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Effect of heme oxygenase-1 on the vulnerability of astrocytes and neurons to hemoglobin
Authors:Chen-Roetling Jing  Regan Raymond F
Affiliation:Thomas Jefferson University, 1020 Sansom Street, Thompson 239, Philadelphia, PA 19107, USA.
Abstract:The heme oxygenase (HO) enzymes catalyze the rate-limiting step of heme breakdown. Prior studies have demonstrated that the vulnerability of neurons and astrocytes to hemoglobin is modified in cells lacking HO-2, the constitutive isoform. The present study assessed the effect of the inducible isoform, HO-1. Wild-type astrocytes treated for 3-5 days with 3-30 microM hemoglobin sustained no loss of viability, as quantified by LDH and MTT assays. The same treatment resulted in death of 25-50% of HO-1 knockout astrocytes, and a 4-fold increase in protein oxidation. Cell injury was attenuated by transfer of the HO-1 gene, but not by bilirubin, the antioxidant heme breakdown product. Conversely, neuronal protein oxidation and cell death after hemoglobin exposure were similar in wild-type and HO-1 knockout cultures. These results suggest that HO-1 induction protects astrocytes from the oxidative toxicity of Hb, but has no effect on neuronal injury.
Keywords:Brain injury   Free radical   Intracerebral hemorrhage   Iron   Oxidative   Stroke   Subarachnoid hemorrhage
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