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Stable nuclear expression of ATP8 and ATP6 genes rescues a mtDNA Complex V null mutant.

Nucleic Acids Res.. 2016-08; 
BoominathanAmutha,VanhoozerShon,BasistyNathan,PowersKathleen,CramptonAlexandra L,WangXiaobin,FriedricksNatalie,SchillingBirgit,BrandMartin D,O'ConnorMatth
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Codon Optimization The ATP8 sequence was taken from mitomap.org, converted into the standard code, and synthesized with some changes to the sequence for codon optimization (Genscript, Piscataway, NJ, USA). Get A Quote

摘要

We explore the possibility of re-engineering mitochondrial genes and expressing them from the nucleus as an approach to rescue defects arising from mitochondrial DNA mutations. We have used a patient cybrid cell line with a single point mutation in the overlap region of the ATP8 and ATP6 genes of the human mitochondrial genome. These cells are null for the ATP8 protein, have significantly lowered ATP6 protein levels and no Complex V function. Nuclear expression of only the ATP8 gene with the ATP5G1 mitochondrial targeting sequence appended restored viability on Krebs cycle substrates and ATP synthesis capabilities but, failed to restore ATP hydrolysis and was insensitive to various inhibitors of oxidative p... More

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