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Superparamagnetic Iron Oxide Nanoparticles for Cancer Theranostic Applications

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TLDR
The role of the SPIONs in the formation of the ferrofluids along with their stabilization process via diverse interactions is described and their intrinsic cancer theranostic efficacies might alter due to the differences in their physicochemical/dispersibility/magnetic properties.
Abstract
In the last few decades, superparamagnetic iron oxide nanoparticles (SPIONs—particularly magnetite (Fe3O4)/maghemite (Fe2O3) nanoparticles) have gained a great deal of attention in many biomedical applications, including magnetic targeting based cell isolation/sorting, tissue engineering, gene delivery, and magnetofection, due to their unique magnetic properties, excellent chemical stability, biodegradability, and low toxicity as compared to other magnetic materials (for instance, Co, Mn, and Ni). But recently, SPIONs (in the form of ferrofluids—i.e., SPIONs dispersed in a carrier fluid) have become a highly promising candidate for their use as therapeutic and diagnostic (theranostic) agents in cancer treatment applications such as magnetic fluid hyperthermia (MFH) and magnetic resonance imaging (MRI), respectively. However, the theranostic efficacies of the SPIONs (or ferrofluids) might alter due to the differences in their physicochemical/dispersibility/magnetic properties that are significantly impacted by their synthesis methods and their stabilization process. In this chapter, we have initially discussed the crystal structure/composition and different synthesis methods of the SPIONs. Then, we have described the role of the SPIONs in the formation of the ferrofluids along with their stabilization process via diverse interactions. Finally, we have discussed about their (1) intrinsic cancer theranostic applications of SPIONs such as magnetic fluid hyperthermia, magnetic resonance imaging, and magnetic nanoparticle-based drug delivery and (2) combined cancer theranostics applications including MRI as an adjuvant to fluorescence imaging, thermo-chemotherapy, thermo-radiotherapy, and thermo-immunotherapy.

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References
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Magnetic nanoparticles for precision oncology: theranostic magnetic iron oxide nanoparticles for image-guided and targeted cancer therapy

TL;DR: An overview of the physicochemical properties, toxicity and theranostic applications of MNPs with a focus on magnetic iron oxide nanoparticles is provided.
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AAPM/RSNA physics tutorial for residents: fundamental physics of MR imaging.

TL;DR: Learning the basic concepts required to understand magnetic resonance (MR) imaging is a straightforward process; there are many concepts to learn and retain simultaneously; this situation may give the illusion that learning the physics of MR imaging is complicated.
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Comparison of active, passive and magnetic targeting to tumors of multifunctional paclitaxel/SPIO-loaded nanoparticles for tumor imaging and therapy

TL;DR: It is demonstrated that compared to untargeted or single targeted nanoparticles, the combination of both active strategy and magnetic targeting drastically enhanced nanoparticle accumulation into the tumor tissue with an 8-fold increase compared to passive targeting.
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Antitumor immunity induction by intracellular hyperthermia using magnetite cationic liposomes.

TL;DR: Results suggest that magnetic particles are potentially effective tools for hyperthermic treatment of solid tumors, because in addition to killing of the tumor cells by heat, a host immune response is induced.
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Magnetic nanoparticles as targeted delivery systems in oncology

TL;DR: This work has demonstrated that binding of nucleic acids to magnetic nanoparticles has been demonstrated as a successful non-viral transfection method of different cell lines in vitro and will hopefully become another form of gene delivery for the treatment of cancer.
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