Pkd 1 a Ctivity

نویسندگان

  • Vitalyi O. Rybin
  • Jianfen Guo
  • Erin Harleton
  • Fan Zhang
  • Susan F. Steinberg
چکیده

The canonical pathway for Protein kinase D1 (PKD1) activation by growth factor receptors involves diacylglycerol binding to the C1 domain and protein kinase C-dependent phosphorylation at the activation loop. PKD1 then autophosphorylates at Ser 916 , a modification frequently used as a surrogate marker of PKD1 activity. PKD1 also is cleaved by caspase-3 at a site in the C1-PH interdomain during apoptosis; the functional consequences of this cleavage event remain uncertain. This study shows that PKD11-321 (an N-terminal deletion mutant lacking the C1 domain and flanking sequence that models the catalytic fragment that accumulates during apoptosis) and PKD1-CD (the isolated catalytic domain) display high basal Ser 916 autocatalytic activity and robust activity toward CREBtide (a peptide substrate), but little-to-no activation loop autophosphorylation and no associated activity toward protein substrates such as CREB and cTnI. In contrast, PKD1-PH (a PH domain deletion mutant) is recovered as a constitutively active enzyme, with high basal autocatalytic activity and high basal activity toward peptide and protein substrates. These results indicate that individual regions in the regulatory domain act in a distinct manner to control PKD1 activity. Finally, cellbased studies show that PKD1-1-321 does not substitute for WT-PKD1 as an in vivo activator of CREB and ERK phosphorylation. Proteolytic events that remove the C1 domain (but not the autoinhibitory PH domain) limit maximal PKD1 activity toward physiologically relevant protein substrates and lead to a defect in PKD1-dependent cellular responses.

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تاریخ انتشار 2012