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Interaction of PINK1 with nucleotides and kinetin.

Zhong Yan GanSylvie CallegariThanh Ngoc NguyenNicholas S KirkAndrew LeisMichael LazarouGrant DewsonDavid Komander
Published in: Science advances (2024)
The ubiquitin kinase PINK1 accumulates on damaged mitochondria to trigger mitophagy, and PINK1 loss-of-function mutations cause early onset Parkinson's disease. Nucleotide analogs such as kinetin triphosphate (KTP) were reported to enhance PINK1 activity and may represent a therapeutic strategy for the treatment of Parkinson's disease. Here, we investigate the interaction of PINK1 with nucleotides, including KTP. We establish a cryo-EM platform exploiting the dodecamer assembly of Pediculus humanus corporis ( Ph ) PINK1 and determine PINK1 structures bound to AMP-PNP and ADP, revealing conformational changes in the kinase N-lobe that help establish PINK1's ubiquitin binding site. Notably, we find that KTP is unable to bind Ph PINK1 or human ( Hs ) PINK1 due to a steric clash with the kinase "gatekeeper" methionine residue, and mutation to Ala or Gly is required for PINK1 to bind and use KTP as a phosphate donor in ubiquitin phosphorylation and mitophagy. Hs PINK1 M318G can be used to conditionally uncouple PINK1 stabilization and activity on mitochondria.
Keyphrases
  • early onset
  • small molecule
  • endothelial cells
  • late onset
  • tyrosine kinase
  • mass spectrometry
  • single molecule
  • molecular docking
  • molecular dynamics simulations