5 ' exonuclease, suggesting that it maintains genome integrity. To investigate TREX2s biochemical and cellular properties, we show that endogenous TREX2 is'/> Biochemical and cellular characteristics of the 3 '- 5 ' exonuclease TREX2
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Biochemical and cellular characteristics of the 3 '- 5 ' exonuclease TREX2

机译:3'-> 5'核酸外切酶TREX2的生化和细胞特性

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TREX2 is an autonomous nonprocessive 3 ' -> 5 ' exonuclease, suggesting that it maintains genome integrity. To investigate TREX2s biochemical and cellular properties, we show that endogenous TREX2 is expressed widely in mouse tissues and human cell lines. Unexpectedly, endogenous human TREX2 is predominantly expressed as a 30-kDa protein (not 26 kDa, as previously believed), which is likely encoded by longer isoforms (TREX2(L1) and/or TREX2(L2)) that possess similar capacity for self-association, DNA binding and catalytic activity. Site-directed mutagenesis analysis shows that the three functional activities of TREX2 are distinct, yet integrated. Mutation of amino acids putatively important for homodimerization significantly impairs both DNA binding and exonuclease activity, while mutation of amino acids (except R163) in the DNA binding and exonuclease domains affects their corresponding activities. Interestingly, however, DNA-binding domain mutations do not impact catalytic activity, while exonuclease domain mutations diminish DNA binding. To understand TREX2 cellular properties, we find endogenous TREX2 is down regulated during G2/M and nuclear TREX2 displays a punctate staining pattern. Furthermore, TREX2 knockdown reduces cell proliferation. Taken together, our results suggest that TREX2 plays an important function during DNA metabolism and cellular proliferation.
机译:TREX2是一种自主的非过程性3'-> 5'核酸外切酶,表明它保持了基因组的完整性。为了研究TREX2的生化和细胞特性,我们表明内源性TREX2在小鼠组织和人类细胞系中广泛表达。出乎意料的是,内源性人类TREX2主要表达为30 kDa的蛋白质(以前认为不是26 kDa的蛋白质),它可能由具有相似自我功能的较长同工型(TREX2(L1)和/或TREX2(L2))编码。 -缔合,DNA结合和催化活性。定点诱变分析表明,TREX2的三个功能活动是不同的,但已整合在一起。假定对同型二聚化重要的氨基酸突变会显着损害DNA结合和核酸外切酶活性,而DNA结合和核酸外切酶域中的氨基酸(R163除外)突变会影响其相应的活性。然而,有趣的是,DNA结合域突变不影响催化活性,而核酸外切酶结构域突变则减少了DNA结合。为了了解TREX2的细胞特性,我们发现内源性TREX2在G2 / M过程中被下调,而核TREX2显示出点状染色模式。此外,TREX2组合式减少细胞增殖。两者合计,我们的结果表明TREX2在DNA代谢和细胞增殖过程中起着重要的作用。

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