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[Cancer Research 64, 7668-7672, November 1, 2004]
© 2004 American Association for Cancer Research


Advances in Brief

Nanoparticle-Aptamer Bioconjugates

A New Approach for Targeting Prostate Cancer Cells

Omid C. Farokhzad1,2, Sangyong Jon3, Ali Khademhosseini4, Thanh-Nga T. Tran2, David A. LaVan2 and Robert Langer2,4,5,6

1 Department of Anesthesiology, Brigham and Women’s Hospital, Boston, Massachusetts; 2 Division of Health Sciences and Technology, Massachusetts Institute of Technology, Cambridge, Massachusetts; 3 Department of Life Science, Gwangju Institute of Science & Technology, Gwangju, South Korea; and 4 Division of Biological Engineering, 5 Department of Chemical Engineering, and 6 Center for Cancer Research, Massachusetts Institute of Technology, Cambridge, Massachusetts

Nucleic acid ligands (aptamers) are potentially well suited for the therapeutic targeting of drug encapsulated controlled release polymer particles in a cell- or tissue-specific manner. We synthesized a bioconjugate composed of controlled release polymer nanoparticles and aptamers and examined its efficacy for targeted delivery to prostate cancer cells. Specifically, we synthesized poly(lactic acid)-block-polyethylene glycol (PEG) copolymer with a terminal carboxylic acid functional group (PLA-PEG-COOH), and encapsulated rhodamine-labeled dextran (as a model drug) within PLA-PEG-COOH nanoparticles. These nanoparticles have the following desirable characteristics: (a) negative surface charge (–50 ± 3 mV, mean ± SD, n = 3), which may minimize nonspecific interaction with the negatively charged nucleic acid aptamers; (b) carboxylic acid groups on the particle surface for potential modification and covalent conjugation to amine-modified aptamers; and (c) presence of PEG on particle surface, which enhances circulating half-life while contributing to decreased uptake in nontargeted cells. Next, we generated nanoparticle-aptamer bioconjugates with RNA aptamers that bind to the prostate-specific membrane antigen, a well-known prostate cancer tumor marker that is overexpressed on prostate acinar epithelial cells. We demonstrated that these bioconjugates can efficiently target and get taken up by the prostate LNCaP epithelial cells, which express the prostate-specific membrane antigen protein (77-fold increase in binding versus control, n = 150 cells per group). In contrast to LNCaP cells, the uptake of these particles is not enhanced in cells that do not express the prostate-specific membrane antigen protein. To our knowledge, this represents the first report of targeted drug delivery with nanoparticle-aptamer bioconjugates.




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