Arsenite-loaded nanoparticles inhibit PARP-1 to overcome multidrug resistance in hepatocellular carcinoma cells

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作者
Hanyu Liu
Zongjun Zhang
Xiaoqin Chi
Zhenghuan Zhao
Dengtong Huang
Jianbin Jin
Jinhao Gao
机构
[1] State Key Laboratory of Physical Chemistry of Solid Surfaces,Department of Chemical Biology
[2] The Key Laboratory for Chemical Biology of Fujian Province,undefined
[3] College of Chemistry and Chemical Engineering,undefined
[4] Xiamen University,undefined
[5] Fujian Provincial Key Laboratory of Chronic Liver Disease and Hepatocellular Carcinoma,undefined
[6] Zhongshan Hospital,undefined
[7] Xiamen University,undefined
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Scientific Reports | / 6卷
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摘要
Hepatocellular carcinoma (HCC) is one of the highest incidences in cancers; however, traditional chemotherapy often suffers from low efficiency caused by drug resistance. Herein, we report an arsenite-loaded dual-drug (doxorubicin and arsenic trioxide, i.e., DOX and ATO) nanomedicine system (FeAsOx@SiO2-DOX, Combo NP) with significant drug synergy and pH-triggered drug release for effective treatment of DOX resistant HCC cells (HuH-7/ADM). This nano-formulation Combo NP exhibits the synergistic effect of DNA damage by DOX along with DNA repair interference by ATO, which results in unprecedented killing efficiency on DOX resistant cancer cells. More importantly, we explored the possible mechanism is that the activity of PARP-1 is inhibited by ATO during the treatment of Combo NP, which finally induces apoptosis of HuH-7/ADM cells by poly (ADP-ribosyl) ation suppression and DNA lesions accumulation. This study provides a smart drug delivery strategy to develop a novel synergistic combination therapy for effectively overcome drug- resistant cancer cells.
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