Cell
Volume 153, Issue 4, 9 May 2013, Pages 840-854
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Article
The mTORC1 Pathway Stimulates Glutamine Metabolism and Cell Proliferation by Repressing SIRT4

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Highlights

  • mTORC1 regulates glutamine anaplerosis (catabolism)

  • mTORC1 represses SIRT4 transcription to regulate glutamate dehydrogenase activity

  • SIRT4 represses cell proliferation and is downregulated in human cancer

  • Combined glutamine and glucose metabolism inhibition results in death of cancer cells

Summary

Proliferating mammalian cells use glutamine as a source of nitrogen and as a key anaplerotic source to provide metabolites to the tricarboxylic acid cycle (TCA) for biosynthesis. Recently, mammalian target of rapamycin complex 1 (mTORC1) activation has been correlated with increased nutrient uptake and metabolism, but no molecular connection to glutaminolysis has been reported. Here, we show that mTORC1 promotes glutamine anaplerosis by activating glutamate dehydrogenase (GDH). This regulation requires transcriptional repression of SIRT4, the mitochondrial-localized sirtuin that inhibits GDH. Mechanistically, mTORC1 represses SIRT4 by promoting the proteasome-mediated destabilization of cAMP-responsive element binding 2 (CREB2). Thus, a relationship between mTORC1, SIRT4, and cancer is suggested by our findings. Indeed, SIRT4 expression is reduced in human cancer, and its overexpression reduces cell proliferation, transformation, and tumor development. Finally, our data indicate that targeting nutrient metabolism in energy-addicted cancers with high mTORC1 signaling may be an effective therapeutic approach.

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5

These authors contributed equally to this work

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Present address: Vesalius Research Center, Flemish Institute of Biotechnology (VIB), B 3000 Leuven, Belgium