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首页> 外文期刊>Journal of oncology >Genotypic and Phenotypic Variables Affect Meiotic Cell Cycle Progression, Tumor Ploidy, and Cancer-Associated Mortality in a brca2-Mutant Zebrafish Model
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Genotypic and Phenotypic Variables Affect Meiotic Cell Cycle Progression, Tumor Ploidy, and Cancer-Associated Mortality in a brca2-Mutant Zebrafish Model

机译:基因型和表型变量影响BRCA2-突变体斑马鱼模型中的减数分裂细胞周期进展,肿瘤倍性和癌症相关的死亡率

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Successful cell replication requires both cell cycle completion and accurate chromosomal segregation. The tumor suppressor BRCA2 is positioned to influence both of these outcomes, and thereby influence genomic integrity, during meiotic and mitotic cell cycles. Accordingly, mutations in BRCA2 induce chromosomal abnormalities and disrupt cell cycle progression in both germ cells and somatic cells. Despite these findings, aneuploidy is not more prevalent in BRCA2-associated versus non-BRCA2-associated human cancers. More puzzlingly, diploidy in BRCA2-associated cancers is a negative prognostic factor, unlike non-BRCA2-associated cancers and many other human cancers. We used a brca2-mutant/tp53-mutant cancer-prone zebrafish model to explore the impact of BRCA2 mutation on cell cycle progression, ploidy, and cancer-associated mortality by performing DNA content/cell cycle analysis on zebrafish germ cells, somatic cells, and cancer cells. First, we determined that combined brca2/tp53 mutations uniquely disrupt meiotic progression. Second, we determined that sex significantly influences ploidy outcome in zebrafish cancers. Third, we determined that brca2 mutation and female sex each significantly reduce survival time in cancer-bearing zebrafish. Finally, we provide evidence to support a link between BRCA2 mutation, tumor diploidy, and poor survival outcome. These outcomes underscore the utility of this model for studying BRCA2-associated genomic aberrations in normal and cancer cells.
机译:成功的细胞复制需要细胞周期完成和准确的染色体偏析。肿瘤抑制剂BRCA2定位以影响这些结果,从而影响减少病毒和有丝分裂细胞循环期间的基因组完整性。因此,BRCA2中的突变诱导染色体异常并破坏胚芽细胞和体细胞中的细胞周期进展。尽管存在这些发现,但在BRCA2相关的与非BRCA2相关人类癌症中不再普遍。更令人困惑的是,BRCA2相关癌症的代号是阴性预后因素,与非BRCA2相关的癌症和许多其他人类癌症不同。我们使用了BRCA2-突变体/ TP53-突变癌症 - 易于斑点模型,以探讨BRCA2突变对细胞周期进展,倍增性和癌症相关的死亡率的影响,通过对斑马鱼生殖细胞,体细胞进行DNA含量/细胞循环分析,和癌细胞。首先,我们确定合并BRCA2 / TP53突变唯一地破坏了减少人民进展。其次,我们确定性别显着影响斑马鱼癌症的倍增性结果。第三,我们确定BRCA2突变和女性各自显着降低患癌症斑马鱼的生存时间。最后,我们提供证据支持BRCA2突变,肿瘤子系统和生存差的结果之间的联系。这些结果强调了该模型用于研究正常和癌细胞中BRCA2相关基因组畸变的效用。

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