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  • Structural and Dynamic Features of F-recruitment Site Driven Substrate Phosphorylation by ERK2.

Structural and Dynamic Features of F-recruitment Site Driven Substrate Phosphorylation by ERK2.

Scientific reports (2015-06-09)
Andrea Piserchio, Venkatesh Ramakrishan, Hsin Wang, Tamer S Kaoud, Boris Arshava, Kaushik Dutta, Kevin N Dalby, Ranajeet Ghose
ABSTRACT

The F-recruitment site (FRS) of active ERK2 binds F-site (Phe-x-Phe-Pro) sequences found downstream of the Ser/Thr phospho-acceptor on cellular substrates. Here we apply NMR methods to analyze the interaction between active ERK2 (ppERK2), and a 13-residue F-site-bearing peptide substrate derived from its cellular target, the transcription factor Elk-1. Our results provide detailed insight into previously elusive structural and dynamic features of FRS/F-site interactions and FRS-driven substrate phosphorylation. We show that substrate F-site engagement significantly quenches slow dynamics involving the ppERK2 activation-loop and the FRS. We also demonstrate that the F-site phenylalanines make critical contacts with ppERK2, in contrast to the proline whose cis-trans isomerization has no significant effect on F-site recognition by the kinase FRS. Our results support a mechanism where phosphorylation of the disordered N-terminal phospho-acceptor is facilitated by its increased productive encounters with the ppERK2 active site due to docking of the proximal F-site at the kinase FRS.

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