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Lcd1p Recruits Mec1p to DNA Lesions In Vitro and In Vivo

机译:Lcd1p招募Mec1p体外和体内DNA损伤

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摘要

The Lcd1p/Mec1p complex is crucial for normal S phase progression and for signaling DNA damage. We show that Lcd1p/Ddc2p and Mec1p in cell extracts bind to DNA ends. Although Lcd1p binds DNA independently of Mec1p, recruitment of Mec1p to DNA requires Lcd1p. DNA binding by Lcd1p is also independent of Rad9p, Rad17p, and Rad24p. Recombinant Lcd1p binds DNA, and this is impaired by Lcd1p mutations that abrogate its in vivo functions. Furthermore, mec1p is recruited to cdc13-induced DNA damage and HO endonuclease-induced double-strand breaks in vivo. This requires Lcd1p, and recruitment of Lcd1p/Mec1p to cdc13-induced damage is abolished by Lcd1p mutations that abrogate its in vivo functions. Recruitment of Lcd1p to these lesions is independent of Mec1p and Rad9p/Rad24p. Thus, recruitment of Mec1p to DNA lesions by Lcd1p is crucial for the DNA damage response.
机译:Lcd1p / Mec1p复合物对于正常的S期进展和信号DNA损伤至关重要。我们显示细胞提取物中的Lcd1p / Ddc2p和Mec1p结合到DNA末端。尽管Lcd1p独立于Mec1p结合DNA,但将Mec1p募集到DNA需要Lcd1p。 Lcd1p的DNA结合也独立于Rad9p,Rad17p和Rad24p。重组Lcd1p结合DNA,而Lcd1p突变会破坏其体内功能,从而削弱DNA的功能。此外,mec1p被募集到cdc13诱导的DNA损伤和HO内切核酸酶诱导的体内双链断裂。这需要Lcd1p,取消Lcd1p / Mec1p对cdc13诱导的损伤的征兆被取消其体内功能的Lcd1p突变所废除。 Lcd1p对这些病变的募集独立于Mec1p和Rad9p / Rad24p。因此,Lcd1p将Mec1p募集到DNA损伤对于DNA损伤反应至关重要。

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