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和文: 
英文:Molecular characterization of the role of the Schizosaccharomyces pombe nip1<sup>+</sup>/ctp1<sup>+</sup>gene in DNA double-strand break repair in association with the Mre11-Rad50-Nbs1 complex 
著者
和文: Akamatsu, Y., 村山泰斗, Yamada, T., Nakazaki, T., 筒井康博, Ohta, K., 岩崎博史.  
英文: Akamatsu, Y., Yasuto Murayama, Yamada, T., Nakazaki, T., Yasuhiro Tsutsui, Ohta, K., Hiroshi Iwasaki.  
言語 English 
掲載誌/書名
和文:Molecular and Cellular Biology 
英文:Molecular and Cellular Biology 
巻, 号, ページ Vol. 28    No. 11    pp. 3639-3651
出版年月 2008年6月 
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会議名称
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公式リンク http://www.scopus.com/inward/record.url?eid=2-s2.0-44349086462&partnerID=MN8TOARS
 
DOI https://doi.org/10.1128/MCB.01828-07
アブストラクト The Schizosaccharomyces pombe nip1+/ctp1+ gene was previously identified as an slr (synthetically lethal with rad2) mutant. Epistasis analysis indicated that Nip1/Ctp1 functions in Rhp51-dependent recombinational repair, together with the Rad32 (spMre11)-Rad50-Nbs1 complex, which plays important roles in the early steps of DNA double-strand break repair. Nip1/Ctp1 was phosphorylated in asynchronous, exponentially growing cells and further phosphorylated in response to bleomycin treatment. Overproduction of Nip1/Ctp1 suppressed the DNA repair defect of an nbs1-s10 mutant, which carries a mutation in the FHA phosphopeptide-binding domain of Nbs1, but not of an nbs1 null mutant. Meiotic DNA double-strand breaks accumulated in the nip1/ctp1 mutant. The DNA repair phenotypes and epistasis relationships of nip1/ctp1 are very similar to those of the Saccharomyces cerevisiae sae2/com1 mutant, suggesting that Nip1/Ctp1 is a functional homologue of Sae2/Com1, although the sequence similarity between the proteins is limited to the C-terminal region containing the RHR motif. We found that the RxxL and CxxC motifs are conserved in Schizosaccharomyces species and in vertebrate CtIP, originally identified as a cofactor of the transcriptional corepressor CtBP. However, these two motifs are not found in other fungi, including Saccharomyces and Aspergillus species. We propose that Nip1/Ctp1 is a functional counterpart of Sae2/Com1 and CtIP.

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