In Vitro Evaluation of Non-Protein Adsorbing Breast Cancer Theranostics Based on 19F-Polymer Containing Nanoparticles
Artikel i vetenskaplig tidskrift, 2013

Eight fluorinated nanoparticles (NPs) are synthesized, loaded with doxorubicin (DOX), and evaluated as theranostic delivery platforms to breast cancer cells. The multifunctional NPs are formed by self-assembly of either linear or star-shaped amphiphilic block copolymers, with fluorinated segments incorporated in the hydrophilic corona of the carrier. The sizes of the NPs confirm that small circular NPs are formed. The release kinetics data of the particles reveals clear hydrophobic core dependence, with longer sustained release from particles with larger hydrophobic cores, suggesting that the DOX release from these carriers can be tailored. Viability assays and flow cytometry evaluation of the ratios of apoptosis/necrosis indicate that the materials are non-toxic to breast cancer cells before DOX loading; however, they are very efficient, similar to free DOX, at killing cancer cells after drug encapsulation. Both flow cytometry and confocal microscopy confirm the cellular uptake of NPs and DOX-NPs into breast cancer cells, and in vitro 19F-MRI measurement shows that the fluorinated NPs have strong imaging signals, qualifying them as a potential in vivo contrast agent for 19F-MRI.

hyperbranched fluoropolymers

copolymer micelles

agent

theranostic nanoparticles

drug delivery

doxorubicin

carriers

doxorubicin

polymers

chemotherapy

tumor-cells

drug-delivery systems

gold nanoparticles

magnetic-resonance

breast cancer

Författare

C. Porsch

Kungliga Tekniska Högskolan (KTH)

Y. N. Zhang

Karolinska Institutet

Åsa Östlund

Chalmers, Kemi- och bioteknik, Teknisk ytkemi

P. Damberg

Karolinska Institutet

C. Ducani

Karolinska Institutet

E. Malmstrom

Kungliga Tekniska Högskolan (KTH)

A. M. Nystrom

Karolinska Institutet

Particle and Particle Systems Characterization

0934-0866 (ISSN) 1521-4117 (eISSN)

Vol. 30 4 381-390

Ämneskategorier

Kemi

DOI

10.1002/ppsc.201300018

Mer information

Senast uppdaterat

2018-02-26