Abstract

The division of eukaryotic cells must occur in a highly faithful manner. During the course of the cell cycle, cells must be able to replicate their DNA with great fidelity. Furthermore, when problems arise during replication, cells must impose a checkpoint-mediated arrest of the cell cycle while they attempt to rectify lesions. Recently, we identified a novel protein called Treslin that is essential for DNA replication in vertebrate cells Treslin acts at a critical regulatory juncture in cellular duplication. In particular, Treslin is akey target of the cyclin-dependent kinase (CDK) that promotes the initial firing of replication origins at the onset of S-phase. Moreover, Treslin also appears to participate in checkpoint regulation. For the studies in this proposal, we will carry out an intensive analysis of Treslin and its functional relationships with other key regulators of S-phase. We will conduct these investigations in both Xenopus egg extracts and human cells. The egg-extract system offers some technical advantages that are not available currently with human cells. Numerous studies have indicated that this Xenopus system offers a valid model for human cells. Overall, we will attempt to reveal how Treslin promotes accurate replication and maintenance of the genome in vertebrates and how cells control the activity of Treslin. In particular, we will analyze the varios domains of Treslin in order to elucidate its functional architecture. We will examine how the collaboration of Treslin with other replication proteins contributes to its function. We will study further how phosphorylation controls the functional properties of Treslin. Moreover, we will also investigate the role of Treslin in checkpoint responses. Finally, we will attempt to identify new partners of Treslin and elucidate potentially novel functions of this protein. In general, these studies hold the promise to yield valuable insights into how cells maintain genomic integrity throughout their lifetimes. This information would be especially relevant for human health. Derangement of genomic integrity as a consequence of environmental insults or inherited mutations or both can result in various human pathologies, most notably cancer. Thus, a thorough understanding of the root causes for genomic instability will be essential for an informed strategy in combating cancer.

Public Health Relevance

Cells must replicate their DNA accurately in order to ensure that the genetic material remains intact throughout life. If errors arise during replication, cells must be able to rectify the problems before cell division. Otherwise, cells would accumulate defects in their chromosomes that might ultimately result in cancer. Therefore, a thorough knowledge of the quality-control mechanisms underlying faithful DNA replication will be essential for an understanding of the root causes of cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM043974-22
Application #
8776310
Study Section
Cellular Signaling and Regulatory Systems Study Section (CSRS)
Program Officer
Hamlet, Michelle R
Project Start
1990-04-01
Project End
2016-11-30
Budget Start
2014-12-01
Budget End
2015-11-30
Support Year
22
Fiscal Year
2015
Total Cost
$423,765
Indirect Cost
$169,251

  Institution

Name
California Institute of Technology
Department
Type
Schools of Arts and Sciences
DUNS #
009584210
City
Pasadena
State
CA
Country
United States
Zip Code
91125

  Publications

Kumagai, Akiko; Dunphy, William G (2017) MTBP, the partner of Treslin, contains a novel DNA-binding domain that is essential for proper initiation of DNA replication. Mol Biol Cell 28:2998-3012
Mu, Ruiling; Tat, John; Zamudio, Robert et al. (2017) CKS Proteins Promote Checkpoint Recovery by Stimulating Phosphorylation of Treslin. Mol Cell Biol 37:
Guo, Cai; Kumagai, Akiko; Schlacher, Katharina et al. (2015) Interaction of Chk1 with Treslin negatively regulates the initiation of chromosomal DNA replication. Mol Cell 57:492-505
Ryu, Hyunju; Yoshida, Makoto M; Sridharan, Vinidhra et al. (2015) SUMOylation of the C-terminal domain of DNA topoisomerase II? regulates the centromeric localization of Claspin. Cell Cycle 14:2777-84
Lee, Joon; Dunphy, William G (2013) The Mre11-Rad50-Nbs1 (MRN) complex has a specific role in the activation of Chk1 in response to stalled replication forks. Mol Biol Cell 24:1343-53
Kumar, Sanjay; Yoo, Hae Yong; Kumagai, Akiko et al. (2012) Role for Rif1 in the checkpoint response to damaged DNA in Xenopus egg extracts. Cell Cycle 11:1183-94
Meng, Zheng; Capalbo, Luisa; Glover, David M et al. (2011) Role for casein kinase 1 in the phosphorylation of Claspin on critical residues necessary for the activation of Chk1. Mol Biol Cell 22:2834-47
Kumagai, Akiko; Shevchenko, Anna; Shevchenko, Andrej et al. (2011) Direct regulation of Treslin by cyclin-dependent kinase is essential for the onset of DNA replication. J Cell Biol 193:995-1007
Ramírez-Lugo, Juan S; Yoo, Hae Yong; Yoon, Su Jin et al. (2011) CtIP interacts with TopBP1 and Nbs1 in the response to double-stranded DNA breaks (DSBs) in Xenopus egg extracts. Cell Cycle 10:469-80
Kumagai, Akiko; Shevchenko, Anna; Shevchenko, Andrej et al. (2010) Treslin collaborates with TopBP1 in triggering the initiation of DNA replication. Cell 140:349-59

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