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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >HPP1-mediated tumor suppression requires activation of STAT1 pathways.
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HPP1-mediated tumor suppression requires activation of STAT1 pathways.

机译:HPP1介导的肿瘤抑制需要激活STAT1途径。

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摘要

HPP1 is a recently discovered gene that is epigenetically silenced in a number of tumor types, suggesting a potential role as a tumor suppressor. However, whether HPP1 has tumor suppressor activity is not clearly known. We have sought to investigate the effects of HPP1 on tumor growth and survival and to identify signaling pathways that mediate HPP1's mechanism of action. Forced expression of HPP1 into HCT116 colon cancer cell lines blocked the ability of HCT116 tumors to grown in vivo in nude mice. In cell culture, ectopic expression of HPP1 induces apoptosis and potently inhibits soft agar colony formation. HPP1 overexpression was also associated with a moderate reduction in in vitro proliferation characterized by an accumulation of cells in the G0/G1 phase of the cell cycle. Microarray analysis revealed that ectopic expression of HPP1 resulted in a dramatic upregulation of STAT1 as well as a large number of associated interferon-inducible genes. RNA interference-mediated abrogation of STAT1 reversedHPP1's antiproliferative effects. We conclude that HPP1 demonstrates tumor suppressive and pro-apoptotic activity, both in vitro and in vivo. Coupled with its inactivation in a number of tumor types, our data provides evidence to support the role of HPP1 as a tumor suppressor gene. Moreover, activation of the STAT1 pathway likely represents the principal mediator of HPP1's tumor suppressive properties.
机译:HPP1是最近发现的一种基因,在许多类型的肿瘤中均在表观遗传上沉默,这表明它可能具有抑癌作用。但是,HPP1是否具有抑癌活性尚不清楚。我们试图研究HPP1对肿瘤生长和存活的影响,并确定介导HPP1作用机制的信号通路。 HPP1在HCT116结肠癌细胞系中的强制表达阻止了HCT116肿瘤在裸鼠体内体内生长的能力。在细胞培养中,HPP1的异位表达可诱导凋亡并有效抑制软琼脂菌落的形成。 HPP1的过表达还与体外增殖的适度降低有关,其特征是细胞在细胞周期的G0 / G1期积累。微阵列分析表明,HPP1的异位表达导致STAT1以及许多相关干扰素诱导基因的显着上调。 RNA干扰介导的STAT1的废除逆转了HPP1的抗增殖作用。我们得出的结论是,HPP1在体外和体内均表现出肿瘤抑制和促凋亡活性。加上其在多种肿瘤类型中的失活,我们的数据提供了支持HPP1作为肿瘤抑制基因的作用的证据。此外,STAT1途径的激活可能代表了HPP1肿瘤抑制特性的主要介质。

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