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Monovalent metal ion binding promotes the first transesterification reaction in the spliceosome.

Jana AupičJure BorišekSebastian M FicaWojciech P GalejAlessandra Magistrato
Published in: Nature communications (2023)
Cleavage and formation of phosphodiester bonds in nucleic acids is accomplished by large cellular machineries composed of both protein and RNA. Long thought to rely on a two-metal-ion mechanism for catalysis, structure comparisons revealed many contain highly spatially conserved second-shell monovalent cations, whose precise function remains elusive. A recent high-resolution structure of the spliceosome, essential for pre-mRNA splicing in eukaryotes, revealed a potassium ion in the active site. Here, we employ biased quantum mechanics/ molecular mechanics molecular dynamics to elucidate the function of this monovalent ion in splicing. We discover that the K + ion regulates the kinetics and thermodynamics of the first splicing step by rigidifying the active site and stabilizing the substrate in the pre- and post-catalytic state via formation of key hydrogen bonds. Our work supports a direct role for the K + ion during catalysis and provides a mechanistic hypothesis likely shared by other nucleic acid processing enzymes.
Keyphrases
  • molecular dynamics
  • nucleic acid
  • high resolution
  • binding protein
  • transcription factor
  • amino acid
  • quantum dots
  • small molecule
  • high speed