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首页> 外文期刊>Human Molecular Genetics >BRCA1 mislocalization leads to aberrant DNA damage response in heterozygous ABRAXAS1 mutation carrier cells
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BRCA1 mislocalization leads to aberrant DNA damage response in heterozygous ABRAXAS1 mutation carrier cells

机译:BRCA1的错误定位导致杂合的abraxas1突变载体细胞中的异常DNA损伤反应

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摘要

Whilst heterozygous germline mutations in the ABRAXAS1 gene have been associated with a hereditary predisposition to breast cancer, their effect on promoting tumourigenesis at the cellular level has not been explored. Here, we demonstrate in patient-derived cells that the Finnish ABRAXAS1 founder mutation (c.1082G> A, Arg361Gln), even in the heterozygous state leads to decreased BRCA1 protein levels as well as reduced nuclear localization and foci formation of BRCA1 and CtIP. This causes disturbances in basal BRCA1-A complex localization, which is reflected by a restraint in error-prone DNA double-strand break repair pathway usage, attenuated DNA damage response and deregulated G2-M checkpoint control. The current study clearly demonstrates how the Finnish ABRAXAS1 founder mutation acts in a dominant-negative manner on BRCA1 to promote genome destabilization in heterozygous carrier cells.
机译:虽然abraxas1基因中的杂合子种系突变与母乳癌的遗传性易感性有关,但它们对在细胞水平促进肿瘤内脉冲脉冲的影响尚未探讨。 在此,我们在患者衍生的细胞中证明即使在杂合状态下,芬兰Abraxas1创始人突变(C.1082G> A,Arg361GlN)导致BRCA1蛋白质水平降低,以及BRCA1和CTIP的核定位和焦点形成。 这导致基础BRCA1-A复合定位的干扰,这被误差易用的DNA双链缓解途径使用中的约束反映,减弱了DNA损伤响应和DEERICOUD G2-M检查点控制。 目前的研究清楚地证明了芬兰Abraxas1创始人突变如何在BRCA1上以显性负面方式作用,以促进杂合载体细胞中的基因组错失。

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  • 来源
    《Human Molecular Genetics》 |2019年第24期|共14页
  • 作者

    Bose Muthiah; Sachsenweger Juliane; Laurila Niina; Parplys Ann Christin; Willmann Jonas; Jungwirth Johannes; Groth Marco; Rapakko Katrin; Nieminen Pentti; Friedl Thomas W. P.; Heiserich Lisa; Meyer Felix; Tuppurainen Hanna; Peltoketo Hellevi; Nevanlinna Heli; Pylkas Katri; Borgmann Kerstin; Wiesmueller Lisa; Winqvist Robert; Pospiech Helmut;

  • 作者单位

    Univ Oulu Bioctr Oulu Canc &

    Translat Med Res Unit Lab Canc Genet &

    Tumor Biol Oulu 90220;

    Univ Oulu Bioctr Oulu Canc &

    Translat Med Res Unit Lab Canc Genet &

    Tumor Biol Oulu 90220;

    Univ Oulu Bioctr Oulu Canc &

    Translat Med Res Unit Lab Canc Genet &

    Tumor Biol Oulu 90220;

    UCCH Univ Med Ctr Hamburg Eppendorf Lab Radiobiol &

    Expt Radiooncol D-20246 Hamburg Germany;

    UCCH Univ Med Ctr Hamburg Eppendorf Lab Radiobiol &

    Expt Radiooncol D-20246 Hamburg Germany;

    Leibniz Inst Aging Project Grp Biochem Fritz Lipmann Inst D-07745 Jena Germany;

    Leibniz Inst Aging Core Facil DNA Sequencing Fritz Lipmann Inst D-07745 Jena Germany;

    Northern Finland Lab Ctr Lab Genet NordLab Oulu Oulu 90220 Finland;

    Univ Oulu Dept Med Informat &

    Stat Oulu 90220 Finland;

    Ulm Univ Dept Obstet &

    Gynecol D-89075 Ulm Germany;

    Medipan GmbH D-15827 Dahlewitz Berlin Germany;

    UCCH Univ Med Ctr Hamburg Eppendorf Lab Radiobiol &

    Expt Radiooncol D-20246 Hamburg Germany;

    Univ Oulu Bioctr Oulu Canc &

    Translat Med Res Unit Lab Canc Genet &

    Tumor Biol Oulu 90220;

    Univ Oulu Bioctr Oulu Canc &

    Translat Med Res Unit Lab Canc Genet &

    Tumor Biol Oulu 90220;

    Univ Helsinki Dept Obstet &

    Gynecol Helsinki 00029 Finland;

    Univ Oulu Bioctr Oulu Canc &

    Translat Med Res Unit Lab Canc Genet &

    Tumor Biol Oulu 90220;

    UCCH Univ Med Ctr Hamburg Eppendorf Lab Radiobiol &

    Expt Radiooncol D-20246 Hamburg Germany;

    Ulm Univ Dept Obstet &

    Gynecol D-89075 Ulm Germany;

    Univ Oulu Bioctr Oulu Canc &

    Translat Med Res Unit Lab Canc Genet &

    Tumor Biol Oulu 90220;

    Leibniz Inst Aging Project Grp Biochem Fritz Lipmann Inst D-07745 Jena Germany;

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  • 正文语种 eng
  • 中图分类 医学遗传学;
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