| Literature DB >> 28405617 |
Qian Li1, Xiaoning Han1, Xi Lan1, Yufeng Gao1, Jieru Wan1, Frederick Durham1, Tian Cheng1, Jie Yang1, Zhongyu Wang1, Chao Jiang1, Mingyao Ying2,3, Raymond C Koehler1, Brent R Stockwell4, Jian Wang1.
Abstract
Intracerebral hemorrhage (ICH) causes high mortality and morbidity, but our knowledge of post-ICH neuronal death and related mechanisms is limited. In this study, we first demonstrated that ferroptosis, a newly identified form of cell death, occurs in the collagenase-induced ICH model in mice. We found that administration of ferrostatin-1, a specific inhibitor of ferroptosis, prevented neuronal death and reduced iron deposition induced by hemoglobin in organotypic hippocampal slice cultures (OHSCs). Mice treated with ferrostatin-1 after ICH exhibited marked brain protection and improved neurologic function. Additionally, we found that ferrostatin-1 reduced lipid reactive oxygen species production and attenuated the increased expression level of PTGS2 and its gene product cyclooxygenase-2 ex vivo and in vivo. Moreover, ferrostatin-1 in combination with other inhibitors that target different forms of cell death prevented hemoglobin-induced cell death in OHSCs and human induced pluripotent stem cell-derived neurons better than any inhibitor alone. These results indicate that ferroptosis contributes to neuronal death after ICH, that administration of ferrostatin-1 protects hemorrhagic brain, and that cyclooxygenase-2 could be a biomarker of ferroptosis. The insights gained from this study will advance our knowledge of the post-ICH cell death cascade and be essential for future preclinical studies.Entities:
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Year: 2017 PMID: 28405617 PMCID: PMC5374066 DOI: 10.1172/jci.insight.90777
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708