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Flexible linkers in CaMKII control the balance between activating and inhibitory autophosphorylation

Moitrayee Bhattacharyya, Young Kwang Lee, Serena Muratcioğlu, Baiyu Qiu, Priya Nyayapati, Howard Schulman, Jay T. Groves, John Kuriyan

2020eLife63 citationsDOIOpen Access PDF

Abstract

/calmodulin-dependent protein kinase II (CaMKII) differ in the lengths and sequences of disordered linkers connecting the kinase domains to the oligomeric hubs of the holoenzyme. CaMKII activity depends on the balance between activating and inhibitory autophosphorylation (on Thr 286 and Thr 305/306, respectively, in the human α isoform). Variation in the linkers could alter transphosphorylation rates within a holoenzyme and the balance of autophosphorylation outcomes. We show, using mammalian cell expression and a single-molecule assay, that the balance of autophosphorylation is flipped between CaMKII variants with longer and shorter linkers. For the principal isoforms in the brain, CaMKII-α, with a ~30 residue linker, readily acquires activating autophosphorylation, while CaMKII-β, with a ~200 residue linker, is biased towards inhibitory autophosphorylation. Our results show how the responsiveness of CaMKII holoenzymes to calcium signals can be tuned by varying the relative levels of isoforms with long and short linkers.

Topics & Concepts

AutophosphorylationLinkerGene isoformInhibitory postsynaptic potentialChemistryCell biologyPhosphorylationCalmodulinBiochemistryKinaseBiophysicsProtein kinase ABiologyEnzymeNeuroscienceGeneOperating systemComputer scienceProtein Kinase Regulation and GTPase SignalingMicrotubule and mitosis dynamicsProtein Tyrosine Phosphatases
Flexible linkers in CaMKII control the balance between activating and inhibitory autophosphorylation | Litcius