Literature DB >> 26468004

Mitoxantrone-loaded superparamagnetic iron oxide nanoparticles as drug carriers for cancer therapy: Uptake and toxicity in primary human tubular epithelial cells.

Iwona Cicha1, Laura Scheffler2, Astrid Ebenau2, Stefan Lyer1, Christoph Alexiou1, Margarete Goppelt-Struebe2.   

Abstract

Superparamagnetic iron oxide nanoparticles (SPIONs) are in use for many clinical diagnostic and experimental therapeutic applications, for example, for targeted drug delivery. To analyze the cellular responses to mitoxantrone-carrying SPIONs (SPION-MTO), and to the drug released from SPIONs, we used an in vitro system that allows comparison of primary human cells with different endocytotic capacities, namely, epithelial cells from proximal and distal parts of the nephron. SPIONs were selectively and rapidly internalized by proximal tubular cells with high endocytotic potential, but not by distal tubular cells. Uptake did not affect cell viability or morphology. In both cell types, free MTO (10-100 nM) induced double-strand DNA breaks and senescence, cell hypertrophy and reduced cell proliferation. However, cadherin-mediated cell-cell adhesion, cytoskeletal structures or polarity of the cells were not affected. Interestingly, a comparable response was also observed upon treatment with SPION-MTO and was independent of uptake of the particles. The effect of SPION-MTO on cells which did not internalize particles was primarily related to the release of MTO from drug-coated particles upon incubation in serum-containing cell growth medium. In conclusion, we show that whereas the uptake of SPIONs does not affect cellular functions or viability, the toxicity of drug-loaded SPIONs depends essentially on the type of drug bound to nanoparticles. Due to the relatively low systemic toxicity of MTO, the effects of MTO-SPIONs on human tubular cells were moderate, but they may become clinically relevant when more nephrotoxic drugs are bound to SPIONs.

Entities:  

Keywords:  Drug delivery; magnetic nanoparticles; nephrotoxicity; senescence; topoisomerase II

Mesh:

Substances:

Year:  2015        PMID: 26468004     DOI: 10.3109/17435390.2015.1095364

Source DB:  PubMed          Journal:  Nanotoxicology        ISSN: 1743-5390            Impact factor:   5.913


  9 in total

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3.  Manipulation of Schwann cell migration across the astrocyte boundary by polysialyltransferase-loaded superparamagnetic nanoparticles under magnetic field.

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4.  Imaging techniques in nanomedical research.

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5.  Rotating Magnetic Nanoparticle Clusters as Microdevices for Drug Delivery.

Authors:  Alexander J Willis; Sebastian P Pernal; Zachary A Gaertner; Sajani S Lakka; Michael E Sabo; Francis M Creighton; Herbert H Engelhard
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6.  Magnetic Field Promotes Migration of Schwann Cells with Chondroitinase ABC (ChABC)-Loaded Superparamagnetic Nanoparticles Across Astrocyte Boundary in vitro.

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7.  Tissue Plasminogen Activator Binding to Superparamagnetic Iron Oxide Nanoparticle-Covalent Versus Adsorptive Approach.

Authors:  Ralf P Friedrich; Jan Zaloga; Eveline Schreiber; Ildikó Y Tóth; Etelka Tombácz; Stefan Lyer; Christoph Alexiou
Journal:  Nanoscale Res Lett       Date:  2016-06-14       Impact factor: 4.703

Review 8.  Iron Oxide Nanoparticles for Biomedical Applications: A Perspective on Synthesis, Drugs, Antimicrobial Activity, and Toxicity.

Authors:  Laís Salomão Arias; Juliano Pelim Pessan; Ana Paula Miranda Vieira; Taynara Maria Toito de Lima; Alberto Carlos Botazzo Delbem; Douglas Roberto Monteiro
Journal:  Antibiotics (Basel)       Date:  2018-06-09

9.  Inhibition of oxygen-sensing prolyl hydroxylases increases lipid accumulation in human primary tubular epithelial cells without inducing ER stress.

Authors:  Gunnar Schley; Steffen Grampp; Margarete Goppelt-Struebe
Journal:  Cell Tissue Res       Date:  2020-03-18       Impact factor: 5.249

  9 in total

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