Nanoparticle-induced vascular blockade in human prostate cancer

Author:

Agemy Lilach1,Sugahara Kazuki N.1,Kotamraju Venkata Ramana1,Gujraty Kunal1,Girard Olivier M.2,Kono Yuko2,Mattrey Robert F.2,Park Ji-Ho3,Sailor Michael J.3,Jimenez Ana I.4,Cativiela Carlos4,Zanuy David5,Sayago Francisco J.4,Aleman Carlos5,Nussinov Ruth67,Ruoslahti Erkki18

Affiliation:

1. Vascular Mapping Laboratory, Center for Nanomedicine, Sanford-Burnham Medical Research Institute at the University of California at Santa Barbara (UCSB), Santa Barbara, CA;

2. Department of Radiology, University of California, San Diego, CA;

3. Materials Science and Engineering Program and Department of Chemistry and Biochemistry, University of California, San Diego, La Jolla, CA;

4. Organic Chemistry Department, Instituto de Ciencia de Materiales de Aragon (ICMA), University of Zaragoza–Instituto de Carboquimica (CSIC), Zaragoza, Spain;

5. Department of Chemical Engineering, Escola Técnica Superior d'Enginyers Industrials de Barcelona (ETSEIB), Polytechnic University of Catalonia, Barcelona, Spain;

6. Basic Science Program, Center for Cancer Research Nanobiology Program, SAIC-Frederick, National Cancer Institute, Frederick, MD;

7. Department of Human Genetics, Sackler Medical School, Tel Aviv University, Tel Aviv, Israel; and

8. Cancer Research Center, Sanford-Burnham Medical Research Institute, La Jolla, CA

Abstract

Abstract The tumor-homing pentapeptide CREKA (Cys-Arg-Glu-Lys-Ala) specifically homes to tumors by binding to fibrin and fibrin-associated clotted plasma proteins in tumor vessels. Previous results show that CREKA-coated superparamagnetic iron oxide particles can cause additional clotting in tumor vessels, which creates more binding sites for the peptide. We have used this self-amplifying homing system to develop theranostic nanoparticles that simultaneously serve as an imaging agent and inhibit tumor growth by obstructing tumor circulation through blood clotting. The CREKA nanoparticles were combined with nanoparticles coated with another tumor-homing peptide, CRKDKC, and nanoparticles with an elongated shape (nanoworms) were used for improved binding efficacy. The efficacy of the CREKA peptide was then increased by replacing some residues with nonproteinogenic counterparts, which increased the stability of the peptide in the circulation. Treatment of mice bearing orthotopic human prostate cancer tumors with the targeted nanoworms caused extensive clotting in tumor vessels, whereas no clotting was observed in the vessels of normal tissues. Optical and magnetic resonance imaging confirmed tumor-specific targeting of the nanoworms, and ultrasound imaging showed reduced blood flow in tumor vessels. Treatment of mice with prostate cancer with multiple doses of the nanoworms induced tumor necrosis and a highly significant reduction in tumor growth.

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

Reference34 articles.

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