Rad17 Phosphorylation Is Required for Claspin Recruitment and Chk1 Activation in Response to Replication Stress

Xin Wang; Lee Zou; Tao Lu; Shilai Bao; Kristen E. Hurov; Walter N. Hittelman; Stephen J. Elledge; Lei Li

doi:10.1016/j.molcel.2006.06.022

Rad17 Phosphorylation Is Required for Claspin Recruitment and Chk1 Activation in Response to Replication Stress

Xin Wang, Lee Zou, Tao Lu, Shilai Bao, Kristen E. Hurov, Walter N. Hittelman, Stephen J. Elledge, Lei Li

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

107 Scopus citations

Abstract

The ATR-mediated checkpoint is not only critical for responding to genotoxic stress but also essential for cell proliferation. The RFC-related checkpoint protein Rad17, a phosphorylation substrate of ATR, is critical for ATR-mediated checkpoint signaling and cell survival. Here, we show that phosphorylation of Rad17 by ATR is important for genomic stability and restraint of S phase but is not essential for cell survival. The phosphomutant Rad17AA exhibits distinct defects in hydroxyurea- (HU) and ultraviolet- (UV) induced Chk1 activation, indicating that separate Rad17 functions are required differently in response to different types of replication interference. Although cells expressing Rad17AA can initiate Chk1 phosphorylation after HU treatment, they fail to sustain Chk1 phosphorylation after withdrawal of HU and are profoundly sensitive to HU. Importantly, we found that phosphorylated Rad17 interacts with Claspin and regulates its phosphorylation. These findings reveal a phosphorylation-dependent function of Rad17 in an ATR-Rad17-Claspin-Chk1-signaling cascade that responds to specific replication stress.

Original language	English (US)
Pages (from-to)	331-341
Number of pages	11
Journal	Molecular cell
Volume	23
Issue number	3
DOIs	https://doi.org/10.1016/j.molcel.2006.06.022
State	Published - Aug 4 2006

Keywords

CELLCYCLE
DNA

ASJC Scopus subject areas

Molecular Biology
Cell Biology

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10.1016/j.molcel.2006.06.022

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title = "Rad17 Phosphorylation Is Required for Claspin Recruitment and Chk1 Activation in Response to Replication Stress",

abstract = "The ATR-mediated checkpoint is not only critical for responding to genotoxic stress but also essential for cell proliferation. The RFC-related checkpoint protein Rad17, a phosphorylation substrate of ATR, is critical for ATR-mediated checkpoint signaling and cell survival. Here, we show that phosphorylation of Rad17 by ATR is important for genomic stability and restraint of S phase but is not essential for cell survival. The phosphomutant Rad17AA exhibits distinct defects in hydroxyurea- (HU) and ultraviolet- (UV) induced Chk1 activation, indicating that separate Rad17 functions are required differently in response to different types of replication interference. Although cells expressing Rad17AA can initiate Chk1 phosphorylation after HU treatment, they fail to sustain Chk1 phosphorylation after withdrawal of HU and are profoundly sensitive to HU. Importantly, we found that phosphorylated Rad17 interacts with Claspin and regulates its phosphorylation. These findings reveal a phosphorylation-dependent function of Rad17 in an ATR-Rad17-Claspin-Chk1-signaling cascade that responds to specific replication stress.",

keywords = "CELLCYCLE, DNA",

author = "Xin Wang and Lee Zou and Tao Lu and Shilai Bao and Hurov, {Kristen E.} and Hittelman, {Walter N.} and Elledge, {Stephen J.} and Lei Li",

note = "Funding Information: We thank Michael Kastan for helpful suggestions to this work and Garry Nolan for providing the retroviral packaging system. The authors are supported by National Institutes of Health grants CA76172 (L.L.) and GM44664 (S.J.E.). S.J.E. is an Investigator with the Howard Hughes Medical Institute. L.Z. is partly supported by the Richard and Susan Smith New Investigator Award. K.E.H. is a Special Fellow of the Leukemia and Lymphoma Society. ",

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AU - Wang, Xin

AU - Zou, Lee

AU - Lu, Tao

AU - Bao, Shilai

AU - Hurov, Kristen E.

AU - Hittelman, Walter N.

AU - Elledge, Stephen J.

AU - Li, Lei

N1 - Funding Information: We thank Michael Kastan for helpful suggestions to this work and Garry Nolan for providing the retroviral packaging system. The authors are supported by National Institutes of Health grants CA76172 (L.L.) and GM44664 (S.J.E.). S.J.E. is an Investigator with the Howard Hughes Medical Institute. L.Z. is partly supported by the Richard and Susan Smith New Investigator Award. K.E.H. is a Special Fellow of the Leukemia and Lymphoma Society.

PY - 2006/8/4

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N2 - The ATR-mediated checkpoint is not only critical for responding to genotoxic stress but also essential for cell proliferation. The RFC-related checkpoint protein Rad17, a phosphorylation substrate of ATR, is critical for ATR-mediated checkpoint signaling and cell survival. Here, we show that phosphorylation of Rad17 by ATR is important for genomic stability and restraint of S phase but is not essential for cell survival. The phosphomutant Rad17AA exhibits distinct defects in hydroxyurea- (HU) and ultraviolet- (UV) induced Chk1 activation, indicating that separate Rad17 functions are required differently in response to different types of replication interference. Although cells expressing Rad17AA can initiate Chk1 phosphorylation after HU treatment, they fail to sustain Chk1 phosphorylation after withdrawal of HU and are profoundly sensitive to HU. Importantly, we found that phosphorylated Rad17 interacts with Claspin and regulates its phosphorylation. These findings reveal a phosphorylation-dependent function of Rad17 in an ATR-Rad17-Claspin-Chk1-signaling cascade that responds to specific replication stress.

AB - The ATR-mediated checkpoint is not only critical for responding to genotoxic stress but also essential for cell proliferation. The RFC-related checkpoint protein Rad17, a phosphorylation substrate of ATR, is critical for ATR-mediated checkpoint signaling and cell survival. Here, we show that phosphorylation of Rad17 by ATR is important for genomic stability and restraint of S phase but is not essential for cell survival. The phosphomutant Rad17AA exhibits distinct defects in hydroxyurea- (HU) and ultraviolet- (UV) induced Chk1 activation, indicating that separate Rad17 functions are required differently in response to different types of replication interference. Although cells expressing Rad17AA can initiate Chk1 phosphorylation after HU treatment, they fail to sustain Chk1 phosphorylation after withdrawal of HU and are profoundly sensitive to HU. Importantly, we found that phosphorylated Rad17 interacts with Claspin and regulates its phosphorylation. These findings reveal a phosphorylation-dependent function of Rad17 in an ATR-Rad17-Claspin-Chk1-signaling cascade that responds to specific replication stress.

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Rad17 Phosphorylation Is Required for Claspin Recruitment and Chk1 Activation in Response to Replication Stress

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