PAXX promotes KU accumulation at DNA breaks and is essential for end-joining in XLF-deficient mice

Xiangyu Liu; Zhengping Shao; Wenxia Jiang; Brian J. Lee; Shan Zha

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PAXX promotes KU accumulation at DNA breaks and is essential for end-joining in XLF-deficient mice

机译：PAXX促进DNA断裂时的KU积累，对于XLF缺陷小鼠的末端连接至关重要

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Non-homologous end-joining (NHEJ) is the most prominent DNA double strand break (DSB) repair pathway in mammalian cells. PAXX is the newest NHEJ factor, which shares structural similarity with known NHEJ factors—XRCC4 and XLF. Here we report that PAXX is dispensable for physiological NHEJ in otherwise wild-type mice. Yet Paxx ?/? mice require XLF and Xlf ?/? mice require PAXX for end-ligation. As such, Xlf ?/? Paxx ?/? mice display severe genomic instability and neuronal apoptosis, which eventually lead to embryonic lethality. Despite their structural similarities, only Xlf ?/? cells, but not Paxx ?/? cells require ATM/DNA-PK kinase activity for end-ligation. Mechanistically, PAXX promotes the accumulation of KU at DSBs, while XLF enhances LIG4 recruitment without affecting KU dynamics at DNA breaks in vivo . Together these findings identify the molecular functions of PAXX in KU accumulation at DNA ends and reveal distinct, yet critically complementary functions of PAXX and XLF during NHEJ.

机译：非同源末端连接（NHEJ）是哺乳动物细胞中最突出的DNA双链断裂（DSB）修复途径。 PAXX是最新的NHEJ因子，与已知的NHEJ因子XRCC4和XLF具有相似的结构。在这里，我们报道了PAXX对于否则为野生型小鼠的生理性NHEJ而言是不可缺少的。但是Paxx ？/？小鼠需要XLF，Xlf ？/？小鼠需要PAXX进行末端连接。因此，Xlf ？/？ Paxx ？/？小鼠表现出严重的基因组不稳定和神经元凋亡，最终导致胚胎致死率。尽管它们的结构相似，但只有Xlf α/？细胞，而不是Paxx α/？细胞需要ATM / DNA-PK激酶活性来进行末端连接。从机理上讲，PAXX促进了DSB处KU的积累，而XLF增强了LIG4募集而又不影响体内DNA断裂时的KU动态。这些发现共同确定了PAXX在DNA末端KU积累中的分子功能，并揭示了NHEJ期间PAXX和XLF的独特但至关重要的互补功能。

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《Nature Communications》 |2017年第1期|共页
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Xiangyu Liu; Zhengping Shao; Wenxia Jiang; Brian J. Lee; Shan Zha;
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1. PAXX, a paralog of XRCC4 and XLF, interacts with Ku to promote DNA double-strand break repair [J] . Takashi Ochi, Andrew N. Blackford, Julia Coates, Science . 2015,第6218期

机译：PAXX是XRCC4和XLF的旁系同源物，与Ku相互作用以促进DNA双链断裂修复
2. Distinct roles of XRCC4 and Ku80 in non-homologous end-joining of endonuclease- and ionizing radiation-induced DNA double-strand breaks. [J] . Schulte-Uentrop L, El-Awady RA, Schliecker L, Nucleic Acids Research . 2008,第8期

机译：XRCC4和Ku80在核酸内切酶和电离辐射诱导的DNA双链断裂的非同源末端连接中的不同作用。
3. Distinct roles of XRCC4 and Ku80 in non-homologous end-joining of endonuclease- and ionizing radiation-induced DNA double-strand breaks [J] . Henning Willers, Jochen Dahm-Daphi, Lena Schliecker, Nucleic acids research . 2008,第8期

机译：XRCC4和Ku80在核酸内切酶和电离辐射诱导的DNA双链断裂的非同源末端连接中的不同作用
4. Repairing DNA double-strand breaks by the prokaryotic non-homologous end-joining pathway [C] . Nigel C. Brissett, Aidan J. Doherty Biochemical Society Symposium . 2009

机译：通过原核非同源终端连接途径修复DNA双链断裂
5. DNA end protection at double strand breaks and telomeres by Ku70/80 and Cdc13. [D] . Krasner, Danielle Sonya. 2015

机译：Ku70 / 80和Cdc13在双链断裂和端粒的DNA末端保护。
6. PAXX promotes KU accumulation at DNA breaks and is essential for end-joining in XLF-deficient mice [O] . Xiangyu Liu, Zhengping Shao, Wenxia Jiang, -1

机译：PAXX促进DNA断裂时的KU积累对于XLF缺陷小鼠的末端连接至关重要
7. PAXX, a paralog of XRCC4 and XLF, interacts with Ku to promote DNA double-strand break repair [O] . Ochi Takashi, Blackford Andrew Nicholas, Coates Julia, 2015

机译：PAXX是XRCC4和XLF的旁系同源物，与Ku相互作用以促进DNA双链断裂修复

PAXX promotes KU accumulation at DNA breaks and is essential for end-joining in XLF-deficient mice

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