4.5 Article

Ultrasmall Copper-Gallic Acid Nanodots for Chemodynamic Therapy

期刊

ADVANCED MATERIALS INTERFACES
卷 8, 期 24, 页码 -

出版社

WILEY
DOI: 10.1002/admi.202101173

关键词

chemodynamic therapy; copper-gallic acid polymers; Fenton reaction; glutathione; hydrogen peroxide; reactive oxygen species; tumor

资金

  1. Natural Science Foundation of China [21974018, 22074011, 21727811]
  2. Fundamental Research Funds for the Central Universities [N2005015, N2005027]
  3. Liaoning Revitalization Talents Program [XLYC1907191, XLYC1802016]

向作者/读者索取更多资源

Cu-GA is an ultrasmall chemodynamic therapeutic agent specifically targeting the tumor microenvironment, which enhances treatment efficacy while protecting normal cells. Its small size allows for fast clearance and minimal systemic toxicity, making it a promising option for cancer treatment.
An ultrasmall chemodynamic therapeutic (CDT) agent with favorable specificity to tumor microenvironment, i.e., high level of glutathione (GSH) and hydrogen peroxide (H2O2), is reported. The coordination polymer nanodot between divalent copper (Cu2+) and gallic acid (GA) is shortly named as Cu-GA. The ultrasmall size of Cu-GA (2.16 +/- 0.3 nm) results in a large specific surface area, which is beneficial for improving its catalytic performance. After endocytosis into tumor cell interior, Cu-GA promotes GSH-activated and H2O2-reinforced CDT in situ, wherein divalent Cu(II) is reduced to monovalent Cu(I) by GSH and induced GSH depletion. Subsequently, the generated Cu(I) catalyzes local H2O2 to generate toxic hydroxyl radical (center dot OH) via Fenton-like reaction, and center dot OH leads to tumor cell apoptosis. The higher levels of GSH and H2O2 in the tumor cell interior significantly improve the efficiency of CDT, and meanwhile protect the normal cells. In addition, the ultrasmall size of Cu-GA facilitates its fast clearance and eliminates long-term body retention, with minimized systemic toxicity during the treatment in vivo. Therefore, as a novel copper-based nanoformulation specifically responsive to the tumor microenvironment, Cu-GA provides promising potentials in CDT.

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