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Substrate discrimination among mitogen-activated protein kinases through distinct docking sequence motifs.


ABSTRACT: Mitogen-activated protein kinases (MAPKs) mediate cellular responses to a wide variety of extracellular stimuli. MAPK signal transduction cascades are tightly regulated, and individual MAPKs display exquisite specificity in recognition of their target substrates. All MAPK family members share a common phosphorylation site motif, raising questions as to how substrate specificity is achieved. Here we describe a peptide library screen to identify sequence requirements of the DEF site (docking site for ERK FXF), a docking motif separate from the phosphorylation site. We show that MAPK isoforms recognize DEF sites with unique sequences and identify two key residues on the MAPK that largely dictate sequence specificity. Based on these observations and computational docking studies, we propose a revised model for MAPK interaction with substrates containing DEF sites. Variations in DEF site sequence requirements provide one possible mechanism for encoding complex target specificity among MAPK isoforms.

SUBMITTER: Sheridan DL 

PROVIDER: S-EPMC2443660 | biostudies-literature | 2008 Jul

REPOSITORIES: biostudies-literature

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Substrate discrimination among mitogen-activated protein kinases through distinct docking sequence motifs.

Sheridan Douglas L DL   Kong Yong Y   Parker Sirlester A SA   Dalby Kevin N KN   Turk Benjamin E BE  

The Journal of biological chemistry 20080515 28


Mitogen-activated protein kinases (MAPKs) mediate cellular responses to a wide variety of extracellular stimuli. MAPK signal transduction cascades are tightly regulated, and individual MAPKs display exquisite specificity in recognition of their target substrates. All MAPK family members share a common phosphorylation site motif, raising questions as to how substrate specificity is achieved. Here we describe a peptide library screen to identify sequence requirements of the DEF site (docking site  ...[more]

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