| Literature DB >> 31056284 |
Ishraq Alim1, Joseph T Caulfield1, Yingxin Chen1, Vivek Swarup2, Daniel H Geschwind3, Elena Ivanova1, Javier Seravalli4, Youxi Ai5, Lauren H Sansing5, Emma J Ste Marie6, Robert J Hondal6, Sushmita Mukherjee7, John W Cave1, Botir T Sagdullaev1, Saravanan S Karuppagounder1, Rajiv R Ratan8.
Abstract
Ferroptosis, a non-apoptotic form of programmed cell death, is triggered by oxidative stress in cancer, heat stress in plants, and hemorrhagic stroke. A homeostatic transcriptional response to ferroptotic stimuli is unknown. We show that neurons respond to ferroptotic stimuli by induction of selenoproteins, including antioxidant glutathione peroxidase 4 (GPX4). Pharmacological selenium (Se) augments GPX4 and other genes in this transcriptional program, the selenome, via coordinated activation of the transcription factors TFAP2c and Sp1 to protect neurons. Remarkably, a single dose of Se delivered into the brain drives antioxidant GPX4 expression, protects neurons, and improves behavior in a hemorrhagic stroke model. Altogether, we show that pharmacological Se supplementation effectively inhibits GPX4-dependent ferroptotic death as well as cell death induced by excitotoxicity or ER stress, which are GPX4 independent. Systemic administration of a brain-penetrant selenopeptide activates homeostatic transcription to inhibit cell death and improves function when delivered after hemorrhagic or ischemic stroke.Entities:
Keywords: GPX4; adaptation; cell death; ferroptosis; intracerebral hemorrhage; selenium; selenoprotein; stroke; therapeutic peptides; transcription
Mesh:
Substances:
Year: 2019 PMID: 31056284 DOI: 10.1016/j.cell.2019.03.032
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582