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Ku heterodimer binds to both ends of the Werner protein and functional interaction occurs at the Werner N-terminus

机译:Ku异二聚体结合到Werner蛋白的两端,并且功能相互作用发生在Werner N末端

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摘要

The human Werner syndrome protein, WRN, is a member of the RecQ helicase family and contains 3′→5′ helicase and 3′→5′ exonuclease activities. Recently, we showed that the exonuclease activity of WRN is greatly stimulated by the human Ku heterodimer protein. We have now mapped this interaction physically and functionally. The Ku70 subunit specifically interacts with the N-terminus (amino acids 1–368) of WRN, while the Ku80 subunit interacts with its C-terminus (amino acids 940– 1432). Binding between Ku70 and the N-terminus of WRN (amino acids 1–368) is sufficient for stimulation of WRN exonuclease activity. A mutant Ku heterodimer of full-length Ku80 and truncated Ku70 (amino acids 430–542) interacts with C-WRN but not with N-WRN and cannot stimulate WRN exonuclease activity. This emphasizes the functional significance of the interaction between the N-terminus of WRN and Ku70. The interaction between Ku80 and the C-terminus of WRN may modulate some other, as yet unknown, function. The strong interaction between Ku and WRN suggests that these two proteins function together in one or more pathways of DNA metabolism.
机译:人类Werner综合征蛋白WRN是RecQ解旋酶家族的成员,并具有3'→5'解旋酶和3'→5'核酸外切酶活性。最近,我们显示了人类Ku异二聚体蛋白极大地刺激了WRN的核酸外切酶活性。现在,我们已在物理上和功能上映射了此交互。 Ku70亚基与WRN的N末端(氨基酸1–368)特异性相互作用,而Ku80亚基与其C末端(氨基酸940–1432)相互作用。 Ku70和WRN的N末端(1-368位氨基酸)之间的结合足以刺激WRN核酸外切酶活性。全长Ku80和截短的Ku70(氨基酸430-542)的突变Ku异二聚体与C-WRN相互作用,但不与N-WRN相互作用,并且不能刺激WRN外切核酸酶活性。这强调了WRN和Ku70的N端相互作用的功能重要性。 Ku80和WRN的C末端之间的相互作用可能会调节某些其他功能(目前尚不清楚)。 Ku和WRN之间的强相互作用表明,这两种蛋白质在DNA代谢的一种或多种途径中共同起作用。

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