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タイトル
和文: 
英文:Fundamental cell cycle kinases collaborate to ensure timely destruction of the synaptonemal complex during meiosis 
著者
和文: Argunhan Bilge, Wing-Kit Leung, Afshar Negar, Yaroslav Terentyev, Vijayalakshmi V Subramanian, 村山 泰斗, Andreas Hochwagen, 岩崎 博史, Tomomi Tsubouchi, 坪内 英生.  
英文: Bilge Argunhan, Wing-Kit Leung, Negar Afshar, Yaroslav Terentyev, Vijayalakshmi V Subramanian, Yasuto Murayama, Andreas Hochwagen, Hiroshi Iwasaki, Tomomi Tsubouchi, Hideo Tsubouchi.  
言語 English 
掲載誌/書名
和文: 
英文:EMBO Journal 
巻, 号, ページ Vol. 36    No. 17    pp. 2488-2509
出版年月 2017年9月 
出版者
和文: 
英文:EMBO Press 
会議名称
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英文: 
開催地
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英文: 
ファイル
公式リンク http://www.scopus.com/inward/record.url?eid=2-s2.0-85022337792&partnerID=MN8TOARS
 
DOI https://doi.org/10.15252/embj.201695895
アブストラクト The synaptonemal complex (SC) is a proteinaceous macromolecular assembly that forms during meiotic prophase I and mediates adhesion of paired homologous chromosomes along their entire lengths. Although prompt disassembly of the SC during exit from prophase I is a landmark event of meiosis, the underlying mechanism regulating SC destruction has remained elusive. Here, we show that DDK (Dbf4-dependent Cdc7 kinase) is central to SC destruction. Upon exit from prophase I, Dbf4, the regulatory subunit of DDK, directly associates with and is phosphorylated by the Polo-like kinase Cdc5. In parallel, upregulated CDK1 activity also targets Dbf4. An enhanced Dbf4-Cdc5 interaction pronounced phosphorylation of Dbf4 and accelerated SC destruction, while reduced/abolished Dbf4 phosphorylation hampered destruction of SC proteins. SC destruction relieved meiotic inhibition of the ubiquitous recombinase Rad51, suggesting that the mitotic recombination machinery is reactivated following prophase I exit to repair any persisting meiotic DNA double-strand breaks. Taken together, we propose that the concerted action of DDK, Polo-like kinase, and CDK1 promotes efficient SC destruction at the end of prophase I to ensure faithful inheritance of the genome.

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