| Literature DB >> 33363457 |
Paul J Derry1, Anh Tran Tram Vo1, Aswini Gnanansekaran1, Joy Mitra2, Anton V Liopo1, Muralidhar L Hegde2, Ah-Lim Tsai3, James M Tour4,5,6, Thomas A Kent1,4,7.
Abstract
Intracerebral hemorrhage (ICH) is a particularly devastating event both because of the direct injury from space-occupying blood to the sequelae of the brain exposed to free blood components from which it is normally protected. Not surprisingly, the usual metabolic and energy pathways are overwhelmed in this situation. In this review article, we detail the complexity of red blood cell degradation, the contribution of eryptosis leading to hemoglobin breakdown into its constituents, the participants in that process, and the points at which injury can be propagated such as elaboration of toxic radicals through the metabolism of the breakdown products. Two prominent products of this breakdown sequence, hemin, and iron, induce a variety of pathologies including free radical damage and DNA breakage, which appear to include events independent from typical oxidative DNA injury. As a result of this confluence of damaging elements, multiple pathways of injury, cell death, and survival are likely engaged including ferroptosis (which may be the same as oxytosis but viewed from a different perspective) and senescence, suggesting that targeting any single cause will likely not be a sufficient strategy to maximally improve outcome. Combination therapies in addition to safe methods to reduce blood burden should be pursued.Entities:
Keywords: ferroptosis; hemoglobin; intracerebral hemorrhage; iron; oxytosis; reactive oxygen species; senescence
Year: 2020 PMID: 33363457 PMCID: PMC7755086 DOI: 10.3389/fncel.2020.603043
Source DB: PubMed Journal: Front Cell Neurosci ISSN: 1662-5102 Impact factor: 5.505