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Publication : p53 regulates mitochondrial respiration.

First Author  Matoba S Year  2006
Journal  Science Volume  312
Issue  5780 Pages  1650-3
PubMed ID  16728594 Mgi Jnum  J:109676
Mgi Id  MGI:3629456 Doi  10.1126/science.1126863
Citation  Matoba S, et al. (2006) p53 regulates mitochondrial respiration. Science 312(5780):1650-3
abstractText  The energy that sustains cancer cells is derived preferentially from glycolysis. This metabolic change, the Warburg effect, was one of the first alterations in cancer cells recognized as conferring a survival advantage. Here, we show that p53, one of the most frequently mutated genes in cancers, modulates the balance between the utilization of respiratory and glycolytic pathways. We identify Synthesis of Cytochrome c Oxidase 2 (SCO2) as the downstream mediator of this effect in mice and human cancer cell lines. SCO2 is critical for regulating the cytochrome c oxidase (COX) complex, the major site of oxygen utilization in the eukaryotic cell. Disruption of the SCO2 gene in human cancer cells with wild-type p53 recapitulated the metabolic switch toward glycolysis that is exhibited by p53-deficient cells. That SCO2 couples p53 to mitochondrial respiration provides a possible explanation for the Warburg effect and offers new clues as to how p53 might affect aging and metabolism.
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