An S/T-Q cluster domain census unveils new putative targets under Tel1/Mec1 control

Hannah C. Cheung; F. Anthony San Lucas; Stephanie Hicks; Kyle Chang; Alison A. Bertuch; Albert Ribes-Zamora

doi:10.1186/1471-2164-13-664

An S/T-Q cluster domain census unveils new putative targets under Tel1/Mec1 control

Hannah C. Cheung, F. Anthony San Lucas, Stephanie Hicks, Kyle Chang, Alison A. Bertuch, Albert Ribes-Zamora

Translational Molecular Pathology

Research output: Contribution to journal › Article › peer-review

12 Scopus citations

Abstract

Background: The cellular response to DNA damage is immediate and highly coordinated in order to maintain genome integrity and proper cell division. During the DNA damage response (DDR), the sensor kinases Tel1 and Mec1 in Saccharomyces cerevisiae and ATM and ATR in human, phosphorylate multiple mediators which activate effector proteins to initiate cell cycle checkpoints and DNA repair. A subset of kinase substrates are recognized by the S/T-Q cluster domain (SCD), which contains motifs of serine (S) or threonine (T) followed by a glutamine (Q). However, the full repertoire of proteins and pathways controlled by Tel1 and Mec1 is unknown.Results: To identify all putative SCD-containing proteins, we analyzed the distribution of S/T-Q motifs within verified Tel1/Mec1 targets and arrived at a unifying SCD definition of at least 3 S/T-Q within a stretch of 50 residues. This new SCD definition was used in a custom bioinformatics pipeline to generate a census of SCD-containing proteins in both yeast and human. In yeast, 436 proteins were identified, a significantly larger number of hits than were expected by chance. These SCD-containing proteins did not distribute equally across GO-ontology terms, but were significantly enriched for those involved in processes related to the DDR. We also found a significant enrichment of proteins involved in telophase and cytokinesis, protein transport and endocytosis suggesting possible novel Tel1/Mec1 targets in these pathways. In the human proteome, a wide range of similar proteins were identified, including homologs of some SCD-containing proteins found in yeast. This list also included high concentrations of proteins in the Mediator, spindle pole body/centrosome and actin cytoskeleton complexes.Conclusions: Using a bioinformatic approach, we have generated a census of SCD-containing proteins that are involved not only in known DDR pathways but several other pathways under Tel1/Mec1 control suggesting new putative targets for these kinases.

Original language	English (US)
Article number	664
Journal	BMC genomics
Volume	13
Issue number	1
DOIs	https://doi.org/10.1186/1471-2164-13-664
State	Published - Nov 23 2012

Keywords

ATM
ATR
DNA damage response
Phosphorylation
Proteome
Tel1/Mec1

ASJC Scopus subject areas

Biotechnology
Genetics

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10.1186/1471-2164-13-664

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title = "An S/T-Q cluster domain census unveils new putative targets under Tel1/Mec1 control",

abstract = "Background: The cellular response to DNA damage is immediate and highly coordinated in order to maintain genome integrity and proper cell division. During the DNA damage response (DDR), the sensor kinases Tel1 and Mec1 in Saccharomyces cerevisiae and ATM and ATR in human, phosphorylate multiple mediators which activate effector proteins to initiate cell cycle checkpoints and DNA repair. A subset of kinase substrates are recognized by the S/T-Q cluster domain (SCD), which contains motifs of serine (S) or threonine (T) followed by a glutamine (Q). However, the full repertoire of proteins and pathways controlled by Tel1 and Mec1 is unknown.Results: To identify all putative SCD-containing proteins, we analyzed the distribution of S/T-Q motifs within verified Tel1/Mec1 targets and arrived at a unifying SCD definition of at least 3 S/T-Q within a stretch of 50 residues. This new SCD definition was used in a custom bioinformatics pipeline to generate a census of SCD-containing proteins in both yeast and human. In yeast, 436 proteins were identified, a significantly larger number of hits than were expected by chance. These SCD-containing proteins did not distribute equally across GO-ontology terms, but were significantly enriched for those involved in processes related to the DDR. We also found a significant enrichment of proteins involved in telophase and cytokinesis, protein transport and endocytosis suggesting possible novel Tel1/Mec1 targets in these pathways. In the human proteome, a wide range of similar proteins were identified, including homologs of some SCD-containing proteins found in yeast. This list also included high concentrations of proteins in the Mediator, spindle pole body/centrosome and actin cytoskeleton complexes.Conclusions: Using a bioinformatic approach, we have generated a census of SCD-containing proteins that are involved not only in known DDR pathways but several other pathways under Tel1/Mec1 control suggesting new putative targets for these kinases.",

keywords = "ATM, ATR, DNA damage response, Phosphorylation, Proteome, Tel1/Mec1",

author = "Cheung, {Hannah C.} and {San Lucas}, {F. Anthony} and Stephanie Hicks and Kyle Chang and Bertuch, {Alison A.} and Albert Ribes-Zamora",

note = "Funding Information: This project was initiated through a class assignment for the Bioinformatics and Genomic Analysis class given at the Baylor College of Medicine Graduate School of Biomedical Sciences led by Dr. Kimberly C. Worley. HCC was supported by the Early Career Award from the Thrasher Research Fund. FASL was supported by the Schissler Foundation. HCC and SH was supported through RP10189 to Dr. Sharon Plon from the Cancer Prevention Research Institute of Texas and SH was additionally supported by NCI T32 training grant CA096520. AB was supported by NIH grant R01 GM077509. AR-Z was supported by the IRACDA grant K12 GM84897.",

year = "2012",

month = nov,

day = "23",

doi = "10.1186/1471-2164-13-664",

language = "English (US)",

volume = "13",

journal = "BMC genomics",

issn = "1471-2164",

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T1 - An S/T-Q cluster domain census unveils new putative targets under Tel1/Mec1 control

AU - Cheung, Hannah C.

AU - San Lucas, F. Anthony

AU - Hicks, Stephanie

AU - Chang, Kyle

AU - Bertuch, Alison A.

AU - Ribes-Zamora, Albert

N1 - Funding Information: This project was initiated through a class assignment for the Bioinformatics and Genomic Analysis class given at the Baylor College of Medicine Graduate School of Biomedical Sciences led by Dr. Kimberly C. Worley. HCC was supported by the Early Career Award from the Thrasher Research Fund. FASL was supported by the Schissler Foundation. HCC and SH was supported through RP10189 to Dr. Sharon Plon from the Cancer Prevention Research Institute of Texas and SH was additionally supported by NCI T32 training grant CA096520. AB was supported by NIH grant R01 GM077509. AR-Z was supported by the IRACDA grant K12 GM84897.

PY - 2012/11/23

Y1 - 2012/11/23

N2 - Background: The cellular response to DNA damage is immediate and highly coordinated in order to maintain genome integrity and proper cell division. During the DNA damage response (DDR), the sensor kinases Tel1 and Mec1 in Saccharomyces cerevisiae and ATM and ATR in human, phosphorylate multiple mediators which activate effector proteins to initiate cell cycle checkpoints and DNA repair. A subset of kinase substrates are recognized by the S/T-Q cluster domain (SCD), which contains motifs of serine (S) or threonine (T) followed by a glutamine (Q). However, the full repertoire of proteins and pathways controlled by Tel1 and Mec1 is unknown.Results: To identify all putative SCD-containing proteins, we analyzed the distribution of S/T-Q motifs within verified Tel1/Mec1 targets and arrived at a unifying SCD definition of at least 3 S/T-Q within a stretch of 50 residues. This new SCD definition was used in a custom bioinformatics pipeline to generate a census of SCD-containing proteins in both yeast and human. In yeast, 436 proteins were identified, a significantly larger number of hits than were expected by chance. These SCD-containing proteins did not distribute equally across GO-ontology terms, but were significantly enriched for those involved in processes related to the DDR. We also found a significant enrichment of proteins involved in telophase and cytokinesis, protein transport and endocytosis suggesting possible novel Tel1/Mec1 targets in these pathways. In the human proteome, a wide range of similar proteins were identified, including homologs of some SCD-containing proteins found in yeast. This list also included high concentrations of proteins in the Mediator, spindle pole body/centrosome and actin cytoskeleton complexes.Conclusions: Using a bioinformatic approach, we have generated a census of SCD-containing proteins that are involved not only in known DDR pathways but several other pathways under Tel1/Mec1 control suggesting new putative targets for these kinases.

AB - Background: The cellular response to DNA damage is immediate and highly coordinated in order to maintain genome integrity and proper cell division. During the DNA damage response (DDR), the sensor kinases Tel1 and Mec1 in Saccharomyces cerevisiae and ATM and ATR in human, phosphorylate multiple mediators which activate effector proteins to initiate cell cycle checkpoints and DNA repair. A subset of kinase substrates are recognized by the S/T-Q cluster domain (SCD), which contains motifs of serine (S) or threonine (T) followed by a glutamine (Q). However, the full repertoire of proteins and pathways controlled by Tel1 and Mec1 is unknown.Results: To identify all putative SCD-containing proteins, we analyzed the distribution of S/T-Q motifs within verified Tel1/Mec1 targets and arrived at a unifying SCD definition of at least 3 S/T-Q within a stretch of 50 residues. This new SCD definition was used in a custom bioinformatics pipeline to generate a census of SCD-containing proteins in both yeast and human. In yeast, 436 proteins were identified, a significantly larger number of hits than were expected by chance. These SCD-containing proteins did not distribute equally across GO-ontology terms, but were significantly enriched for those involved in processes related to the DDR. We also found a significant enrichment of proteins involved in telophase and cytokinesis, protein transport and endocytosis suggesting possible novel Tel1/Mec1 targets in these pathways. In the human proteome, a wide range of similar proteins were identified, including homologs of some SCD-containing proteins found in yeast. This list also included high concentrations of proteins in the Mediator, spindle pole body/centrosome and actin cytoskeleton complexes.Conclusions: Using a bioinformatic approach, we have generated a census of SCD-containing proteins that are involved not only in known DDR pathways but several other pathways under Tel1/Mec1 control suggesting new putative targets for these kinases.

KW - ATM

KW - ATR

KW - DNA damage response

KW - Phosphorylation

KW - Proteome

KW - Tel1/Mec1

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An S/T-Q cluster domain census unveils new putative targets under Tel1/Mec1 control

Abstract

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