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首页> 外文期刊>International Journal of Molecular Sciences >Karyopherin α-2 Mediates MDC1 Nuclear Import through a Functional Nuclear Localization Signal in the tBRCT Domain of MDC1
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Karyopherin α-2 Mediates MDC1 Nuclear Import through a Functional Nuclear Localization Signal in the tBRCT Domain of MDC1

机译:Karyopherinα-2通过MDC1的TBRCT结构域中的功能核定位信号调解MDC1核导入

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Mediator of DNA damage checkpoint protein 1 (MDC1) plays a vital role in DNA damage response (DDR) by coordinating the repair of double strand breaks (DSBs). Here, we identified a novel interaction between MDC1 and karyopherin α-2 (KPNA2), a nucleocytoplasmic transport adaptor, and showed that KPNA2 is necessary for MDC1 nuclear import. Thereafter, we identified a functional nuclear localization signal (NLS) between amino acid residues 1989–1994 of the two Breast Cancer 1 (BRCA1) carboxyl-terminal (tBRCT) domain of MDC1 and demonstrated disruption of this NLS impaired interaction between MDC1 and KPNA2 and reduced nuclear localization of MDC1. In KPNA2-depleted cells, the recruitment of MDC1, along with the downstream signaling p roteins Ring Finger Protein 8 (RNF8), 53BP1-binding protein 1 (53BP1), BRCA1, and Ring Finger Protein 168 (RNF168), to DNA damage sites was abolished. Additionally, KPNA2-depleted cells had a decreased rate of homologous recombination (HR) repair. Our data suggest that KPNA2-mediated MDC1 nuclear import is important for DDR signaling and DSB repair.
机译:DNA损伤检查点蛋白1(MDC1)通过协调双链断裂(DSB)的修复在DNA损伤响应(DDR)中起着至关重要的作用。在此,我们鉴定了MDC1和Karyopherinα-2(KPNA2),核细胞质传输适配器之间的新型相互作用,并显示KPNA2是MDC1核导入所必需的。此后,我们鉴定了MDC1的两个乳腺癌1(BRCA1)羧基末端(TBRCT)结构域的氨基酸残基1989-1994之间的功能核定位信号(NLS),并证明了该NLS之间的破坏,MDC1和KPNA2之间的相互作用受损减少MDC1的核定位。在KPNA2-耗尽的细胞中,MDC1的募集以及下游信号传导PROTINS环手指蛋白8(RNF8),53bp1结合蛋白1(53bp1),BRCA1和无名指蛋白质168(RNF168),对DNA损伤部位被废除了。另外,KPNA2耗尽的细胞具有降低的同源重组(HR)修复。我们的数据表明,KPNA2介导的MDC1核导入对于DDR信令和DSB修复非常重要。

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