Accession Number : ADA580311


Title :   M13 Bacteriophage-Polymer Nanoassemblies as Drug Delivery Vehicles


Descriptive Note : Journal article


Corporate Author : SOUTH CAROLINA UNIV COLUMBIA DEPT OF CHEMISTRY AND BIOCHEMISTRY


Personal Author(s) : Suthiwangcharoen, Nisaraporn ; Li, Tao ; Li, Kai ; Thompson, Preston ; You, Shaojin ; Wang, Qian


Full Text : https://apps.dtic.mil/dtic/tr/fulltext/u2/a580311.pdf


Report Date : Jan 2011


Pagination or Media Count : 14


Abstract : Poly(caprolactone-b-2-vinylpyridine) (PCL P2VP) coated with folate-conjugated M13 (FA M13) provides a nanosized delivery system which is capable of encapsulating hydrophobic antitumor drugs such as doxorubicin (DOX). The DOX-loaded FA M13 PCL P2VP assemblies had an average diameter of approximately 200 nm and their structure was characterized using transmission electron microscopy, scanning electron microscopy, and dynamic light scattering. The particles were stable at physiological pH but could be degraded at a lower pH. The release of DOX from the nanoassemblies under acidic conditions was shown to be significantly faster than that observed at physiological pH. In addition, the DOX-loaded FA M13 PCL P2VP particles showed a distinctly greater cellular uptake and cytotoxicity against folate-receptor-positive cancer cells than folatereceptor- negative cells, indicating that the receptor facilitates folate uptake via receptor-mediated endocytosis. Furthermore, the DOX-loaded particles also had a significantly higher tumor uptake and selectivity compared to free DOX. This study therefore offers a new way to fabricate nanosized drug delivery vehicles.


Descriptors :   *DRUGS , *NANOTECHNOLOGY , *POLYMERS , ACETONES , CELLS(BIOLOGY) , CYTOTOXINS , IN VITRO ANALYSIS , PH FACTOR , PYRIDINES


Subject Categories : Pharmacology
      Polymer Chemistry


Distribution Statement : APPROVED FOR PUBLIC RELEASE