Different proteolipid protein mutants exhibit unique metabolic defects |
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| Authors: | Maik Hüttemann Zhan Zhang Chadwick Mullins Denise Bessert Icksoo Lee Klaus-Armin Nave Sunita Appikatla Robert P Skoff |
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| Affiliation: | *Center for Molecular Medicine and Genetics, Wayne State University School of Medicine, Detroit, MI 48201, U.S.A.;†Department of Anatomy and Cell Biology, Wayne State University School of Medicine, Detroit, MI 48201, U.S.A.;‡Department of Neurogenetics, Max Planck Institute of Experimental Medicine, Göttingen 37075, Germany |
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| Abstract: | PMD (Pelizaeus–Merzbacher disease), a CNS (central nervous system) disease characterized by shortened lifespan and severe neural dysfunction, is caused by mutations of the PLP1 (X-linked myelin proteolipid protein) gene. The majority of human PLP1 mutations are caused by duplications; almost all others are caused by missense mutations. The cellular events leading to the phenotype are unknown. The same mutations in non-humans make them ideal models to study the mechanisms that cause neurological sequelae. In the present study we show that mice with Plp1 duplications (Plp1tg) have major mitochondrial deficits with a 50% reduction in ATP, a drastically reduced mitochondrial membrane potential and increased numbers of mitochondria. In contrast, the jp (jimpy) mouse with a Plp1 missense mutation exhibits normal mitochondrial function. We show that PLP in the Plp1tg mice and in Plp1-transfected cells is targeted to mitochondria. PLP has motifs permissive for insertion into mitochondria and deletions near its N-terminus prevent its co-localization to mitochondria. These novel data show that Plp1 missense mutations and duplications of the native Plp1 gene initiate uniquely different cellular responses. |
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| Keywords: | mitochondrion, oligodendrocyte, oxidative phosphorylation, Pelizaeus– Merzbacher disease, Plp1 mutant |
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