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The leucine rich region of DNA-PKcs contributes to its innate DNA affinity

机译:DNA-PKcs富含亮氨酸的区域有助于其固有的DNA亲和力

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摘要

DNA-PK is a protein complex that consists of a DNA-binding, regulatory subunit [Ku] and a larger similar to 465 kDa catalytic subunit [DNA-PKcs], a serine/threonine protein kinase. The kinase activity of DNA-PKcs resides between residues 3745 and 4013, a PI3 kinase domain. Another recognized domain within this large protein is a leucine zipper (LZ) motif or perhaps more appropriately designated a leucine rich region (LRR) that spans residues 1503-1602. Whereas, DNA-PK's kinase activity has been shown to be absolutely indispensable for its function in non-homologous end joining (NHEJ), little is known about the functional relevance of the LRR. Here we show that DNA-PKcs with point mutations in the LRR can only partially reverse the radiosensitive phenotype and V(D)J recombination deficits of DNA-PKcs deficient cells. Disruption of the LRR motif affects the ability to purify DNA-PKcs via its binding to DNA-cellulose, but does not affect its interaction with Ku or its catalytic activity. These data suggest that the LRR region of DNA-PKcs may contribute to its intrinsic DNA affinity, and moreover, that intrinsic DNA binding is important for optimal function of DNA-PKcs in repairing double strand breaks in living cells.
机译:DNA-PK是一种蛋白质复合物,由DNA结合的调节亚基[Ku]和更大的类似于465 kDa的催化亚基[DNA-PKcs](一种丝氨酸/苏氨酸蛋白激酶)组成。 DNA-PKcs的激酶活性位于PI3激酶结构域3745和4013残基之间。这种大蛋白中的另一个公认结构域是亮氨酸拉链(LZ)基序,或者可能更恰当地指定为跨越残基1503-1602的富亮氨酸区域(LRR)。鉴于DNA-PK的激酶活性已证明其在非同源末端连接(NHEJ)中的功能是绝对必不可少的,对LRR的功能相关性知之甚少。在这里,我们显示LRR中具有点突变的DNA-PKcs只能部分逆转DNA-PKcs缺陷细胞的放射敏感性表型和V(D)J重组缺陷。 LRR基序的破坏通过与DNA纤维素结合而影响纯化DNA-PKcs的能力,但不影响其与Ku的相互作用或催化活性。这些数据表明DNA-PKcs的LRR区可能有助于其固有的DNA亲和力,此外,固有的DNA结合对于修复活细胞中双链断裂的DNA-PKcs的最佳功能很重要。

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