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  5. Cell Type-Specific Activation of AKT and ERK Signaling Pathways by Small Negatively-Charged Magnetic Nanoparticles
 
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Cell Type-Specific Activation of AKT and ERK Signaling Pathways by Small Negatively-Charged Magnetic Nanoparticles

Author(s)
Rauch, Jens  
Kolch, Walter  
Mahmoudi, Morteza  
Uri
http://hdl.handle.net/10197/5573
Date Issued
2012-11-16
Date Available
2014-05-02T08:39:11Z
Abstract
The interaction of nanoparticles (NPs) with living organisms has become a focus of public and scientific debate due to their potential wide applications in biomedicine, but also because of unwanted side effects. Here, we show that superparamagnetic iron oxide NPs (SPIONs) with different surface coatings can differentially affect signal transduction pathways. Using isogenic pairs of breast and colon derived cell lines we found that the stimulation of ERK and AKT signaling pathways by SPIONs is selectively dependent on the cell type and SPION type. In general, cells with Ras mutations respond better than their non-mutant counterparts. Small negatively charged SPIONs (snSPIONs) activated ERK to a similar extent as epidermal growth factor (EGF), and used the same upstream signaling components including activation of the EGF receptor. Importantly, snSPIONs stimulated the proliferation of Ras transformed breast epithelial cells as efficiently as EGF suggesting that NPs can mimic physiological growth factors.
Other Sponsorship
SFI GrantNo. 06/CE/B1129.
Type of Material
Journal Article
Publisher
Nature Publishing Group
Journal
Scientific Reports
Volume
2
Start Page
868
Copyright (Published Version)
2012 Nature Publishing Group
Subjects

Cancer models

Cell signalling

Nanoparticles

Nanobiotechnology

DOI
10.1038/srep00868
Language
English
Status of Item
Peer reviewed
This item is made available under a Creative Commons License
https://creativecommons.org/licenses/by-nc-nd/3.0/ie/
File(s)
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Paper30.pdf

Size

32.99 MB

Format

Adobe PDF

Checksum (MD5)

f6ea5df16063dc238becada5a886df00

Owning collection
SBI Research Collection
Mapped collections
Conway Institute Research Collection

Item descriptive metadata is released under a CC-0 (public domain) license: https://creativecommons.org/public-domain/cc0/.
All other content is subject to copyright.

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