A Model of a MAPK•Substrate Complex in an Active Conformation: A Computational and Experimental Approach

The mechanisms by which MAP kinases recognize and phosphorylate substrates are not completely understood. Efforts to understand the mechanisms have been compromised by the lack of MAPK-substrate structures. While MAPK-substrate docking is well established as a viable mechanism for bringing MAPKs and...

Descripción completa

Detalles Bibliográficos
Autores principales: Lee, Sunbae, Warthaka, Mangalika, Yan, Chunli, Kaoud, Tamer S., Piserchio, Andrea, Ghose, Ranajeet, Ren, Pengyu, Dalby, Kevin N.
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3073974/
https://www.ncbi.nlm.nih.gov/pubmed/21494553
http://dx.doi.org/10.1371/journal.pone.0018594
_version_ 1782201673982148608
author Lee, Sunbae
Warthaka, Mangalika
Yan, Chunli
Kaoud, Tamer S.
Piserchio, Andrea
Ghose, Ranajeet
Ren, Pengyu
Dalby, Kevin N.
author_facet Lee, Sunbae
Warthaka, Mangalika
Yan, Chunli
Kaoud, Tamer S.
Piserchio, Andrea
Ghose, Ranajeet
Ren, Pengyu
Dalby, Kevin N.
author_sort Lee, Sunbae
collection PubMed
description The mechanisms by which MAP kinases recognize and phosphorylate substrates are not completely understood. Efforts to understand the mechanisms have been compromised by the lack of MAPK-substrate structures. While MAPK-substrate docking is well established as a viable mechanism for bringing MAPKs and substrates into close proximity the molecular details of how such docking promotes phosphorylation is an unresolved issue. In the present study computer modeling approaches, with restraints derived from experimentally known interactions, were used to predict how the N-terminus of Ets-1 associates with ERK2. Interestingly, the N-terminus does not contain a consensus-docking site ((R/K)(2-3)-X(2-6)-Φ(A)-X-Φ(B), where Φ is aliphatic hydrophobic) for ERK2. The modeling predicts that the N-terminus of Ets-1 makes important contributions to the stabilization of the complex, but remains largely disordered. The computer-generated model was used to guide mutagenesis experiments, which support the notion that Leu-11 and possibly Ile-13 and Ile-14 of Ets-1 1-138 (Ets) make contributions through binding to the hydrophobic groove of the ERK2 D-recruiting site (DRS). Based on the modeling, a consensus-docking site was introduced through the introduction of an arginine at residue 7, to give the consensus (7)RK-X(2)-Φ(A)-X-Φ(B) (13). This results in a 2-fold increase in k (cat)/K (m) for the phosphorylation of Ets by ERK2. Similarly, the substitution of the N-terminus for two different consensus docking sites derived from Elk-1 and MKK1 also improves k (cat)/K (m) by two-fold compared to Ets. Disruption of the N-terminal docking through deletion of residues 1-23 of Ets results in a 14-fold decrease in k (cat)/K (m), with little apparent change in k (cat). A peptide that binds to the DRS of ERK2 affects K (m), but not k (cat). Our kinetic analysis suggests that the unstructured N-terminus provides 10-fold uniform stabilization of the ground state ERK2•Ets•MgATP complex and intermediates of the enzymatic reaction.
format Text
id pubmed-3073974
institution National Center for Biotechnology Information
language English
publishDate 2011
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-30739742011-04-14 A Model of a MAPK•Substrate Complex in an Active Conformation: A Computational and Experimental Approach Lee, Sunbae Warthaka, Mangalika Yan, Chunli Kaoud, Tamer S. Piserchio, Andrea Ghose, Ranajeet Ren, Pengyu Dalby, Kevin N. PLoS One Research Article The mechanisms by which MAP kinases recognize and phosphorylate substrates are not completely understood. Efforts to understand the mechanisms have been compromised by the lack of MAPK-substrate structures. While MAPK-substrate docking is well established as a viable mechanism for bringing MAPKs and substrates into close proximity the molecular details of how such docking promotes phosphorylation is an unresolved issue. In the present study computer modeling approaches, with restraints derived from experimentally known interactions, were used to predict how the N-terminus of Ets-1 associates with ERK2. Interestingly, the N-terminus does not contain a consensus-docking site ((R/K)(2-3)-X(2-6)-Φ(A)-X-Φ(B), where Φ is aliphatic hydrophobic) for ERK2. The modeling predicts that the N-terminus of Ets-1 makes important contributions to the stabilization of the complex, but remains largely disordered. The computer-generated model was used to guide mutagenesis experiments, which support the notion that Leu-11 and possibly Ile-13 and Ile-14 of Ets-1 1-138 (Ets) make contributions through binding to the hydrophobic groove of the ERK2 D-recruiting site (DRS). Based on the modeling, a consensus-docking site was introduced through the introduction of an arginine at residue 7, to give the consensus (7)RK-X(2)-Φ(A)-X-Φ(B) (13). This results in a 2-fold increase in k (cat)/K (m) for the phosphorylation of Ets by ERK2. Similarly, the substitution of the N-terminus for two different consensus docking sites derived from Elk-1 and MKK1 also improves k (cat)/K (m) by two-fold compared to Ets. Disruption of the N-terminal docking through deletion of residues 1-23 of Ets results in a 14-fold decrease in k (cat)/K (m), with little apparent change in k (cat). A peptide that binds to the DRS of ERK2 affects K (m), but not k (cat). Our kinetic analysis suggests that the unstructured N-terminus provides 10-fold uniform stabilization of the ground state ERK2•Ets•MgATP complex and intermediates of the enzymatic reaction. Public Library of Science 2011-04-11 /pmc/articles/PMC3073974/ /pubmed/21494553 http://dx.doi.org/10.1371/journal.pone.0018594 Text en Lee et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Lee, Sunbae
Warthaka, Mangalika
Yan, Chunli
Kaoud, Tamer S.
Piserchio, Andrea
Ghose, Ranajeet
Ren, Pengyu
Dalby, Kevin N.
A Model of a MAPK•Substrate Complex in an Active Conformation: A Computational and Experimental Approach
title A Model of a MAPK•Substrate Complex in an Active Conformation: A Computational and Experimental Approach
title_full A Model of a MAPK•Substrate Complex in an Active Conformation: A Computational and Experimental Approach
title_fullStr A Model of a MAPK•Substrate Complex in an Active Conformation: A Computational and Experimental Approach
title_full_unstemmed A Model of a MAPK•Substrate Complex in an Active Conformation: A Computational and Experimental Approach
title_short A Model of a MAPK•Substrate Complex in an Active Conformation: A Computational and Experimental Approach
title_sort model of a mapk•substrate complex in an active conformation: a computational and experimental approach
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3073974/
https://www.ncbi.nlm.nih.gov/pubmed/21494553
http://dx.doi.org/10.1371/journal.pone.0018594
work_keys_str_mv AT leesunbae amodelofamapksubstratecomplexinanactiveconformationacomputationalandexperimentalapproach
AT warthakamangalika amodelofamapksubstratecomplexinanactiveconformationacomputationalandexperimentalapproach
AT yanchunli amodelofamapksubstratecomplexinanactiveconformationacomputationalandexperimentalapproach
AT kaoudtamers amodelofamapksubstratecomplexinanactiveconformationacomputationalandexperimentalapproach
AT piserchioandrea amodelofamapksubstratecomplexinanactiveconformationacomputationalandexperimentalapproach
AT ghoseranajeet amodelofamapksubstratecomplexinanactiveconformationacomputationalandexperimentalapproach
AT renpengyu amodelofamapksubstratecomplexinanactiveconformationacomputationalandexperimentalapproach
AT dalbykevinn amodelofamapksubstratecomplexinanactiveconformationacomputationalandexperimentalapproach
AT leesunbae modelofamapksubstratecomplexinanactiveconformationacomputationalandexperimentalapproach
AT warthakamangalika modelofamapksubstratecomplexinanactiveconformationacomputationalandexperimentalapproach
AT yanchunli modelofamapksubstratecomplexinanactiveconformationacomputationalandexperimentalapproach
AT kaoudtamers modelofamapksubstratecomplexinanactiveconformationacomputationalandexperimentalapproach
AT piserchioandrea modelofamapksubstratecomplexinanactiveconformationacomputationalandexperimentalapproach
AT ghoseranajeet modelofamapksubstratecomplexinanactiveconformationacomputationalandexperimentalapproach
AT renpengyu modelofamapksubstratecomplexinanactiveconformationacomputationalandexperimentalapproach
AT dalbykevinn modelofamapksubstratecomplexinanactiveconformationacomputationalandexperimentalapproach

Ejemplares similares