Acid-labile core cross-linked micelles for pH-triggered release of antitumor drugs.

Biomacromolecules

Centre for Advanced Macromolecular Design, The University of New South Wales, Sydney 2052, NSW, Australia.

Published: July 2008

AI Article Synopsis

  • Researchers developed micelles from a block copolymer (PHEA-b-PBA) using RAFT polymerization, which were then cross-linked to form a stable core without altering micelle size.
  • The presence of the cross-linker was confirmed through physicochemical analysis after the micelles were cleaved under acidic conditions.
  • The system demonstrated a high capacity for loading doxorubicin (60 wt%) and showed that releasing the drug at acidic pH is faster due to partial hydrolysis of the cross-links, indicating a novel approach for controlled drug delivery.

Article Abstract

Micelles of a model amphiphilic block copolymer, poly(hydroxyethyl acrylate)-block-poly(n-butyl acrylate) (PHEA-b-PBA), synthesized via the RAFT polymerization were cross-linked by copolymerization of a degradable cross-linker from the living RAFT-end groups of PBA chains, yielding a cross-linked core without affecting significantly the original micelle size. The cross-linker incorporation into the micelles was evidenced via physicochemical analysis of the copolymer unimers formed upon acidic cleavage of the cross-linked micelles. High doxorubicin loading capacities (60 wt %) were obtained. Hydrolysis of less than half of the cross-links in the core was found to be sufficient to release doxorubicin faster at acidic pH compared to neutral pH. The system represents the first example of core-cross-linked micelles that can be destabilized (potentially both above and below CMC) by the pH-dependent cleavage of the cross-links and the subsequent polarity change in the core to enable the release of hydrophobic drugs entrapped inside the micelle.

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Source
http://dx.doi.org/10.1021/bm800043nDOI Listing

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