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Survivin stable knockdown by siRNA inhibits tumor cell growth and angiogenesis in breast and cervical cancers.

机译:siRNA对Survivin的稳定抑制作用抑制了乳腺癌和宫颈癌中肿瘤细胞的生长和血管生成。

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Increased resistance to apoptosis is a hallmark of many tumor cells. Survivin, a member of IAP family protein, is expressed in many human cancers and plays an important role in protecting cells from apoptosis. Here we show that vector-based small interfering RNAs (siRNA) stably knockdown survivin expression in several cancer cell lines, leading to increased apoptotic rate in response to different proapoptotic stimuli, such as doxorubicin or TNF-alpha. The apoptotic susceptibility was dependent on divergent levels of survivin expression. The stable transfectants exhibited abnormal morphology, suppressed cell growth, enhanced spontaneous apoptosis and cell cycle hindrance. Furthermore, in nude mice xenografts of survivin-positive tumors, cells expressing survivin-targeted siRNAs exhibited decreased tumor formation and reduced angiogenesis. Results from these studies: (1) provide direct evidence that intracellular silencing of survivin by siRNA sensitizes human tumor cells to apoptosis; (2) define survivin as a promising molecular target for cancer therapy; and (3) suggest the potential applicability of survivin-targeted siRNA for treating human tumors, probably in combination with chemotherapy.
机译:对凋亡的抵抗力增加是许多肿瘤细胞的标志。 Survivin是IAP家族蛋白的成员,在许多人类癌症中都有表达,并且在保护细胞免于凋亡方面起着重要作用。在这里,我们显示了基于载体的小干扰RNA(siRNA)在几种癌细胞系中稳定敲低survivin表达,从而导致对不同促凋亡刺激物(例如阿霉素或TNF-α)的凋亡率增加。凋亡敏感性取决于survivin表达的不同水平。稳定的转染子表现出异常的形态,抑制的细胞生长,增强的自发凋亡和细胞周期障碍。此外,在裸鼠存活蛋白阳性肿瘤的异种移植中,表达以存活蛋白为靶标的siRNA的细胞表现出减少的肿瘤形成和减少的血管生成。这些研究的结果:(1)提供直接证据表明,siRNA对survivin的细胞内沉默可使人肿瘤细胞对细胞凋亡敏感; (2)将生存素定义为癌症治疗的有希望的分子靶标; (3)提示以survivin为靶标的siRNA可能与化学疗法联合用于治疗人类肿瘤。

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