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GartnerAnton

Gartner, Anton
DNA Damage Response and Genetic Toxicology
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Cell cycle progression requires the CDC-48(UFD-1/NPL-4) complex for efficient DNA replication

Author(s)
Mouysset, JulienDeichsel, AlexandraMoser, SandraHoege, CarstenHyman, Anthony A.Gartner, AntonHoppe, Thorsten
Issued Date
2008-09
DOI
10.1073/pnas.0805944105
URI
https://scholarworks.unist.ac.kr/handle/201301/31007
Fulltext
https://www.pnas.org/content/105/35/12879
Citation
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, v.105, no.35, pp.12879 - 12884
Abstract
Since cdc48 mutants were isolated by the first genetic screens for cell division cycle (cdc) mutants in yeast, the requirement of the chaperone-like ATPase Cdc48/p97 during cell division has remained unclear. Here, we discover an unanticipated function for Caenorhabditis elegans CDC-48 in DNA replication linked to cell cycle control. Our analysis of the CDC-48(UFD-1/NPL-4) complex identified a general role in S phase progression of mitotic cells essential for embryonic cell division and germline development of adult worms. These developmental defects result from activation of the DNA replication checkpoint caused by replication stress. Similar to loss of replication licensing factors, DNA content is strongly reduced in worms depleted for CDC-48, UFD-1, and NPL-4. In addition, these worms show decreased DNA synthesis and hypersensitivity toward replication blocking agents. Our findings identified a role for CDC-48(UFD-1/NPL-4) in DNA replication, which is important for cell cycle progression and genome stability.
Publisher
NATL ACAD SCIENCES
ISSN
0027-8424
Keyword (Author)
ATL-1/ATRC. elegansCDC-48/p97genome stability
Keyword
UNFOLDED PROTEIN RESPONSEAAA-ATPASE P97/VCPCAENORHABDITIS-ELEGANSMEMBRANE-FUSIONC-ELEGANSRECOMBINATION PROTEINUBIQUITINMITOSISP97CDC48/P97

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