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Human RECQL5 beta stimulates flap endonuclease 1

机译:人RECQL5 beta刺激皮瓣内切核酸酶1

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Human RECQL5 is a member of the RecQ helicase family which is implicated in genome maintenance. Five human members of the family have been identified; three of them, BLM, WRN and RECQL4 are associated with elevated cancer risk. RECQL1 and RECQL5 have not been linked to any human disorder yet; cells devoid of RECQL1 and RECQL5 display increased chromosomal instability. Here, we report the physical and functional interaction of the large isomer of RECQL5, RECQL5 beta, with the human flap endonuclease 1, FEN1, which plays a critical role in DNA replication, recombination and repair. RECQL5 beta dramatically stimulates the rate of FEN1 cleavage of flap DNA substrates. Moreover, we show that RECQL5 beta and FEN1 interact physically and co-localize in the nucleus in response to DNA damage. Our findings, together with the previous literature on WRN, BLM and RECQL4's stimulation of FEN1, suggests that the ability of RecQ helicases to stimulate FEN1 may be a general feature of this class of enzymes. This could indicate a common role for the RecQ helicases in the processing of oxidative DNA damage.
机译:人RECQL5是RecQ解旋酶家族的一员,与基因组维护有关。已确定该家庭的五名人类成员; BLM,WRN和RECQL4这三个与癌症风险升高相关。 RECQL1和RECQL5尚未与任何人类疾病相关;缺少RECQL1和RECQL5的细胞显示出增加的染色体不稳定性。在这里,我们报告RECQL5的大异构体RECQL5 beta与人类皮瓣内切核酸酶1 FEN1的物理和功能相互作用,该酶在DNA复制,重组和修复中起关键作用。 RECQL5 beta极大地刺激了皮瓣DNA底物的FEN1切割速率。此外,我们表明RECQL5 beta和FEN1物理相互作用,并在细胞核中共定位,以响应DNA损伤。我们的发现以及有关WRN,BLM和RECQL4对FEN1的刺激的先前文献表明,RecQ解旋酶刺激FEN1的能力可能是此类酶的普遍特征。这可能表明RecQ解旋酶在氧化DNA损伤的处理中具有共同的作用。

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