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首页> 外文期刊>Marine Drugs >Activation of the Tumor Suppressor PP2A Emerges as a Potential Therapeutic Strategy for Treating Prostate Cancer
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Activation of the Tumor Suppressor PP2A Emerges as a Potential Therapeutic Strategy for Treating Prostate Cancer

机译:肿瘤抑制物PP2A的激活成为治疗前列腺癌的潜在治疗策略。

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摘要

Protein phosphatase 2A (PP2A) is a tumor suppressor complex that has recently been reported as a novel and highly relevant molecular target in prostate cancer (PCa). However, its potential therapeutic value remains to be fully clarified. We treated PC-3 and LNCaP cell lines with the PP2A activators forskolin and FTY720 alone or combined with the PP2A inhibitor okadaic acid. We examined PP2A activity, cell growth, prostasphere formation, levels of PP2A phosphorylation, CIP2A and SET expression, and AKT and ERK activation. Interestingly, both forskolin and FTY720 dephosphorylated and activated PP2A, impairing proliferation and prostasphere formation and inducing changes in AKT and ERK phosphorylation. Moreover, FTY720 led to reduced CIP2A levels. Treatment with okadaic acid impaired PP2A activation thus demonstrating the antitumoral PP2A-dependent mechanism of action of both forskolin and FTY720. Levels of PP2A phosphorylation together with SET and CIP2A protein expression were studied in 24 PCa patients and both were associated with high Gleason scores and presence of metastatic disease. Altogether, our results suggest that PP2A inhibition could be involved in PCa progression, and the use of PP2A-activating drugs might represent a novel alternative therapeutic strategy for treating PCa patients.
机译:蛋白磷酸酶2A(PP2A)是一种肿瘤抑制复合物,最近被报道为前列腺癌(PCa)中一种新颖且高度相关的分子靶标。但是,其潜在的治疗价值仍有待充分阐明。我们用单独的PP2A激活剂福司高林和FTY720或与PP2A抑制剂冈田酸联合处理PC-3和LNCaP细胞系。我们检查了PP2A活性,细胞生长,前球体形成,PP2A磷酸化水平,CIP2A和SET表达以及AKT和ERK激活。有趣的是,福司高林和FTY720都对PP2A进行了去磷酸化和活化,从而损害了增殖和前列腺素的形成,并诱导了AKT和ERK磷酸化的改变。此外,FTY720降低了CIP2A水平。冈田酸处理损害了PP2A的活化,因此证明了福司高林和FTY720的抗肿瘤PP2A依赖性作用机制。在24位PCa患者中研究了PP2A磷酸化水平以及SET和CIP2A蛋白表达,二者均与高Gleason评分和转移性疾病的存在有关。总之,我们的结果表明,PP2A抑制可能与PCa的进展有关,使用PP2A激活药物可能代表了治疗PCa患者的新型替代治疗策略。

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