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Rif1 is a global regulator of timing of replication origin firing in fission yeast

机译:Rif1是裂变酵母中复制起点触发时间的全球调节者

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摘要

One of the long-standing questions in eukaryotic DNA replication is the mechanisms that determine where and when a particular segment of the genome is replicated. Cdc7/Hsk1 is a conserved kinase required for initiation of DNA replication and may affect the site selection and timing of origin firing. We identified rif1D, a null mutant of rif1+, a conserved telomere-binding factor, as an efficient bypass mutant of fission yeast hsk1. Extensive deregulation of dormant origins over a wide range of the chromosomes occurs in rif1D in the presence or absence of hydroxyurea (HU). At the same time, many early-firing, efficient origins are suppressed or delayed in firing timing in rif1D. Rif1 binds not only to telomeres, but also to many specific locations on the arm segments that only partially overlap with the prereplicative complex assembly sites, although Rif1 tends to bind in the vicinity of the late/dormant origins activated in rif1D. The binding to the arm segments occurs through M to G1 phase in a manner independent of Taz1 and appears to be essential for the replication timing program during the normal cell cycle. Our data demonstrate that Rif1 is a critical determinant of the origin activation program on the fission yeast chromosomes.
机译:真核DNA复制中长期存在的问题之一是确定基因组特定片段在何处以及何时复制的机制。 Cdc7 / Hsk1是启动DNA复制所需的保守激酶,可能会影响位点的选择和起始时间。我们确定rif1D,rif1 +的无效突变体,一种保守的端粒结合因子,是裂变酵母hsk1的有效旁路突变体。在存在或不存在羟基脲(HU)的情况下,在rif1D中会发生广泛的染色体休眠起源的广泛失控。同时,在rif1D中,许多早期射击的有效起源被抑制或延迟了射击时机。尽管Rif1倾向于结合在rif1D中激活的晚期/休眠起源附近,但Rif1不仅与端粒结合,而且与臂节上的许多特定位置结合,这些特定位置仅部分与复制前的复杂装配位点重叠。与臂节的结合通过M到G1阶段以独立于Taz1的方式发生,并且似乎对于正常细胞周期中的复制计时程序至关重要。我们的数据表明Rif1是裂变酵母染色体上起源激活程序的关键决定因素。

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