4.8 Article

Resonance Energy Transfer-Promoted Photothermal and Photodynamic Performance of Gold- Copper Sulfide Yolk-Shell Nanoparticles for Chemophototherapy of Cancer

Journal

NANO LETTERS
Volume 18, Issue 2, Pages 886-897

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acs.nanolett.7b04162

Keywords

Copper sulfide; yolk-shell nanoparticles; resonance energy transfer; chemophototherapy

Funding

  1. National Natural Science Foundation of China [21573216, 21703232, 21703016, 21777152]
  2. Hundred Talent Program of Chinese Academy of Sciences
  3. Science and Technology Development Project Foundation of Jilin Province [20160101304JC, 20180520145JH]

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Gold (Au) core@void@copper sulfide (CuS) shell (Au-CuS) yolk-shell nanoparticles (YSNPs) were prepared in the present study for potential chemo-, photo-thermal, and photodynamic combination therapy, so-called chemophototherapy. The resonance energy transfer (RET) process was utilized in Au CuS YSNPs to achieve both enhanced photothermal and photodynamic performance compared with those of CuS hollow nanoparticles (HNPs). A series of Au nanomaterials as cores that had different localized surface plasmon resonance (LSPR) absorption peaks at 520, 700, 808, 860, and 980 nm were embedded in CuS HNPs to screen the most effective Au-CuS YSNPs according to the RET process. Thermoresponsive polymer was fabricated on these YSNPs' surface to allow for controlled drug release. AU(808)-CuS and Au-980-CuS YSNPs were found capable of inducing the largest temperature elevation and producing the most significant hydroxyl radicals under 808 and 980 nm laser irradiation, respectively, which could accordingly cause the most severe 4T1 cell injury through oxidative stress mechanism. Moreover, doxorubicin-loaded (Dox-loaded) P(NIPAM-co-AM)-coated Au-980-CuS (p-Au-980-CuS@Dox) YSNPs could more efficiently kill cells than unloaded particles upon 980 nm laser irradiation. After intravenous administration to 4T1 tumor-bearing mice, p-nAu(980)-CuS YSNPs could significantly accumulate in the tumor and effectively inhibit the tumor growth after 980 nm laser irradiation, and p-Au-980-CuS@Dox YSNPs could further potentiate the inhibition efficiency and exhibit excellent in vivo biocompatibility. Taken together, this study sheds light on the rational design of Au CuS YSNPs to offer a promising candidate for chemophototherapy.

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