| Literature DB >> 26423448 |
Hui-Teng Cheng1, Chung-Jen Yen2, Chen-Chih Chang3, Kuo-Tong Huang4, Kuo-Hsuan Chen3, Rui-Yang Zhang5, Ping-Yi Lee3, Shi-Chuen Miaw6, Jenq-Wen Huang7, Chih-Kang Chiang8, Kwan-Dun Wu3, Kuan-Yu Hung3.
Abstract
The phenomenon that heme oxygenase-1 (HO-1) protects cell from injury yet its enzymatic product, iron, may facilitate generation of free radical has been long puzzling. Here we establish a functional connection between ferritin heavy chain (FHC) and HO-1. In human lupus nephritis HO-1 and FHC are colocalized within the glomeruli. In rodent anti-Thy1 (thymocyte antigen 1) induced glomerulonephritis, heme oxygenase blockade lowers the expression of FHC and accelerates mesangial cell death. Stimulation of heme oxygenase in cultured rat mesangial cell enhances its resistance to hydrogen peroxide, whereas FHC knockdown by RNA interference compromises this salutary effect. RNA interference of HO-1 makes the cell more susceptible to hydrogen peroxide, which can be rescued by forced expression of wild-type FHC but not mutants that lose the capacity of iron storage and ferroxidase activity. Phosphorylation of JunD was not sustained in these cells. Microarray analysis identifies four candidate transcriptional factors that may regulate the HO-1-induced transcription of FHC. Our results support the role of FHC in neutralizing the iron toxicity as well as mediating the protective effect of HO-1 in response to oxidative stress.Entities:
Keywords: Ferritin heavy chain; Heme oxygenase-1; Inflammation; Oxidative stress
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Year: 2015 PMID: 26423448 DOI: 10.1016/j.bbagen.2015.09.018
Source DB: PubMed Journal: Biochim Biophys Acta ISSN: 0006-3002