Zinc Promotes the Death of Hypoxic Astrocytes by Upregulating Hypoxia‐Induced Hypoxia‐Inducible Factor‐1alpha Expression via Poly( ADP ‐ribose) Polymerase‐1

Summary Aim Pathological release of excess zinc ions has been implicated in ischemic brain cell death. However, the underlying mechanisms remain to be elucidated. In stroke, ischemia‐induced zinc release and hypoxia‐inducible factor‐1 ( HIF ‐1) accumulation concurrently occur in the ischemic tissue. The present study tests the hypothesis that the presence of high intracellular zinc concentration is a major cause of modifications to PARP ‐1 and HIF ‐1α during hypoxia, which significantly contributes to cell death during ischemia. Methods Primary cortical astrocytes and C8‐D1A cells were exposed to different concentrations of zinc chloride. Cell death rate and protein expression of HIF ‐1 and Poly( ADP ‐ribose) polymerase ( PARP )‐1 were examined after 3‐h hypoxic treatment. Results Although 3‐h hypoxia or 100 μM of zinc alone did not induce noticeable cytotoxicity, their combination led to a dramatic increase in astrocytic cell death in a zinc‐concentration‐dependent manner. Exposure of astrocytes to hypoxia for 3 h remarkably increased the levels of intracellular zinc and HIF ‐1α protein, which was further augmented by added exogenous zinc. Notably, HIF ‐1α knockdown blocked zinc‐induced astrocyte death. Moreover, knockdown of PARP ‐1, another important protein in the response of hypoxia, attenuated the overexpression of HIF ‐1α and reduced the cell death rate. Conclusions Our studies show that zinc promotes hypoxic cell death through overexpression of the hypoxia response factor HIF ‐1α via the cell fate determine factor PARP ‐1 modification, which provides a novel mechanism for zinc‐mediated ischemic brain injury.