Nature Communications (May 2024)

Platform-directed allostery and quaternary structure dynamics of SAMHD1 catalysis

  • Oliver J. Acton,
  • Devon Sheppard,
  • Simone Kunzelmann,
  • Sarah J. Caswell,
  • Andrea Nans,
  • Ailidh J. O. Burgess,
  • Geoff Kelly,
  • Elizabeth R. Morris,
  • Peter B. Rosenthal,
  • Ian A. Taylor

DOI
https://doi.org/10.1038/s41467-024-48237-w
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 16

Abstract

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Abstract SAMHD1 regulates cellular nucleotide homeostasis, controlling dNTP levels by catalysing their hydrolysis into 2’-deoxynucleosides and triphosphate. In differentiated CD4+ macrophage and resting T-cells SAMHD1 activity results in the inhibition of HIV-1 infection through a dNTP blockade. In cancer, SAMHD1 desensitizes cells to nucleoside-analogue chemotherapies. Here we employ time-resolved cryogenic-EM imaging and single-particle analysis to visualise assembly, allostery and catalysis by this multi-subunit enzyme. Our observations reveal how dynamic conformational changes in the SAMHD1 quaternary structure drive the catalytic cycle. We capture five states at high-resolution in a live catalytic reaction, revealing how allosteric activators support assembly of a stable SAMHD1 tetrameric core and how catalysis is driven by the opening and closing of active sites through pairwise coupling of active sites and order-disorder transitions in regulatory domains. This direct visualisation of enzyme catalysis dynamics within an allostery-stabilised platform sets a precedent for mechanistic studies into the regulation of multi-subunit enzymes.