2-Nitroimidazoles induce mitochondrial stress and ferroptosis in glioma stem cells residing in a hypoxic niche.
Naoyoshi KoikeRyuichi KotaYoshiko NaitoNoriyo HayakawaTomomi MatsuuraTakako HishikiNobuyuki OnishiJunichi FukadaMakoto SuematsuNaoyuki ShigematsuHideyuki SayaOltea SampetreanPublished in: Communications biology (2020)
Under hypoxic conditions, nitroimidazoles can replace oxygen as electron acceptors, thereby enhancing the effects of radiation on malignant cells. These compounds also accumulate in hypoxic cells, where they can act as cytotoxins or imaging agents. However, whether these effects apply to cancer stem cells has not been sufficiently explored. Here we show that the 2-nitroimidazole doranidazole potentiates radiation-induced DNA damage in hypoxic glioma stem cells (GSCs) and confers a significant survival benefit in mice harboring GSC-derived tumors in radiotherapy settings. Furthermore, doranidazole and misonidazole, but not metronidazole, manifested radiation-independent cytotoxicity for hypoxic GSCs that was mediated by ferroptosis induced partially through blockade of mitochondrial complexes I and II and resultant metabolic alterations in oxidative stress responses. Doranidazole also limited the growth of GSC-derived subcutaneous tumors and that of tumors in orthotopic brain slices. Our results thus reveal the theranostic potential of 2-nitroimidazoles as ferroptosis inducers that enable targeting GSCs in their hypoxic niche.
Keyphrases
- radiation induced
- stem cells
- cell death
- induced apoptosis
- dna damage
- oxidative stress
- cell cycle arrest
- radiation therapy
- early stage
- endoplasmic reticulum stress
- photodynamic therapy
- squamous cell carcinoma
- multiple sclerosis
- white matter
- mesenchymal stem cells
- cell therapy
- fluorescence imaging
- endothelial cells
- climate change
- genome wide
- bone marrow
- locally advanced
- skeletal muscle
- free survival
- mass spectrometry