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GartnerAnton

Gartner, Anton
DNA Damage Response and Genetic Toxicology
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C. elegans SIR-2.1 translocation is linked to a proapoptotic pathway parallel to cep-1/p53 during DNA damage-induced apoptosis

Author(s)
Greiss, SebastianHall, JulieAhmed, ShawnGartner, Anton
Issued Date
2008-10
DOI
10.1101/gad.482608
URI
https://scholarworks.unist.ac.kr/handle/201301/31006
Fulltext
http://genesdev.cshlp.org/content/22/20/2831
Citation
GENES & DEVELOPMENT, v.22, no.20, pp.2831 - 2842
Abstract
Caenorhabditis elegans SIR-2.1, a member of the sirtuin family related to Saccharomyces cerevisiae Sir2p, has previously been implicated in aging. The mammalian homolog SIRT1 plays important roles in multiple cellular processes including transcriptional repression and stress response. We show that sir-2.1 is essential for the execution of apoptosis in response to DNA damage, and that sir-2.1 genetically acts in parallel to the worm p53-like gene cep-1. This novel cep-1-independent proapoptotic pathway does not require the daf-16 FOXO transcription factor. Cytological analysis of SIR-2.1 suggests a novel mechanism of apoptosis induction. During apoptosis SIR-2.1 changes its subcellular localization from the nucleus to the cytoplasm and transiently colocalizes with the C. elegans Apaf-1 homolog CED-4 at the nuclear periphery. SIR-2.1 translocation is an early event in germ cell apoptosis and is independent of apoptosis execution and cep- 1, raising the possibility that SIR-2.1 translocation is linked to the induction of DNA damage- induced apoptosis.
Publisher
COLD SPRING HARBOR LAB PRESS, PUBLICATIONS DEPT
ISSN
0890-9369
Keyword (Author)
sir-2.1SIR2sirtuinC. elegansDNA damage responseapoptosis
Keyword
PROGRAMMED CELL-DEATHCAENORHABDITIS-ELEGANSLIFE-SPANSACCHAROMYCES-CEREVISIAECHECKPOINT PROTEINSIRT1 DEACETYLASETUMOR-SUPPRESSORSTRAND BREAKSGERM-LINEP53

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