Neurological phenotype and reduced lifespan in heterozygous Tim23 knockout mice, the first mouse model of defective mitochondrial import

Martin Hrabé de Angelis,Eva Kling,Holger Prokisch,Valérie Gailus-Durner,Ilka Schneider-Lohmar,Thomas Klopstock,Thomas Meitinger,Helmut Fuchs,Wolfgang Wurst,Uwe Ahting,Andreas Bender,Lore Becker,Thomas Floss,Arcangela Iuso,Nikolas Uez

doi:10.1016/j.bbabio.2008.12.001

Neurological phenotype and reduced lifespan in heterozygous Tim23 knockout mice, the first mouse model of defective mitochondrial import

Martin Hrabé de Angelis, Eva Kling + Show 13 more

https://doi.org/10.1016/j.bbabio.2008.12.001

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Journal: BBA - Bioenergetics	Publication Date: Dec 9, 2008
Citations: 60	License type: elsevier-specific: oa user license

Affiliation: Helmholtz Zentrum München, Rechts der Isar Hospital, Ludwig-Maximilians-Universität München

#Mitochondrial Import #Gene Trap Embryonic Stem Cell + Show 8 more

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Abstract

The Tim23 protein is the key component of the mitochondrial import machinery. It locates to the inner mitochondrial membrane and its own import is dependent on the DDP1/TIM13 complex. Mutations in human DDP1 cause the Mohr-Tranebjaerg syndrome (MTS/DFN-1; OMIM #304700), which is one of the two known human diseases of the mitochondrial protein import machinery. We created a Tim23 knockout mouse from a gene trap embryonic stem cell clone. Homozygous Tim23 mice were not viable. Heterozygous F1 mutants showed a 50% reduction of Tim23 protein in Western blot, a neurological phenotype and a markedly reduced life span. Haploinsufficiency of the Tim23 mutation underlines the critical role of the mitochondrial import machinery for maintaining mitochondrial function.

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