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Cdc24 Is Essential for Long-range End Resection in the Repair of Double-stranded DNA Breaks

机译:Cdc24是修复双链DNA断裂的远程末端切除必不可少的

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摘要

Double-stranded DNA breaks (DSBs) are highly detrimental DNA lesions, which may be repaired by the homologous recombination-mediated repair pathway. The 5′ to 3′ direction of long-range end resection on one DNA strand, in which 3′-single-stranded DNA overhangs are created from broken DNA ends, is an essential step in this pathway. Dna2 has been demonstrated as an essential nuclease in this event, but the molecular mechanism of how Dna2 is recruited to DNA break sites in vivo has not been elucidated. In this study, a novel recombination factor called Cdc24 was identified in fission yeast. We demonstrated that Cdc24 localizes to DNA break sites during the repair of DNA breaks and is an essential factor in long-range end resection. We also determined that Cdc24 plays a direct role in recruiting Dna2 to DNA break sites through its interaction with Dna2 and replication protein A (RPA). Further, this study revealed that RPA acts as the foundation for assembling the machinery for long-range end resection by its essential role in recruiting Cdc24 and Dna2 to DNA break sites. These results define Cdc24 as an essential factor for long-range end resection in the repair of DSBs, opening the door for further investigations into the enzymes involved in long-range end resection for DSB repair.
机译:双链DNA断裂(DSB)是高度有害的DNA损伤,可通过同源重组介导的修复途径修复。在一条DNA链上进行长距离末端切除的5'至3'方向是此途径中的重要步骤,其中3'单链DNA突出端由断裂的DNA末端形成。在这种情况下,Dna2已被证明是一种必需的核酸酶,但尚未阐明Dna2在体内如何被募集至DNA断裂位点的分子机制。在这项研究中,在裂殖酵母中发现了一种新的重组因子Cdc24。我们证明了Cdc24在DNA断裂修复过程中定位于DNA断裂位点,并且是远距离末端切除的重要因素。我们还确定,Cdc24通过与Dna2和复制蛋白A(RPA)相互作用,在将Dna2募集到DNA断裂位点中起直接作用。此外,这项研究表明RPA通过将Cdc24和Dna2募集至DNA断裂位点,发挥了重要作用,从而成为了组装远程末端切除术的基础。这些结果将Cdc24定义为DSB修复远距离末端切除的必要因素,为进一步研究DSB修复远距离末端切除涉及的酶打开了大门。

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