Cystine uptake through the cystine/glutamate antiporter xCT triggers glioblastoma cell death under glucose deprivation

DOI IR (HANDLE) HANDLE Web Site Web Site View 2 Remaining Hide 8 Citations 43 References Open Access

Bibliographic Information

Other Title
  • Cystine uptake through the cystine/glutamine antiporter xCT triggers glioblastoma cell death under glucose deprivation

Description

Oncogenic signaling in cancer cells alters glucose uptake and utilization to supply sufficient energy and biosynthetic intermediates for survival and sustained proliferation. Oncogenic signaling also prevents oxidative stress and cell death caused by increased production of reactive oxygen species. However, elevated glucose metabolism in cancer cells, especially in glioblastoma, results in the cells becoming sensitive to glucose deprivation (i.e. in high glucose dependence), which rapidly induces cell death. However, the precise mechanism of this type of cell death remains unknown. Here, we report that glucose deprivation alone does not trigger glioblastoma cell death. We found that, for cell death to occur in glucose-deprived glioblastoma cells, cystine and glutamine also need to be present in culture media. We observed that cystine uptake through the cystine/glutamate antiporter xCT under glucose deprivation rapidly induces NADPH depletion, reactive oxygen species accumulation, and cell death. We conclude that although cystine uptake is crucial for production of antioxidant glutathione in cancer cells its transport through xCT also induces oxidative stress and cell death in glucose-deprived glioblastoma cells. Combining inhibitors targeting cancer-specific glucose metabolism with cystine and glutamine treatment may offer a therapeutic approach for glioblastoma tumors exhibiting high xCT expression.

Journal

  • Journal of Biological Chemistry

    Journal of Biological Chemistry 292 (48), 19721-19732, 2017-12-01

    American Society for Biochemistry and Molecular Biolog (ASBMB)

Citations (8)*help

See more

References(43)*help

See more

Related Projects

See more

Details 詳細情報について

Report a problem

Back to top