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Synergistic effect of the combination of nanoparticulate Fe(3)O(4) and Au with daunomycin on K562/A02 cells

In this study, we have explored the possibility of the combination of the high reactivity of nano Fe(3)O(4) or Au nanoparticles and daunomycin, one of the most important antitumor drugs in the treatment of acute leukemia clinically, to inhibit MDR of K562/A02 cells. Initially, to determine whether t...

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Autores principales: Chen, Bao-An, Dai, Yong-Yuan, Wang, Xue-Mei, Zhang, Ren-Yun, Xu, Wen-Lin, Shen, Hui-Ling, Gao, Feng, Sun, Qian, Deng, Xiao-Jing, Ding, Jia-hua, Gao, Chong, Sun, Yun-Yu, Cheng, Jian, Wang, Jun, Zhao, Gang, Chen, Ning-Na
Formato: Texto
Lenguaje:English
Publicado: Dove Medical Press 2008
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2626936/
https://www.ncbi.nlm.nih.gov/pubmed/18990943
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author Chen, Bao-An
Dai, Yong-Yuan
Wang, Xue-Mei
Zhang, Ren-Yun
Xu, Wen-Lin
Shen, Hui-Ling
Gao, Feng
Sun, Qian
Deng, Xiao-Jing
Ding, Jia-hua
Gao, Chong
Sun, Yun-Yu
Cheng, Jian
Wang, Jun
Zhao, Gang
Chen, Ning-Na
author_facet Chen, Bao-An
Dai, Yong-Yuan
Wang, Xue-Mei
Zhang, Ren-Yun
Xu, Wen-Lin
Shen, Hui-Ling
Gao, Feng
Sun, Qian
Deng, Xiao-Jing
Ding, Jia-hua
Gao, Chong
Sun, Yun-Yu
Cheng, Jian
Wang, Jun
Zhao, Gang
Chen, Ning-Na
author_sort Chen, Bao-An
collection PubMed
description In this study, we have explored the possibility of the combination of the high reactivity of nano Fe(3)O(4) or Au nanoparticles and daunomycin, one of the most important antitumor drugs in the treatment of acute leukemia clinically, to inhibit MDR of K562/A02 cells. Initially, to determine whether the magnetic nanoparticle Fe(3)O(4) and Au can facilitate the anticancer drug to reverse the resistance of cancer cells, we have explored the cytotoxic effect of daunomycin (DNR) with and without the magnetic nano-Fe(3)O(4) or nano-Au on K562 and K562/A02 cells by MTT assay. Besides, the intracellular DNR concentration and apoptosis of the K562/A02 cells was further investigated by flow cytometry and confocal fluorescence microscopic studies. The MDR1 gene expression of the K562/A02 cells was also studied by RT-PCR method. Our results indicate that 5.0 × 10(−7) M nano-Fe(3)O(4) or 2.0 × 10(−8) M nano-Au is biocompatible and can apparently raise the intracellular DNR accumulation of the K562/A02 cells and increase the apoptosis of tumor cells. Moreover, our observations illustrate that although these two kinds of nanoparticles themselves could not lower the MDR1 gene expression of the K562/A02 cells, yet they could degrade the MDR1 gene level when combining with anticancer drug DNR. This raises the possibility to combine the nano-Fe(3)O(4) or nano-Au with DNR to reverse the drug resistance of K562/A02 cells, which could offer a new strategy for the promising efficient chemotherapy of the leukemia patients.
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spelling pubmed-26269362009-02-18 Synergistic effect of the combination of nanoparticulate Fe(3)O(4) and Au with daunomycin on K562/A02 cells Chen, Bao-An Dai, Yong-Yuan Wang, Xue-Mei Zhang, Ren-Yun Xu, Wen-Lin Shen, Hui-Ling Gao, Feng Sun, Qian Deng, Xiao-Jing Ding, Jia-hua Gao, Chong Sun, Yun-Yu Cheng, Jian Wang, Jun Zhao, Gang Chen, Ning-Na Int J Nanomedicine Original Research In this study, we have explored the possibility of the combination of the high reactivity of nano Fe(3)O(4) or Au nanoparticles and daunomycin, one of the most important antitumor drugs in the treatment of acute leukemia clinically, to inhibit MDR of K562/A02 cells. Initially, to determine whether the magnetic nanoparticle Fe(3)O(4) and Au can facilitate the anticancer drug to reverse the resistance of cancer cells, we have explored the cytotoxic effect of daunomycin (DNR) with and without the magnetic nano-Fe(3)O(4) or nano-Au on K562 and K562/A02 cells by MTT assay. Besides, the intracellular DNR concentration and apoptosis of the K562/A02 cells was further investigated by flow cytometry and confocal fluorescence microscopic studies. The MDR1 gene expression of the K562/A02 cells was also studied by RT-PCR method. Our results indicate that 5.0 × 10(−7) M nano-Fe(3)O(4) or 2.0 × 10(−8) M nano-Au is biocompatible and can apparently raise the intracellular DNR accumulation of the K562/A02 cells and increase the apoptosis of tumor cells. Moreover, our observations illustrate that although these two kinds of nanoparticles themselves could not lower the MDR1 gene expression of the K562/A02 cells, yet they could degrade the MDR1 gene level when combining with anticancer drug DNR. This raises the possibility to combine the nano-Fe(3)O(4) or nano-Au with DNR to reverse the drug resistance of K562/A02 cells, which could offer a new strategy for the promising efficient chemotherapy of the leukemia patients. Dove Medical Press 2008-09 /pmc/articles/PMC2626936/ /pubmed/18990943 Text en © 2008 Dove Medical Press Limited. All rights reserved
spellingShingle Original Research
Chen, Bao-An
Dai, Yong-Yuan
Wang, Xue-Mei
Zhang, Ren-Yun
Xu, Wen-Lin
Shen, Hui-Ling
Gao, Feng
Sun, Qian
Deng, Xiao-Jing
Ding, Jia-hua
Gao, Chong
Sun, Yun-Yu
Cheng, Jian
Wang, Jun
Zhao, Gang
Chen, Ning-Na
Synergistic effect of the combination of nanoparticulate Fe(3)O(4) and Au with daunomycin on K562/A02 cells
title Synergistic effect of the combination of nanoparticulate Fe(3)O(4) and Au with daunomycin on K562/A02 cells
title_full Synergistic effect of the combination of nanoparticulate Fe(3)O(4) and Au with daunomycin on K562/A02 cells
title_fullStr Synergistic effect of the combination of nanoparticulate Fe(3)O(4) and Au with daunomycin on K562/A02 cells
title_full_unstemmed Synergistic effect of the combination of nanoparticulate Fe(3)O(4) and Au with daunomycin on K562/A02 cells
title_short Synergistic effect of the combination of nanoparticulate Fe(3)O(4) and Au with daunomycin on K562/A02 cells
title_sort synergistic effect of the combination of nanoparticulate fe(3)o(4) and au with daunomycin on k562/a02 cells
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2626936/
https://www.ncbi.nlm.nih.gov/pubmed/18990943
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