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首页> 外文期刊>Apoptosis: An international journal on programmed cell death >mTOR is a fine tuning molecule in CDK inhibitors-induced distinct cell death mechanisms via PI3K/AKT/mTOR signaling axis in prostate cancer cells
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mTOR is a fine tuning molecule in CDK inhibitors-induced distinct cell death mechanisms via PI3K/AKT/mTOR signaling axis in prostate cancer cells

机译:mTOR是CDK抑制剂通过PI3K / AKT / mTOR信号传导轴在前列腺癌细胞中诱导的独特细胞死亡机制中的微调分子

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Purvalanol and roscovitine are cyclin dependent kinase (CDK) inhibitors that induce cell cycle arrest and apoptosis in various cancer cells. We further hypothesized that co-treatment of CDK inhibitors with rapamycin, an mTOR inhibitor, would be an effective combinatory strategy for the inhibition of prostate cancer regard to androgen receptor (AR) status due to inhibition of proliferative pathway, PI3K/AKT/mTOR, and induction of cell death mechanisms. Androgen responsive (AR+), PTEN-/- LNCaP and androgen independent (AR-), PTEN+/- DU145 prostate cancer cells were exposed to purvalanol (20 A mu M) and roscovitine (30 A mu M) with or without rapamycin for 24 h. Cell viability assay, immunoblotting, flow cytometry and fluorescence microscopy was used to define the effect of CDK inhibitors with or without rapamycin on proliferative pathway and cell death mechanisms in LNCaP and DU145 prostate cancer cells. Co-treatment of rapamycin modulated CDK inhibitors-induced cytotoxicity and apoptosis that CDK inhibitors were more potent to induce cell death in AR (+) LNCaP cells than AR (-) DU145 cells. CDK inhibitors in the presence or absence of rapamycin induced cell death via modulating upstream PI3K/AKT/mTOR signaling pathway in LNCaP cells, exclusively only treatment of purvalanol have strong potential to inhibit both upstream and downstream targets of mTOR in LNCaP and DU145 cells. However, co-treatment of rapamycin with CDK inhibitors protects DU145 cells from apoptosis via induction of autophagy mechanism. We confirmed that purvalanol and roscovitine were strong apoptotic and autophagy inducers that based on regulation of PI3K/AKT/mTOR signaling pathway. Co-treatment of rapamycin with purvalanol and roscovitine exerted different effects on cell survival and death mechanisms in LNCaP and DU145 cell due to their AR receptor status. Our studies show that co-treatment of rapamycin with CDK inhibitors inhibit prostate cancer cell viability more effectively than either agent alone, in part, by targeting the mTOR signaling cascade in AR (+) LNCaP cells. In this point, mTOR is a fine-tuning player in purvalanol and roscovitine-induced apoptosis and autophagy via regulation of PI3K/AKT and the downstream targets, which related with cell proliferation.
机译:嘌呤醇和roscovitine是细胞周期蛋白依赖性激酶(CDK)抑制剂,可诱导各种癌细胞的细胞周期停滞和凋亡。我们进一步假设CDK抑制剂与雷帕霉素(mTOR抑制剂)共同治疗将是一种抑制前列腺癌的有效组合策略,因为它通过抑制增殖途径PI3K / AKT / mTOR来抑制雄激素受体(AR)的状态,和诱导细胞死亡机制。将雄激素反应性(AR +),PTEN-/-LNCaP和雄激素非依赖性(AR-),PTEN +/- DU145前列腺癌细胞暴露于含有或不含有雷帕霉素的嘌呤醇(20 AμM)和roscovitine(30 AμM)中24 H。细胞生存力测定,免疫印迹,流式细胞术和荧光显微镜术用于定义含或不含雷帕霉素的CDK抑制剂对LNCaP和DU145前列腺癌细胞增殖途径和细胞死亡机制的影响。雷帕霉素调节的CDK抑制剂共同治疗诱导的细胞毒性和细胞凋亡,即CDK抑制剂比AR(-)DU145细胞更有效地诱导AR(+)LNCaP细胞死亡。在存在或不存在雷帕霉素的情况下,CDK抑制剂可通过调节LNCaP细胞中的上游PI3K / AKT / mTOR信号通路来诱导细胞死亡,仅对紫苏醇的处理具有强大的潜力,可抑制LNCaP和DU145细胞中mTOR的上游和下游靶标。但是,雷帕霉素与CDK抑制剂的共处理可通过诱导自噬机制保护DU145细胞免于凋亡。我们证实,基于PI3K / AKT / mTOR信号传导通路的调节,嘌呤醇和roscovitine是强凋亡和自噬诱导剂。雷帕霉素与戊醇和roscovitine的共处理对LNCaP和DU145细胞的AR受体状态起着不同的细胞存活和死亡机制的作用。我们的研究表明,雷帕霉素与CDK抑制剂的共同治疗比单独使用任一种药物更有效地抑制了前列腺癌细胞的生存,部分是通过靶向AR(+)LNCaP细胞中的mTOR信号级联。在这一点上,mTOR是通过调节PI3K / AKT和下游靶标(与细胞增殖有关)而在嘌呤醇和roscovitine诱导的细胞凋亡和自噬中的微调参与者。

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