Pannexins in ischemia-induced neurodegeneration

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Abstract

Pannexin 1 (Px1, Panx1) and pannexin 2 (Px2, Panx2) form largepore nonselective channels in the plasma membrane of cells and were suggested to play a role in the pathophysiology of cerebral ischemia. To directly test a potential contribution of pannexins in ischemia-related mechanisms, we performed experiments in Px1 -/-, Px2 -/-, and Px1 -/-Px2 -/- knockout mice. IL-1β release, channel function in astrocytes, and cortical spreading depolarization were not altered in Px1 -/-Px2 -/- mice, indicating that, in contrast to previous concepts, these processes occur normally in the absence of pannexin channels. However, ischemia-induced dye release from cortical neurons was lower, indicating that channel function in Px1 -/-Px2 -/- neurons was impaired. Furthermore, Px1 -/-Px2 -/-mice had a better functional outcome and smaller infarcts than wild-type mice when subjected to ischemic stroke. In conclusion, our data demonstrate that Px1 and Px2 underlie channel function in neurons and contribute to ischemic brain damage.

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APA

Bargiotas, P., Krenz, A., Hormuzdi, S. G., Ridder, D. A., Herb, A., Barakat, W., … Schwaninger, M. (2011). Pannexins in ischemia-induced neurodegeneration. Proceedings of the National Academy of Sciences of the United States of America, 108(51), 20772–20777. https://doi.org/10.1073/pnas.1018262108

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