Essential role of Tip60-dependent recruitment of ribonucleotide reductase at DNA damage sites in DNA repair during G1 phase

Tip60 依赖的核苷酸还原酶在 DNA 损伤位点的募集在 G1 期 DNA 修复中的重要作用

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作者：Hiroyuki Niida, Yuko Katsuno, Misuzu Sengoku, Midori Shimada, Megumi Yukawa, Masae Ikura, Tsuyoshi Ikura, Kazuteru Kohno, Hiroki Shima, Hidekazu Suzuki, Satoshi Tashiro, Makoto Nakanishi

期刊：	Genes & Development	影响因子：	1.900
时间：	2010	起止号：	2010 Feb 15;24(4):333-8.
doi：	10.1101/gad.1863810	方法学：	FCM、IF、IHC-P、WB
靶点：	CHK1	研究方向：	信号转导

Abstract

A balanced deoxyribonucleotide (dNTP) supply is essential for DNA repair. Here, we found that ribonucleotide reductase (RNR) subunits RRM1 and RRM2 accumulated very rapidly at damage sites. RRM1 bound physically to Tip60. Chromatin immunoprecipitation analyses of cells with an I-SceI cassette revealed that RRM1 bound to a damage site in a Tip60-dependent manner. Active RRM1 mutants lacking Tip60 binding failed to rescue an impaired DNA repair in RRM1-depleted G1-phase cells. Inhibition of RNR recruitment by an RRM1 C-terminal fragment sensitized cells to DNA damage. We propose that Tip60-dependent recruitment of RNR plays an essential role in dNTP supply for DNA repair.

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