| Literature DB >> 27160910 |
Nadine Assmann1, Katja Dettmer1, Johann M B Simbuerger1, Carsten Broeker2, Nadine Nuernberger1, Kathrin Renner3, Holly Courtneidge4, Enriko D Klootwijk4, Axel Duerkop5, Andrew Hall6, Robert Kleta4, Peter J Oefner1, Markus Reichold2, Joerg Reinders7.
Abstract
We recently reported an autosomal dominant form of renal Fanconi syndrome caused by a missense mutation in the third codon of the peroxisomal protein EHHADH. The mutation mistargets EHHADH to mitochondria, thereby impairing mitochondrial energy production and, consequently, reabsorption of electrolytes and low-molecular-weight nutrients in the proximal tubule. Here, we further elucidate the molecular mechanism underlying this pathology. We find that mutated EHHADH is incorporated into mitochondrial trifunctional protein (MTP), thereby disturbing β-oxidation of long-chain fatty acids. The resulting MTP deficiency leads to a characteristic accumulation of hydroxyacyl- and acylcarnitines. Mutated EHHADH also limits respiratory complex I and corresponding supercomplex formation, leading to decreases in oxidative phosphorylation capacity, mitochondrial membrane potential maintenance, and ATP generation. Activity of the Na(+)/K(+)-ATPase is thereby diminished, ultimately decreasing the transport activity of the proximal tubule cells.Entities:
Keywords: Fanconi syndrome; fatty acid oxidation; mitochondriopathy; supercomplexes
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Year: 2016 PMID: 27160910 DOI: 10.1016/j.celrep.2016.04.037
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423