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PH-dependent, thermosensitive polymeric nanocarriers for drug delivery to solid tumors.


ABSTRACT: Polymeric micelles are promising carriers for anti-cancer agents due to their small size, ease of assembly, and versatility for functionalization. A current challenge in the use of polymeric micelles is the sensitive balance that must be achieved between stability during prolonged blood circulation and release of active drug at the tumor site. Stimuli-responsive materials provide a mechanism for triggered drug release in the acidic tumor and intracellular microenvironments. In this work, we synthesized a series of dual pH- and temperature-responsive block copolymers containing a poly(?-caprolactone) (PCL) hydrophobic block with a poly(triethylene glycol) block that were copolymerized with an amino acid-functionalized monomer. The block copolymers formed micellar structures in aqueous solutions. An optimized polymer that was functionalized with 6-aminocaproic acid (ACA) possessed pH-sensitive phase transitions at mildly acidic pH and body temperature. Doxorubicin-loaded micelles formed from these polymers were stable at blood pH (~7.4) and showed increased drug release at acidic pH. In addition, these micelles displayed more potent anti-cancer activity than free doxorubicin when tested in a tumor xenograft model in mice.

SUBMITTER: Chen CY 

PROVIDER: S-EPMC3620673 | biostudies-literature | 2013 Jun

REPOSITORIES: biostudies-literature

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pH-dependent, thermosensitive polymeric nanocarriers for drug delivery to solid tumors.

Chen Ching-Yi CY   Kim Tae Hee TH   Wu Wen-Chung WC   Huang Chi-Ming CM   Wei Hua H   Mount Christopher W CW   Tian Yanqing Y   Jang Sei-Hum SH   Pun Suzie H SH   Jen Alex K-Y AK  

Biomaterials 20130315 18


Polymeric micelles are promising carriers for anti-cancer agents due to their small size, ease of assembly, and versatility for functionalization. A current challenge in the use of polymeric micelles is the sensitive balance that must be achieved between stability during prolonged blood circulation and release of active drug at the tumor site. Stimuli-responsive materials provide a mechanism for triggered drug release in the acidic tumor and intracellular microenvironments. In this work, we synt  ...[more]

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