4.8 Article

Enhanced Human Epidermal Growth Factor Receptor 2 Degradation in Breast Cancer Cells by Lysosome-Targeting Gold Nanoconstructs

期刊

ACS NANO
卷 9, 期 10, 页码 9859-9867

出版社

AMER CHEMICAL SOC
DOI: 10.1021/acsnano.5b05138

关键词

nanoparticles; targeted drug delivery; gold nanostars; DNA aptamers; lysosomes

资金

  1. Cancer Center Nanotechnology Excellence (CCNE) of the NIH National Cancer Institute at Northwestern University [U54 CA151880]
  2. National Institutes of Health (NIH) Director's Pioneer Award [DP1 EB016540]
  3. H Foundation Cancer Research Fund
  4. Malkin Scholar Award by the Robert H. Lurie Comprehensive Cancer Center at Northwestern University
  5. Post Graduate Program in Cutaneous Biology [NIH T32 AR060710]

向作者/读者索取更多资源

This paper describes how gold nanoparticle nanoconstructs can enhance anticancer effects of lysosomal targeting aptamers in breast cancer cells. Nanoconstructs consisting of anti-HER2 aptamer (human epidermal growth factor receptor 2, HApt) densely grafted on gold nanostars (AuNS) first targeted HER2 and then were internalized via HER2-mediated endocytosis. As incubation time increased, the nanoconstruct complexes were found in vesicular structures, starting from early endosomes to lysosomes as visualized by confocal fluorescence and differential interference contrast microscopy. Within the target organelle, lysosomes, HER2 was degraded by enzymes at low pH, which resulted in apoptosis. At specific time points related to the doubling time of the cancer cells, we found that accumulation of HER2-HApt-AuNS complexes in lysosomes, lysosonnal activity, and lysosomal degradation of HER2 were positively correlated. Increased HER2 degradation by HApt-AuNS triggered cell death and cell cycle arrest in the G0/G1 phase inhibition of cell proliferation. This work shows how a perceived disadvantage of nanoparticle-based therapeutics the inability of nanoconstructs to escape from vesicles and thus induce a biological response can be overcome by both targeting lysosomes and exploiting lysosomal degradation of the biomarkers.

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