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Local production of reactive oxygen species drives vincristine-induced axon degeneration

Jorge Gómez-Deza, Anastasia L. Slavutsky, Matthew Nebiyou, Claire E. Le Pichon

2023Cell Death and Disease28 citationsDOIOpen Access PDF

Abstract

Neurological side effects arising from chemotherapy, such as severe pain and cognitive impairment, are a major concern for cancer patients. These major side effects can lead to reduction or termination of chemotherapy medication in patients, negatively impacting their prognoses. With cancer survival rates improving dramatically, addressing side effects of cancer treatment has become pressing. Here, we use iPSC-derived human neurons to investigate the molecular mechanisms that lead to neurotoxicity induced by vincristine, a common chemotherapeutic used to treat solid tumors. Our results uncover a novel mechanism by which vincristine causes a local increase in mitochondrial proteins that produce reactive oxygen species (ROS) in the axon. Vincristine triggers a cascade of axon pathology, causing mitochondrial dysfunction that leads to elevated axonal ROS levels and SARM1-dependent axon degeneration. Importantly, we show that the neurotoxic effect of increased axonal ROS can be mitigated by the small molecule mitochondrial division inhibitor 1 (mdivi-1) and antioxidants glutathione and mitoquinone, identifying a novel therapeutic avenue to treat the neurological effects of chemotherapy.

Topics & Concepts

Reactive oxygen speciesNeurotoxicityVincristineAxonSide effect (computer science)MitochondrionChemotherapyPharmacologyGlutathioneOxidative stressCancer researchBiologyDegeneration (medical)MedicinePathologyNeuroscienceCell biologyInternal medicineToxicityBiochemistryCyclophosphamideEnzymeProgramming languageComputer scienceCancer-related cognitive impairment studiesGlioma Diagnosis and TreatmentBrain Metastases and Treatment
Local production of reactive oxygen species drives vincristine-induced axon degeneration | Litcius