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The molecular basis of Human FN3K mediated phosphorylation of glycated substrates

Author

Listed:
  • Ankur Garg

    (Cold Spring Harbor
    Cold Spring Harbor)

  • Kin Fan On

    (Cold Spring Harbor
    Cold Spring Harbor)

  • Yang Xiao

    (Memorial Sloan Kettering Cancer Center
    Tri-Institutional PhD Program in Chemical Biology)

  • Elad Elkayam

    (Cold Spring Harbor
    Waltham)

  • Paolo Cifani

    (Cold Spring Harbor)

  • Yael David

    (Memorial Sloan Kettering Cancer Center
    Tri-Institutional PhD Program in Chemical Biology)

  • Leemor Joshua-Tor

    (Cold Spring Harbor
    Cold Spring Harbor)

Abstract

Glycation, a non-enzymatic post-translational modification occurring on proteins, can be actively reversed via site-specific phosphorylation of the fructose-lysine moiety by FN3K kinase, to impact the cellular function of the target protein. A regulatory axis between FN3K and glycated protein targets has been associated with conditions like diabetes and cancer. However, the molecular basis of this relationship has not been explored so far. Here, we determined a series of crystal structures of HsFN3K in the apo-state, and in complex with different nucleotide analogs together with a sugar substrate mimic to reveal the features important for its kinase activity and substrate recognition. Additionally, the dynamics in sugar substrate binding during the kinase catalytic cycle provide important mechanistic insights into HsFN3K function. Our structural work provides the molecular basis for rational small molecule design targeting FN3K.

Suggested Citation

  • Ankur Garg & Kin Fan On & Yang Xiao & Elad Elkayam & Paolo Cifani & Yael David & Leemor Joshua-Tor, 2025. "The molecular basis of Human FN3K mediated phosphorylation of glycated substrates," Nature Communications, Nature, vol. 16(1), pages 1-14, December.
    • Handle: RePEc:nat:natcom:v:16:y:2025:i:1:d:10.1038_s41467-025-56207-z
    DOI: 10.1038/s41467-025-56207-z
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