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Structural Basis of Protein Kinase R Autophosphorylation.

Christopher B MayoHeidi ErlandsenDavid J MouserAaron G FeinsteinVictoria L RobinsonEric R MayJames L Cole
Published in: Biochemistry (2019)
The RNA-activated protein kinase, PKR, is a key mediator of the innate immunity response to viral infection. Viral double-stranded RNAs induce PKR dimerization and autophosphorylation. The PKR kinase domain forms a back-to-back dimer. However, intermolecular ( trans) autophosphorylation is not feasible in this arrangement. We have obtained PKR kinase structures that resolves this dilemma. The kinase protomers interact via the known back-to-back interface as well as a front-to-front interface that is formed by exchange of activation segments. Mutational analysis of the front-to-front interface support a functional role in PKR activation. Molecular dynamics simulations reveal that the activation segment is highly dynamic in the front-to-front dimer and can adopt conformations conducive to phosphoryl transfer. We propose a mechanism where back-to-back dimerization induces a conformational change that activates PKR to phosphorylate a "substrate" kinase docked in a front-to-front geometry. This mechanism may be relevant to related kinases that phosphorylate the eukaryotic initiation factor eIF2α.
Keyphrases
  • protein kinase
  • molecular dynamics simulations
  • structural basis
  • molecular docking
  • sars cov
  • molecular dynamics
  • single cell
  • genome wide
  • mass spectrometry
  • drug induced
  • energy transfer