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Heterozygous mutations cause genetic instability in a yeast model of cancer evolution

机译:杂合突变导致癌症进化的酵母模型中的遗传不稳定

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摘要

Genetic instability, a heritable increase in the rate of genetic mutation, accelerates evolutionary adaptation(1) and is widespread in cancer(2,3). In mammals, instability can arise from damage to both copies of genes involved in DNA metabolism and cell cycle regulation(4) or from inactivation of one copy of a gene whose product is present in limiting amounts (haploinsufficiency(5)); however, it has proved difficult to determine the relative importance of these two mechanisms. In Escherichia coli(6), the application of repeated, strong selection enriches for genetic instability. Here we have used this approach to evolve genetic instability in diploid cells of the budding yeast Saccharomyces cerevisiae, and have isolated clones with increased rates of point mutation, mitotic recombination, and chromosome loss. We identified candidate, heterozygous, instability-causing mutations; engineering these mutations, as heterozygotes, into the ancestral diploid strain caused genetic instability. Mutations that inactivated one copy of haploinsufficient genes were more common than those that dominantly altered the function of the mutated gene copy. The mutated genes were enriched for genes functioning in transport, protein quality control, and DNA metabolism, and have revealed new targets for genetic instability(7-11), including essential genes. Although only a minority (10 out of 57 genes with orthologues or close homologues) of the targets we identified have homologous human genes that have been implicated in cancer(2), the remainder are candidates to contribute to human genetic instability. To test this hypothesis, we inactivated six examples in a near-haploid human cell line; five of these mutations increased instability. We conclude that single genetic events cause genetic instability in diploid yeast cells, and propose that similar, heterozygous mutations in mammalian homologues initiate genetic instability in cancer.
机译:遗传不稳定性是遗传突变率的可遗传增加,可加速进化适应(1),并广泛分布于癌症中(2,3)。在哺乳动物中,不稳定性可能是由于参与DNA代谢和细胞周期调节的基因的两个拷贝受到破坏(4),或者是由于其产物以有限量存在的一个拷贝的基因被灭活(单倍不足(5));然而,事实证明很难确定这两种机制的相对重要性。在大肠杆菌(6)中,重复,强力选择的应用丰富了基因的不稳定性。在这里,我们已经使用这种方法来进化出芽酵母酿酒酵母的二倍体细胞中的遗传不稳定性,并分离出了具有点突变,有丝分裂重组和染色体丢失率增加的克隆。我们确定了候选的,杂合的,引起不稳定的突变;将这些突变作为杂合子工程化到祖先二倍体菌株中,导致遗传不稳定。灭活一个单倍基因不足的基因拷贝的突变比那些显着改变突变基因拷贝功能的突变更为普遍。突变的基因丰富了在运输,蛋白质质量控​​制和DNA代谢中起作用的基因,并揭示了遗传不稳定性的新靶标(7-11),包括必需基因。尽管我们确定的靶标中只有少数(57个具有直向同源物或紧密同源物的基因中的10个)具有与癌症有关的同源人类基因(2),但其余的候选物可能导致人类遗传不稳定。为了验证这一假设,我们在一个接近单倍体的人类细胞系中失活了六个实例。这些突变中有五个增加了不稳定性。我们得出的结论是,单个遗传事件会导致二倍体酵母细胞中的遗传不稳定,并提出哺乳动物同源物中类似的杂合突变会引发癌症的遗传不稳定。

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  • 来源
    《Nature》 |2019年第7743期|275-278|共4页
  • 作者单位

    Harvard Univ, FAS Ctr Syst Biol, Cambridge, MA 02138 USA;

    Harvard Univ, Mol & Cell Biol, Cambridge, MA 02138 USA;

    Harvard Med Sch, Dept Neurol, Boston, MA USA;

    Massachusetts Gen Hosp, Ctr Genom Med, Boston, MA 02114 USA;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
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  • 正文语种 eng
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