4.8 Article

Mammals divert endogenous genotoxic formaldehyde into one-carbon metabolism

Journal

NATURE
Volume 548, Issue 7669, Pages 549-+

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/nature23481

Keywords

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Funding

  1. CRUK Cambridge Cancer Centre studentship
  2. Wellcome Trust
  3. Children With Cancer
  4. CRUK
  5. European Union (FEDER) [BFU2013-42918-P, AES15/01409 (CP12/03273)]
  6. NIH [GM 79465, ES004705]
  7. Chemical Biology Training Grant from the NIH [T32 GM066698]
  8. MRC
  9. EPSRC
  10. CRUK [C596/A21140, C596/A18076]
  11. DFG Fellowship [ME 4636/2-1]
  12. Medical Research Council
  13. [RYC-2015-18670]
  14. Wellcome Trust [106202/Z/14/Z] Funding Source: Wellcome Trust
  15. MRC [MC_U105178811] Funding Source: UKRI
  16. Cancer Research UK [23273] Funding Source: researchfish
  17. Cancer Research UK
  18. Versus Arthritis [21140] Funding Source: researchfish
  19. Medical Research Council [MC_U105178811] Funding Source: researchfish
  20. Wellcome Trust [106202/Z/14/Z] Funding Source: researchfish

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The folate-driven one-carbon (1C) cycle is a fundamental metabolic hub in cells that enables the synthesis of nucleotides and amino acids and epigenetic modifications. This cycle might also release formaldehyde, a potent protein and DNA crosslinking agent that organisms produce in substantial quantities. Here we show that supplementation with tetrahydrofolate, the essential cofactor of this cycle, and other oxidation-prone folate derivatives kills human, mouse and chicken cells that cannot detoxify formaldehyde or that lack DNA crosslink repair. Notably, formaldehyde is generated from oxidative decomposition of the folate backbone. Furthermore, we find that formaldehyde detoxification in human cells generates formate, and thereby promotes nucleotide synthesis. This supply of 1C units is sufficient to sustain the growth of cells that are unable to use serine, which is the predominant source of 1C units. These findings identify an unexpected source of formaldehyde and, more generally, indicate that the detoxification of this ubiquitous endogenous genotoxin creates a benign 1C unit that can sustain essential metabolism.

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