AI Article Synopsis

  • Ferroptosis is being explored as a novel anticancer strategy that enhances conventional treatments like chemotherapy to address their limitations.
  • A nanoreactor utilizing UV upconversion combines ferroptosis and apoptosis by using a UV-catalyzed Fenton reaction with ferric ammonium citrate and the chemotherapy drug cisplatin to target triple negative breast cancer (TNBC).
  • This innovative approach displayed excellent tumor-fighting capability in a mouse model while showing minimal side effects, indicating its potential for improving TNBC therapy.

Article Abstract

As an emerging anticancer strategy, ferroptosis has recently been developed in combination with current therapeutic modalities to overcome the existing limitations of conventional therapies. Herein, an ultraviolet (UV) upconversion luminescence-fueled nanoreactor is explored to combine ferroptosis and apoptosis through the UV-catalyzed Fenton reaction of an iron supplement (ferric ammonium citrate) loaded in a mesoporous silica layer in addition to the support of a chemotherapeutic agent (cisplatin) attached on the functionalized silica surface for the treatment of triple negative breast cancer (TNBC). The nanoplatform can circumvent the low penetration depth typical of UV light by upconverting near-infrared irradiation and emitting UV photons that convert Fe to Fe to boost the generation of hydroxyl radicals (·OH), causing devastating lipid peroxidation. Apart from DNA damage-induced apoptosis, cisplatin can also catalyze Fenton-based therapy by its abundant production of hydrogen peroxide (HO). As a bioinspired lipid membrane, the folate receptor-targeted liposome as the coating layer offers high biocompatibility and colloidal stability for the upconversion nanoparticles, in addition to prevention of the premature release of encapsulated hydrophilic compounds, before driving the nanoformulation to the target tumor site. As a result, superior antitumor efficacy has been observed in a 4T1 tumor-bearing mouse model with negligible side effects, suggesting that such a nanoformulation could play a pivotal role in effective apoptosis-strengthened ferroptosis TNBC therapy.

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http://dx.doi.org/10.1021/acsnano.2c08706DOI Listing

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