Mouse mtDNA mutant model of Leber hereditary optic neuropathy

Chun Shi Lin; Mark S. Sharpley; Weiwei Fan; Katrina G. Waymire; Alfredo A. Sadun; Valério Carelli; Fred N. Ross‐Cisneros; Peter Baciu; Eric Sung; Meagan J. McManus; Billy X. Pan; Daniel W. Gil; Grant R. MacGregor; Douglas C. Wallace

doi:10.1073/pnas.1217113109

Mouse mtDNA mutant model of Leber hereditary optic neuropathy

Chun Shi Lin(Children's Hospital of Philadelphia), Mark S. Sharpley(Children's Hospital of Philadelphia), Weiwei Fan(University of California, Irvine), Katrina G. Waymire(University of California, Irvine), Alfredo A. Sadun(University of Southern California), Valério Carelli(University of Southern California), Fred N. Ross‐Cisneros(University of Southern California), Peter Baciu(Allergan (Ireland)), Eric Sung(Allergan (Ireland)), Meagan J. McManus(Children's Hospital of Philadelphia), Billy X. Pan(University of Southern California), Daniel W. Gil(Allergan (Ireland)), Grant R. MacGregor(University of California, Irvine), Douglas C. Wallace(Children's Hospital of Philadelphia)

Proceedings of the National Academy of Sciences

November 5, 2012

10.1073/pnas.1217113109

Cited by 242Open Access

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Abstract

An animal model of Leber hereditary optic neuropathy (LHON) was produced by introducing the human optic atrophy mtDNA ND6 P25L mutation into the mouse. Mice with this mutation exhibited reduction in retinal function by elecroretinogram (ERG), age-related decline in central smaller caliber optic nerve fibers with sparing of larger peripheral fibers, neuronal accumulation of abnormal mitochondria, axonal swelling, and demyelination. Mitochondrial analysis revealed partial complex I and respiration defects and increased reactive oxygen species (ROS) production, whereas synaptosome analysis revealed decreased complex I activity and increased ROS but no diminution of ATP production. Thus, LHON pathophysiology may result from oxidative stress.

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