles for a higher degree of cellular uptake by folate receptor-mediated endocytosis, and exhibit higher cytotoxicity.

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