Retinal Ganglion Cell Axotomy Induces an Increase in Intracellular Superoxide Anion

doi:10.1167/iovs.05-0921

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(Investigative Ophthalmology and Visual Science. 2006;47:1477-1485.)
© 2006 by The Association for Research in Vision and Ophthalmology, Inc.
DOI: 10.1167/iovs.05-0921

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Retinal Ganglion Cell Axotomy Induces an Increase in Intracellular Superoxide Anion

Christopher J. Lieven, Mark J. Hoegger, Christopher R. Schlieve, and Leonard A. Levin

From the Department of Ophthalmology and Visual Sciences, University of Wisconsin Medical School, Madison, Wisconsin.

PURPOSE. Retinal ganglion cells (RGCs) undergo apoptosis afteraxonal injury. The time course of cell death is variable anddepends in part on the degree of injury sustained. Decreasingreactive oxygen species (ROS) levels or shifting the redox stateto reduction promotes the survival of RGCs in tissue cultureafter axotomy. It was hypothesized that a specific ROS, superoxideanion, acts as an intracellular signaling molecule for RGC deathafter axotomy.

METHODS. Intracellular superoxide levels were measured afterdissociation in retrograde-labeled rat RGCs with use of thesuperoxide-sensitive fluorophores hydroethidium and MitoSOXRed. Having found a significant increase, the effect of axotomywas determined on superoxide levels independent of dissociationwith an optic nerve crush model.

RESULTS. Optic nerve crush caused RGCs to undergo a superoxideburst. The burst was asynchronous and was manifested in onlya fraction of cells at any given time. Neurotrophin deprivationwas not responsible for the superoxide burst because it wasnot prevented by incubation with the neurotrophic factors brain-derivedneurotrophic factor, ciliary neurotrophic factor, forskolin,or insulin. Several inhibitors of intracellular superoxide generationwere studied, but only antimycin A, which inhibits complex IIIof the mitochondrial electron transport chain, blocked the increasein superoxide.

CONCLUSIONS. These findings suggest that superoxide generatedin the mitochondrial electron transport chain could be a parallelsystem to neurotrophic deprivation for signaling cell deathafter axonal injury.

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