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The unique catalytic properties of PSAT1 mediate metabolic adaptation to glutamine blockade.

Yijian QiuOlivia T StamatatosQingting HuJed Ruiter SwainSuzanne RussoAva SannAna S H CostaSara ViolanteDavid L SpectorJustin R CrossMichael J Lukey
Published in: Nature metabolism (2024)
Cultured cancer cells frequently rely on the consumption of glutamine and its subsequent hydrolysis by glutaminase (GLS). However, this metabolic addiction can be lost in the tumour microenvironment, rendering GLS inhibitors ineffective in the clinic. Here we show that glutamine-addicted breast cancer cells adapt to chronic glutamine starvation, or GLS inhibition, via AMPK-mediated upregulation of the serine synthesis pathway (SSP). In this context, the key product of the SSP is not serine, but α-ketoglutarate (α-KG). Mechanistically, we find that phosphoserine aminotransferase 1 (PSAT1) has a unique capacity for sustained α-KG production when glutamate is depleted. Breast cancer cells with resistance to glutamine starvation or GLS inhibition are highly dependent on SSP-supplied α-KG. Accordingly, inhibition of the SSP prevents adaptation to glutamine blockade, resulting in a potent drug synergism that suppresses breast tumour growth. These findings highlight how metabolic redundancy can be context dependent, with the catalytic properties of different metabolic enzymes that act on the same substrate determining which pathways can support tumour growth in a particular nutrient environment. This, in turn, has practical consequences for therapies targeting cancer metabolism.
Keyphrases
  • breast cancer cells
  • stem cells
  • signaling pathway
  • protein kinase
  • papillary thyroid
  • mouse model
  • endothelial cells
  • squamous cell carcinoma
  • cell proliferation
  • squamous cell
  • anti inflammatory