Molecular responses of cells to 2-mercapto-1-methylimidazole gold nanoparticles (AuNPs)-mmi: investigations of histone methylation changes

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作者
Arianna Polverino
Angela Longo
Aldo Donizetti
Denise Drongitis
Maria Frucci
Loredana Schiavo
Gianfranco Carotenuto
Luigi Nicolais
Marina Piscopo
Emilia Vitale
Laura Fucci
机构
[1] National Research Council (CNR) of Pozzuoli,Institute of Cybernetics
[2] National Research Council (CNR),Institute for Polymers, Composites and Biomaterials
[3] University of Naples Federico II,Department of Biology
[4] University of Naples Federico II,Department of Chemical, Materials and Industrial Engineering DICMAPI
[5] National Research Council (CNR),Institute for High
[6] National Research Council (CNR),Performance Computing and Networking
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Gold nanoparticles (AuNPs); (AuNPs)-mmi; Histone dimethylation; Chromatin;
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摘要
While nanomedicine has an enormous potential to improve the precision of specific therapy, the ability to efficiently deliver these materials to regions of disease in vivo remains limited. In this study, we describe analyses of (AuNPs)-mmi cellular intake via fluorescence microscopy and its effects on H3K4 and H3K9 histone dimethylation. Specifically, we studied the level of H3K4 dimethylation in serving the role of an epigenetic marker of euchromatin, and of H3K9 dimethylation as a marker of transcriptional repression in four different cell lines. We analyzed histone di-methyl-H3K4 and di-methyl-H3K9 using either variable concentrations of nanoparticles or variable time points after cellular uptake. The observed methylation effects decreased consistently with decreasing (AuNPs)-mmi concentrations. Fluorescent microscopy and a binarization algorithm based on a thresholding process with RGB input images demonstrated the continued presence of (AuNPs)-mmi in cells at the lowest concentration used. Furthermore, our results show that the treated cell line used is able to rescue the untreated cell phenotype.
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