Drug delivery by polymeric micelles: an in vitro and in vivo study to deliver lipophilic substances to colonocytes and selectively target inflamed colon

Abstract Colitis is the term used for chronic inflammatory bowel diseases at substantially increased risk of developing a form of colorectal cancer (CRC) known as colitis-associated cancer. In our study we synthesized core-shell polymeric micelles obtained by self-assembly of block copolymers for hi...

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Veröffentlicht in:Nanomedicine 2013-07, Vol.9 (5), p.675-685
Hauptverfasser: Valerii, Maria Chiara, PhD, Benaglia, Massimo, PhD, Caggiano, Cinzia, Papi, Alessio, PhD, Strillacci, Antonio, PhD, Lazzarini, Giorgia, Campieri, Massimo, MD, Gionchetti, Paolo, MD, Rizzello, Fernando, MD, Spisni, Enzo, PhD
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Sprache:eng
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Zusammenfassung:Abstract Colitis is the term used for chronic inflammatory bowel diseases at substantially increased risk of developing a form of colorectal cancer (CRC) known as colitis-associated cancer. In our study we synthesized core-shell polymeric micelles obtained by self-assembly of block copolymers for high efficiency delivery of anti-inflammatory and anti-cancer compounds to colonocytes and colon mucosa. We achieved an efficient intracellular delivery of these hydrophobic compounds (prednisone, retinoic acid and doxorubicin) to cultured colonocytes without cellular toxicity. The efficacy of retinoic acid and doxorubicin administration was significantly increased using these nanosized carriers. Moreover, these polymeric micelles have been shown to overcome the multidrug resistance efflux mechanism effectively delivering doxorubicin to multidrug-resistant colon cancer cells. These nanocarriers are also suitable for selective in vivo delivery of lipophilic drugs by enema administration to the inflamed colon tissue, specifically targeting the inflamed mucosa. From the Clinical Editor This team of investigators studied polymeric micelles as highly efficient drug delivery systems enabling intracellular delivery of hydrophobic compounds (prednisone, retinoic acid, and doxorubicin) to cultured colonocytes without cellular toxicity, also demonstrating beneficial in vivo effects.
ISSN:1549-9634
1549-9642
DOI:10.1016/j.nano.2012.11.007