Ultrasmall nanoparticles induce ferroptosis in nutrient-deprived cancer cells and suppress tumour growth

نویسندگان

  • Sung Eun Kim
  • Li Zhang
  • Kai Ma
  • Michelle Riegman
  • Feng Chen
  • Irina Ingold
  • Marcus Conrad
  • Melik Ziya Turker
  • Minghui Gao
  • Xuejun Jiang
  • Sebastien Monette
  • Mohan Pauliah
  • Mithat Gonen
  • Pat Zanzonico
  • Thomas Quinn
  • Ulrich Wiesner
  • Michelle S. Bradbury
  • Michael Overholtzer
چکیده

The design of cancer-targeting particles with precisely tuned physicochemical properties may enhance the delivery of therapeutics and access to pharmacological targets. However, a molecular-level understanding of the interactions driving the fate of nanomedicine in biological systems remains elusive. Here, we show that ultrasmall (<10 nm in diameter) poly(ethylene glycol)-coated silica nanoparticles, functionalized with melanoma-targeting peptides, can induce a form of programmed cell death known as ferroptosis in starved cancer cells and cancer-bearing mice. Tumour xenografts in mice intravenously injected with nanoparticles using a high-dose multiple injection scheme exhibit reduced growth or regression, in a manner that is reversed by the pharmacological inhibitor of ferroptosis, liproxstatin-1. These data demonstrate that ferroptosis can be targeted by ultrasmall silica nanoparticles and may have therapeutic potential.

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عنوان ژورنال:

دوره 11  شماره 

صفحات  -

تاریخ انتشار 2016