Magnetic drug targeting : preclinical in vivo studies, mathematical modeling, and extrapolation to humans

A sound theoretical rationale for the design of a magnetic nanocarrier capable of magnetic capture in vivo after intravenous administration could help elucidate the parameters necessary for in vivo magnetic tumor targeting. In this work, we utilized our long-circulating polymeric magnetic nano carriers, encapsulating increasing amounts of superparamagnetic iron oxide nanoparticles (SPIONs) in a biocompatible oil carrier, to study the effects of SPION loading and of applied magnetic field strength on magnetic tumor targeting in CT26 tumor-bearing mice. Under controlled conditions, the in vivo magnetic targeting was quantified and found to be directly proportional to SPION loading and magnetic field strength. Highest SPION loading, however, resulted in a reduced blood circulation time and a plateauing of the magnetic targeting. Mathematical modeling was undertaken to compute the in vivo magnetic, viscoelastic, convective, and diffusive forces acting on the nanocapsules (NCs) in accordance with the Nacev-Shapiro construct, and this was then used to extrapolate to the expected behavior in humans. The model predicted that in the latter case, the NCs and magnetic forces applied here would have been sufficient to achieve successful targeting in humans. Lastly, an in vivo murine tumor growth delay study was performed using docetaxel (DTX)-encapsulated NCs. Magnetic targeting was found to offer enhanced therapeutic efficacy, and improve mice survival compared to passive targeting at drug doses of ca. 5-8 mg, of DTX/kg. This is,, to our knowledge, the first study that truly bridges the gap between preclinical experiments and clinical translation in the field of magnetic drug targeting.

Language

English

Source (journal)

Nano letters / American Chemical Society. - Washington

Publication

Washington : 2016

ISSN

1530-6984

DOI

10.1021/ACS.NANOLETT.6B02261

Volume/pages

16 :9 (2016) , p. 5652-5660

ISI

000383412100050

Pubmed ID

27541372

Full text (Publisher's DOI)

https://doi.org/10.1021/ACS.NANOLETT.6B02261

Full text (open access)

https://repository.uantwerpen.be/docman/irua/b5c0b5/137136.pdf

Faculty/Department				Faculty of Sciences. Physics

Research group				Electron microscopy for materials research (EMAT)
Publication type				A1 Journal article

Subject				Physics Chemistry Engineering sciences. Technology

Affiliation				Publications with a UAntwerp address

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Identifier

Creation

21.11.2016

Last edited

09.10.2023

To cite this reference

https://hdl.handle.net/10067/1371360151162165141