4.8 Article

Erythrocyte-Membrane-Coated Prussian Blue/Manganese Dioxide Nanoparticles as H2O2-Responsive Oxygen Generators To Enhance Cancer Chemotherapy/Photothermal Therapy

Journal

ACS APPLIED MATERIALS & INTERFACES
Volume 9, Issue 51, Pages 44410-44422

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acsami.7b17022

Keywords

hypoxia; combinational therapy; long circulation; chemotherapy; photothermal therapy

Funding

  1. National Natural Science Fund for Distinguished Young Scholar [NSFC31525009]
  2. National Natural Science Funds [31500809, 31771096]
  3. Luzhou Science and Technology Plan [2013CDLZ-S21]
  4. Sichuan Innovative Research Team Program for Young Scientists [2016TD0004]
  5. Distinguished Young Scholars of Sichuan University [2011SCU04B18]

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Because of the nontargeting release of anticancer drugs, conventional chemotherapy results in serious side effects and poor therapeutic outcomes. In addition, hypoxia situation in the tumor microenvironment also promotes the growth and metastasis of tumors. Multifunctional nanocarriers with stimuli-activation and hypoxia-relieving properties can help overcome some of these limitations. In this study, we have constructed a nanocarrier which is named PBMn DOX@RBC. A Prussian blue/manganese dioxide (PBMn) nanoparticle is used as an oxygen precursor or catalyzer for H2O2 activation, and a red blood cell (RBC) membrane is used to increase the loading capacity of doxorubicin (DOX) and prolong the circulation time in vivo. H2O2 is overproduced in tumor tissues and tumor cells. It can be used as a stimulus to activate drug release. In the presence of H2O2, the hypoxia inside the tumors is relieved by the administration of PBMn DOX@RBC. The generated oxygen disrupts the RBC coated on the surface of PBMn, which accelerates the release of DOX. RBCs also prolong the circulation time of the nanometer system in vivo. By combining the photothermal therapy (PTT) and chemotherapy, the tumor growth inhibition mediated by PBMn DOX@RBC is further enhanced. PBMn DOX@RBC fulfills the demands to relieve tumor hypoxia and enhance cancer chemotherapy/PTT.

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