[HTML][HTML] Cancer's sweet tooth
T Bui, CB Thompson - Cancer cell, 2006 - cell.com
T Bui, CB Thompson
Cancer cell, 2006•cell.comEven in the presence of an adequate oxygen supply, many tumors metabolize the majority of
the glucose they take up through glycolysis. It has been a long-held belief that this glycolytic
phenotype is due to cancer-specific defects in mitochondrial oxidative phosphorylation. In
this issue of Cancer Cell, Fantin et al. now report that most tumor cells have a substantial
reserve capacity to produce ATP by oxidative phosphorylation when glycolysis is
suppressed. These new data add to mounting evidence that the high rate of glycolysis …
the glucose they take up through glycolysis. It has been a long-held belief that this glycolytic
phenotype is due to cancer-specific defects in mitochondrial oxidative phosphorylation. In
this issue of Cancer Cell, Fantin et al. now report that most tumor cells have a substantial
reserve capacity to produce ATP by oxidative phosphorylation when glycolysis is
suppressed. These new data add to mounting evidence that the high rate of glycolysis …
Even in the presence of an adequate oxygen supply, many tumors metabolize the majority of the glucose they take up through glycolysis. It has been a long-held belief that this glycolytic phenotype is due to cancer-specific defects in mitochondrial oxidative phosphorylation. In this issue of Cancer Cell, Fantin et al. now report that most tumor cells have a substantial reserve capacity to produce ATP by oxidative phosphorylation when glycolysis is suppressed. These new data add to mounting evidence that the high rate of glycolysis exhibited by most tumors is required to support cell growth rather than to compensate for defect(s) in mitochondrial function.
cell.com