Tumor-Specific Endogenous FeII-Activated, MRI-Guided Self-Targeting Gadolinium-Coordinated Theranostic Nanoplatforms for Amplification of ROS and Enhanced Chemodynamic Chemotherapy
2020
Low
drug payload and lack of tumor-targeting for chemodynamic therapy
(CDT) result in an insufficient reactive oxygen species (ROS) generation,
which seriously hinders its further clinical application. Therefore,
how to improve the drug payload and tumor targeting for amplification
of ROS and combine it with chemotherapy has been a huge challenge
in CDT. Herein, methotrexate (MTX), gadolinium (Gd), and artesunate
(ASA) were used as theranostic building blocks to be coordinately
assembled into tumor-specific endogenous FeII-activated
and magnetic resonance imaging (MRI)-guided self-targeting carrier-free
nanoplatforms (NPs) for amplification of ROS and enhanced chemodynamic
chemotherapy. The obtained ASA-MTX-GdIII NPs exhibited
extremely high drug payload (∼96 wt %), excellent physiological
stability, long circulating ability (half-time: ∼12 h), and
outstanding tumor accumulation. Moreover, ASA-MTX-GdIII NPs could be specifically uptaken by tumor cells via folate (FA)
receptors and subsequently be disassembled via lysosomal acidity-induced
coordination breakage, resulting in drug burst release. Most strikingly,
the produced ASA could be catalyzed by tumor-specific overexpressed
endogenous FeII ions to generate sufficient ROS for enhancing
the main chemodynamic efficacy, which could exert a synergistic effect
with the assistant chemotherapy of MTX. Interestingly, ASA-MTX-GdIII NPs caused a lower ROS generation and toxicity on normal
cell lines that seldom expressed endogenous FeII ions.
Under MRI guidance with assistance of self-targeting, significantly
superior synergistic tumor therapy was performed on FA receptor-overexpressed
tumor-bearing mice with a higher ROS generation and an almost complete
elimination of tumor. This work highlights ASA-MTX-GdIII NPs as an efficient chemodynamic-chemotherapeutic agent for MRI
imaging and tumor theranostics.
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