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首页> 外文期刊>Molecular and Cellular Biology >The RASSF1A Isoform of RASSF1 Promotes Microtubule Stability and Suppresses Tumorigenesis
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The RASSF1A Isoform of RASSF1 Promotes Microtubule Stability and Suppresses Tumorigenesis

机译:RASSF1A的RASSF1A亚型可促进微管稳定性并抑制肿瘤发生。

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摘要

The RASSF1A isoform of RASSF1 is frequently inactivated by epigenetic alterations in human cancers, but it remains unclear if and how it acts as a tumor suppressor. RASSF1A overexpression reduces in vitro colony formation and the tumorigenicity of cancer cell lines in vivo. Conversely, RASSF1A knockdown causes multiple mitotic defects that may promote genomic instability. Here, we have used a genetic approach to address the function of RASSF1A as a tumor suppressor in vivo by targeted deletion of Rassf1A in the mouse. Rassf1A null mice were viable and fertile and displayed no pathological abnormalities. Rassf1A null embryonic fibroblasts displayed an increased sensitivity to microtubule depolymerizing agents. No overtly altered cell cycle parameters or aberrations in centrosome number were detected in Rassf1A null fibroblasts. Rassf1A null fibroblasts did not show increased sensitivity to microtubule poisons or DNA-damaging agents and showed no evidence of gross genomic instability, suggesting that cellular responses to genotoxins were unaffected. Rassf1A null mice showed an increased incidence of spontaneous tumorigenesis and decreased survival rate compared with wild-type mice. Irradiated Rassf1A null mice also showed increased tumor susceptibility, particularly to tumors associated with the gastrointestinal tract, compared with wild-type mice. Thus, our results demonstrate that Rassf1A acts as a tumor suppressor gene.
机译:在人类癌症中, RASSF1 RASSF1A 亚型经常被表观遗传改变所灭活,但尚不清楚它是否以及如何充当肿瘤抑制因子。 RASSF1A的过表达减少了体外菌落的形成和体内癌细胞系的致瘤性。相反,RASSF1A敲低会导致多个有丝分裂缺陷,可能会促进基因组不稳定。在这里,我们已经使用一种遗传学方法通过在小鼠中有针对性地删除 Rassf1A 来解决RASSF1A作为体内肿瘤抑制因子的功能。 Rassf1A 无效小鼠存活且可育,未显示任何病理异常。 Rassf1A 空胚成纤维细胞对微管解聚剂的敏感性增加。在 Rassf1A 无效成纤维细胞中未检测到明显改变的细胞周期参数或中心体数目畸变。 Rassf1A 无效的成纤维细胞未显示出对微管中毒或DNA破坏剂的敏感性增加,也未显示出明显的基因组不稳定性证据,表明细胞对基因毒素的反应未受影响。与野生型小鼠相比, Rassf1A 缺失小鼠自发肿瘤发生率增加,成活率降低。与野生型小鼠相比,受辐射的 Rassf1A 无效小鼠也显示出更高的肿瘤易感性,尤其是与胃肠道相关的肿瘤。因此,我们的结果证明 Rassf1A 可以作为抑癌基因。

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