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A PHGDH inhibitor reveals coordination of serine synthesis and 1-carbon unit fate

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2016

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Pacold, M. E., K. R. Brimacombe, S. H. Chan, J. M. Rohde, C. A. Lewis, L. J. Swier, R. Possemato, et al. 2016. “A PHGDH inhibitor reveals coordination of serine synthesis and 1-carbon unit fate.” Nature chemical biology 12 (6): 452-458. doi:10.1038/nchembio.2070. http://dx.doi.org/10.1038/nchembio.2070.

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Serine is a both a proteinogenic amino acid and the source of one-carbon units essential for de novo purine and deoxythymidine synthesis. In the canonical glucose-derived serine synthesis pathway, Homo sapiens phosphoglycerate dehydrogenase (PHGDH) catalyzes the first, rate-limiting step. Genetic loss of PHGDH is toxic towards PHGDH-overexpressing breast cancer cell lines even in the presence of exogenous serine. Here, we use a quantitative high-throughput screen to identify small molecule PHGDH inhibitors. These compounds reduce the production of glucose-derived serine in cells and suppress the growth of PHGDH-dependent cancer cells in culture and in orthotopic xenograft tumors. Surprisingly, PHGDH inhibition reduced the incorporation into nucleotides of one-carbon units from glucose-derived and exogenous serine. We conclude that glycolytic serine synthesis coordinates the use of one-carbon units from endogenous and exogenous serine in nucleotide synthesis, and suggest that one-carbon unit wasting may contribute to the efficacy of PHGDH inhibitors in vitro and in vivo.

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