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  4. Effective heating of magnetic nanoparticle aggregates for in vivo nano-theranostic hyperthermia
 
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Effective heating of magnetic nanoparticle aggregates for in vivo nano-theranostic hyperthermia

Journal
International Journal of Nanomedicine
Journal Volume
12
Pages
6273-6287
Date Issued
2017
Author(s)
Wang, C.
Hsu, C.-H.
Li, Z.
Hwang, L.-P.
Lin, Y.-C.  
Chou, P.-T.  
DOI
10.2147/IJN.S141072
URI
https://www.scopus.com/inward/record.uri?eid=2-s2.0-85028594741&doi=10.2147%2fIJN.S141072&partnerID=40&md5=15fd1bd0e39b889193e422745107e26a
https://scholars.lib.ntu.edu.tw/handle/123456789/412019
Abstract
Magnetic resonance (MR) nano-theranostic hyperthermia uses magnetic nanoparticles to target and accumulate at the lesions and generate heat to kill lesion cells directly through hyperthermia or indirectly through thermal activation and control releasing of drugs. Preclinical and translational applications of MR nano-theranostic hyperthermia are currently limited by a few major theoretical difficulties and experimental challenges in in vivo conditions. For example, conventional models for estimating the heat generated and the optimal magnetic nanoparticle sizes for hyperthermia do not accurately reproduce reported in vivo experimental results. In this work, a revised cluster-based model was proposed to predict the specific loss power (SLP) by explicitly considering magnetic nanoparticle aggregation in in vivo conditions. By comparing with the reported experimental results of magnetite Fe3O4 and cobalt ferrite CoFe2O4 magnetic nanoparticles, it is shown that the revised cluster-based model provides a more accurate prediction of the experimental values than the conventional models that assume magnetic nanoparticles act as single units. It also provides a clear physical picture: the aggregation of magnetic nanoparticles increases the cluster magnetic anisotropy while reducing both the cluster domain magnetization and the average magnetic moment, which, in turn, shift the predicted SLP toward a smaller magnetic nanoparticle diameter with lower peak values. As a result, the heating efficiency and the SLP values are decreased. The improvement in the prediction accuracy in in vivo conditions is particularly pronounced when the magnetic nanoparticle diameter is in the range of ~10–20 nm. This happens to be an important size range for MR cancer nano-theranostics, as it exhibits the highest efficacy against both primary and metastatic tumors in vivo. Our studies show that a relatively 20%–25% smaller magnetic nanoparticle diameter should be chosen to reach the maximal heating efficiency in comparison with the optimal size predicted by previous models. ? 2017 Wang et al.
SDGs

[SDGs]SDG3

Other Subjects
cobalt ferrite; ferrite; magnetic nanoparticle; magnetite; monomer; unclassified drug; cobalt; ferric ion; magnetite nanoparticle; accuracy; animal experiment; animal model; animal tissue; anisotropy; Article; cancer tissue; controlled study; heating; human; in vivo study; magnetic resonance nano theranostic hyperthermia; magnetism; male; mouse; nonhuman; pancreas cancer; pancreatic cancer cell line; photon correlation spectroscopy; prediction; thermotherapy; tumor xenograft; animal; chemistry; devices; drug screening; neoplasm; procedures; theoretical model; theranostic nanomedicine; thermotherapy; Animals; Anisotropy; Cobalt; Ferric Compounds; Ferrosoferric Oxide; Humans; Hyperthermia, Induced; Magnetite Nanoparticles; Mice; Models, Theoretical; Neoplasms; Theranostic Nanomedicine; Xenograft Model Antitumor Assays
Type
journal article

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