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An N-terminal domain of Dbf4p mediates interaction with both origin recognition complex (ORC) and Rad53p and can deregulate late origin firing

机译：Dbf4p的N末端域介导与起源识别复合体（ORC）和Rad53p的相互作用，并且可以解除对晚期起源射击的管制

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摘要

The Dbf4/Cdc7 kinase acts at the level of individual origins to promote the initiation of DNA replication. We demonstrate through both immunoprecipitation and two-hybrid assays that a domain comprising the first 296 aa of Dbf4p interacts with Orc2p and Orc3p subunits of the origin recognition complex (ORC). Given that the activation of Rad53 kinase in response to the DNA replication checkpoint leads to the release of Dbf4p from an ORC-containing chromatin fraction, we also examined interaction between Dbf4p and Rad53p. This same domain of Dbf4p binds specifically to the forkhead homology-associated (FHA) domains of Rad53p. Cell cycle arrest in G_2/M, provoked by the overexpression of the Dbf4 domain, is suppressed in a rad53 mutant. Moreover, its overexpression perturbs the regulation of late, but not early, origin firing in wild-type cells after treatment with hydroxyurea.

机译：Dbf4 / Cdc7激酶在单个来源的水平上起作用，以促进DNA复制的启动。我们通过免疫沉淀和双重杂交试验证明，包含Dbf4p的前296 aa的域与起源识别复合体（ORC）的Orc2p和Orc3p亚基相互作用。鉴于响应DNA复制检查点激活Rad53激酶导致Dbf4p从含ORC的染色质组分中释放出来，我们还研究了Dbf4p和Rad53p之间的相互作用。 Dbf4p的同一域与Rad53p的叉头同源相关（FHA）域特异性结合。在rad53突变体中，由于Dbf4结构域的过度表达引起的G_2 / M细胞周期停滞被抑制。此外，其过表达扰乱了在用羟基脲处理后野生型细胞中晚期而非早期起源放电的调控。

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《Proceedings of the National Academy of Sciences of the United States of America》 |2002年第25期|p.16087-16092|共6页
作者
Bernard P. Duncker; Kenji Shimada; Monika Tsai-Pflugfelder; Philippe Pasero; Susan M. Gasser;
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作者单位

Department of Biology, University of Waterloo, Waterloo, ON, Canada N2L 3G1;

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收录信息美国《科学引文索引》(SCI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
原文格式 PDF
正文语种 eng
中图分类自然科学总论;
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入库时间 2022-08-18 00:47:02

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机译：人体细胞中的一般复制子和复制起点，以及酵母ORC在介导组蛋白甲基化中的作用。
6. An N-terminal domain of Dbf4p mediates interaction with both origin recognition complex (ORC) and Rad53p and can deregulate late origin firing [O] . Bernard P. Duncker, Kenji Shimada, Monika Tsai-Pflugfelder, 2002

机译：Dbf4p的N末端域介导与起源识别复合体（ORC）和Rad53p的相互作用并且可以解除对晚期起源射击的管制
7. An N-terminal domain of Dbf4p mediates interaction with both origin recognition complex (ORC) and Rad53p and can deregulate late origin firing [O] . Duncker, Bernard P., Shimada, Kenji, Tsai-Pflugfelder, Monika, 2002

机译：Dbf4p的N末端域介导与起源识别复合体（ORC）和Rad53p的相互作用，并且可以解除对晚期起源射击的管制

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