4-in-1 Fe 3 O 4 /g-C 3 N 4 @PPy-DOX nanocomposites: Magnetic targeting guided trimode combinatorial chemotherapy/PDT/PTT for cancer

At present, cancer has become a major disease threatening human health worldwide. Therefore, developing targeting guided multimode synergetic therapy has become one of the hot spots in current antitumor research and is also a great challenge. Herein, a new Fe O /g-C N @PPy-DOX nanocomposite containi...

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Published in:Journal of inorganic biochemistry 2021-02, Vol.215, p.111329
Main Authors: Cheng, Han-Long, Guo, Hai-Ling, Xie, An-Jian, Shen, Yu-Hua, Zhu, Man-Zhou
Format: Article
Language:English
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Summary:At present, cancer has become a major disease threatening human health worldwide. Therefore, developing targeting guided multimode synergetic therapy has become one of the hot spots in current antitumor research and is also a great challenge. Herein, a new Fe O /g-C N @PPy-DOX nanocomposite containing magnetic iron oxide (Fe O ) nanoparticles (NPs), lamellar structure of graphite-like carbon nitride (g-C N ) and polypyrrole (PPy) shell with the loaded anti-tumor drug doxorubicin hydrochloride (DOX) was designed and prepared. The monodisperse Fe O nanoparticles (NPs) with the diameter of 20 nm endowed the nanocomposite with the magnetic targeting ability, reducing damage to normal tissues. It is very interesting that the Fe O NPs also possessed photosensitizer function for photodynamic therapy (PDT). The g-C N sheets as the photocatalysis towards the degradation of water for generating O could effectively improve the hypoxia of solid tumors and increase the efficiency of PDT. In addition, PPy has high light-to-heat conversion efficiency, so was chosen for the cancer photothermal therapy (PTT). Finally, an anticancer drug (DOX) was loaded on the nanocomposite because the presence of mesoporous structure. Thus, the prepared Fe O /g-C N @PPy-DOX nanocomposites exhibit synergetic chemotherapy/PTT/enhanced PDT antitumor effect. This study provides an inspiration for combining targeting and multimodality to improve the anticancer efficiency.
ISSN:1873-3344
DOI:10.1016/j.jinorgbio.2020.111329