Identification and characterization of ERK MAP kinase phosphorylation sites in Smad3.

Matsuura I; Wang G; He D; Liu F

doi:10.1021/bi050560g

Identification and characterization of ERK MAP kinase phosphorylation sites in Smad3.

Matsuura I ¹,

Wang G ,

He D ,

Liu F

Affiliations

1. Center for Advanced Biotechnology and Medicine, Piscataway, New Jersey 08854, USA.
Authors
Matsuura I¹
(1 author)

Biochemistry, 01 Sep 2005, 44(37):12546-12553
https://doi.org/10.1021/bi050560g PMID: 16156666

Abstract

Smad3 is phosphorylated by ERK MAP kinase upon EGF treatment. We have mapped the ERK phosphorylation sites to Ser 207, Ser 203, and Thr 178 in Smad3. We show that, upon EGF treatment, Smad3 is rapidly phosphorylated in these sites, peaking at approximately 15-30 min and that MEK1 inhibitors PD98059 and U0216 inhibit Smad3 phosphorylation induced by EGF. Ser 207 is the best ERK site in Smad3. Its phosphorylation shows the highest EGF induction in Smad3. It is also a very sensitive site to EGF treatment, significantly responding to low concentrations of EGF. These three sites are also phosphorylated by recombinant ERK2 in vitro. We have compared the kinetic parameters of Smad3 with those of ELK1 and MBP for ERK2. We further show that mutation of the ERK phosphorylation sites increases the ability of Smad3 to stimulate a Smad target gene, suggesting that ERK phosphorylation inhibits Smad3 activity.

Full text links

Read article at publisher's site: https://doi.org/10.1021/bi050560g

Citations & impact

Impact metrics

Citations

Jump to Citations

Data citations

Jump to Data

Citations of article over time

Alternative metrics

Altmetric item for https://www.altmetric.com/details/42867247

Altmetric
Discover the attention surrounding your research
https://www.altmetric.com/details/42867247

Smart citations by scite.ai
Explore citation contexts and check if this article has been supported or disputed.
https://scite.ai/reports/10.1021/bi050560g

Supporting

Mentioning

Contrasting

108

Article citations

Targeted dephosphorylation of SMAD3 as an approach to impede TGF-β signaling.
Brewer A, Zhao JF, Fasimoye R, Shpiro N, Macartney TJ, Wood NT, Wightman M, Alessi DR, Sapkota GP
iScience, 27(8):110423, 05 Jul 2024
Cited by: 0 articles | PMID: 39104417 | PMCID: PMC11298613
This article is in the Europe PMC Open access subset. Refer to the copyright information in the article for licensing details.
Free full text in Europe PMC
Alternative splicing in EMT and TGF-β signaling during cancer progression.
Zhang YE, Stuelten CH
Semin Cancer Biol, 101:1-11, 15 Apr 2024
Cited by: 1 article | PMID: 38614376
Review
Cell type-specific transforming growth factor-β (TGF-β) signaling in the regulation of salivary gland fibrosis and regeneration.
Muñoz Forti K, Weisman GA, Jasmer KJ
J Oral Biol Craniofac Res, 14(3):257-272, 21 Mar 2024
Cited by: 0 articles | PMID: 38559587 | PMCID: PMC10979288
This article is in the Europe PMC Open access subset. Refer to the copyright information in the article for licensing details.
Free full text in Europe PMC
Receptor-activated transcription factors and beyond: multiple modes of Smad2/3-dependent transmission of TGF-β signaling.
Miyazawa K, Itoh Y, Fu H, Miyazono K
J Biol Chem, 300(5):107256, 02 Apr 2024
Cited by: 2 articles | PMID: 38569937 | PMCID: PMC11063908
Review
This article is in the Europe PMC Open access subset. Refer to the copyright information in the article for licensing details.
Free full text in Europe PMC
Targeting SMAD-Dependent Signaling: Considerations in Epithelial and Mesenchymal Solid Tumors.
Runa F, Ortiz-Soto G, de Barros NR, Kelber JA
Pharmaceuticals (Basel), 17(3):326, 01 Mar 2024
Cited by: 1 article | PMID: 38543112 | PMCID: PMC10975212
Review
This article is in the Europe PMC Open access subset. Refer to the copyright information in the article for licensing details.
Free full text in Europe PMC

Go to all (85) article citations

Data

Data that cites the article

This data has been provided by curated databases and other sources that have cited the article.

Proteins in UniProt (4)

Mitogen-activated protein kinase 1(UniProt - P28482)
Mothers against decapentaplegic homolog 2(UniProt - Q15796)
Mitogen-activated protein kinase 3(UniProt - P27361)
Mothers against decapentaplegic homolog 3(UniProt - P84022)

GlyGen is an international glycobioinformatics knowledgebase funded by The National Institutes of Health to facilitate glycoscience research by integrating diverse kinds of information, including glycomics, genomics, proteomics (and glycoproteomics), cell biology, developmental biology and biochemistry.

https://www.glygen.org/publication/MED/16156666

Protein post-translational modifications in iPTMnet

http://research.bioinformatics.udel.edu/iptmnet/pmid/16156666/

Funding

Funders who supported this work.

NCI NIH HHS (1)

Grant ID: CA93771
5 publications

Search life-sciences literature (45,103,589 articles, preprints and more)

Identification and characterization of ERK MAP kinase phosphorylation sites in Smad3.

Affiliations

Authors

Abstract

Full text links

Citations & impact

Impact metrics

Citations of article over time

Alternative metrics

Smart citations by scite.ai
Explore citation contexts and check if this article has been supported or disputed.
https://scite.ai/reports/10.1021/bi050560g

Article citations

Targeted dephosphorylation of SMAD3 as an approach to impede TGF-β signaling.

Alternative splicing in EMT and TGF-β signaling during cancer progression.

Cell type-specific transforming growth factor-β (TGF-β) signaling in the regulation of salivary gland fibrosis and regeneration.

Receptor-activated transcription factors and beyond: multiple modes of Smad2/3-dependent transmission of TGF-β signaling.

Targeting SMAD-Dependent Signaling: Considerations in Epithelial and Mesenchymal Solid Tumors.

Data

Data that cites the article

Proteins in UniProt (4)

Protein post-translational modifications in iPTMnet

Similar Articles

Activation of extracellular signal-regulated kinase signaling by epidermal growth factor mediates c-Jun activation and p300 recruitment in keratin 16 gene expression.

Unique role of SNT-2/FRS2beta/FRS3 docking/adaptor protein for negative regulation in EGF receptor tyrosine kinase signaling pathways.

c-Fos accelerates hepatocyte conversion to a fibroblastoid phenotype through ERK-mediated upregulation of paxillin-Serine178 phosphorylation.

The effect of concomitant stimulation with cholecystokinin and epidermal growth factor on extracellular signal-regulated kinase (ERK) activity in pancreatic acinar cells.

Funding

NCI NIH HHS (1)

Partnerships & funding

Search life-sciences literature (45,103,589 articles, preprints and more)

Identification and characterization of ERK MAP kinase phosphorylation sites in Smad3.

Author information

Affiliations

Authors

Abstract

Full text links

Citations & impact

Impact metrics

Citations of article over time

Alternative metrics

Article citations

Data

Data that cites the article

Proteins in UniProt (4)

Protein post-translational modifications in iPTMnet

Similar Articles

Funding

NCI NIH HHS (1)﻿

Partnerships & funding

NCI NIH HHS (1)