Literature DB >> 20411956

Oxidized ultrashort nanotubes as carbon scaffolds for the construction of cell-penetrating NF-kappaB decoy molecules.

Rita Crinelli1, Elisa Carloni, Michele Menotta, Elisa Giacomini, Marzia Bianchi, Gianluca Ambrosi, Luca Giorgi, Mauro Magnani.   

Abstract

Oligonucleotide (ODN) decoys are synthetic ODNs containing the DNA binding sequence of a transcription factor. When delivered to cells, these molecules can compete with endogenous sequences for binding the transcription factor, thus inhibiting its ability to activate the expression of target genes. Modulation of gene expression by decoy ODNs against nuclear factor-kappaB (NF-kappaB), a transcription factor regulating many genes involved in immunity, has been achieved in a variety of immune/inflammatory disorders. However, the successful use of transcription factor decoys depends on an efficient means to bring the synthetic DNA to target cells. It is known that single-walled carbon nanotubes (SWCNTs), under certain conditions, are able to cross the cell membrane. Thus, we have evaluated the possibility to functionalize SWCNTs with decoy ODNs against NF-kappaB in order to improve their intracellular delivery. To couple ODNs to CNTs, we have exploited the carbodiimide chemistry which allows covalent binding of amino-modified ODNs to carboxyl groups introduced onto SWCNTs through oxidation. The effective binding of ODNs to nanotubes has been demonstrated by a combination of microscopic, spectroscopic, and electrophoretic techniques. The uptake and subcellular distribution of ODN decoys bound to SWCNTs was analyzed by fluorescence microscopy. ODNs were internalized into macrophages and accumulated in the cytosol. Moreover, no cytotoxicity associated with SWCNT administration was observed. Finally, NF-kappaB-dependent gene expression was significantly reduced in cells receiving nanomolar concentrations of SWCNT-NF-kappaB decoys compared to cells receiving SWCNTs or SWCNTs functionalized with a nonspecific ODN sequence, demonstrating both efficacy and specificity of the approach.

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Year:  2010        PMID: 20411956     DOI: 10.1021/nn100057c

Source DB:  PubMed          Journal:  ACS Nano        ISSN: 1936-0851            Impact factor:   15.881


  9 in total

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3.  Molecular Dissection of the Human Ubiquitin C Promoter Reveals Heat Shock Element Architectures with Activating and Repressive Functions.

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Review 4.  Carbon nanotubes as cancer therapeutic carriers and mediators.

Authors:  Kuk Hui Son; Jeong Hee Hong; Jin Woo Lee
Journal:  Int J Nanomedicine       Date:  2016-10-07

5.  Selective nuclear localization of siRNA by metallic versus semiconducting single wall carbon nanotubes in keratinocytes.

Authors:  John Torin Huzil; Evi Saliaj; Marina V Ivanova; Marjan Gharagozloo; Maria Jimena Loureiro; Constanze Lamprecht; Andreas Korinek; Ding Wen Chen; Marianna Foldvari
Journal:  Future Sci OA       Date:  2015-11-01

6.  Systematic evaluation of oligodeoxynucleotide binding and hybridization to modified multi-walled carbon nanotubes.

Authors:  Anika Kaufmann; Silke Hampel; Christiane Rieger; David Kunhardt; Darja Schendel; Susanne Füssel; Bernd Schwenzer; Kati Erdmann
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Review 7.  Functionalized carbon nanotubes: biomedical applications.

Authors:  Sandhya Vardharajula; Sk Z Ali; Pooja M Tiwari; Erdal Eroğlu; Komal Vig; Vida A Dennis; Shree R Singh
Journal:  Int J Nanomedicine       Date:  2012-10-09

8.  MAZ-binding G4-decoy with locked nucleic acid and twisted intercalating nucleic acid modifications suppresses KRAS in pancreatic cancer cells and delays tumor growth in mice.

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Journal:  Nucleic Acids Res       Date:  2013-03-06       Impact factor: 16.971

Review 9.  Impact of carbon nanotubes and graphene on immune cells.

Authors:  Marco Orecchioni; Davide Bedognetti; Francesco Sgarrella; Francesco M Marincola; Alberto Bianco; Lucia Gemma Delogu
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  9 in total

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