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The phytohormone forchlorfenuron decreases viability and proliferation of malignant mesothelioma cells in vitro and in vivo

机译:氯芬隆的植物激素会降低体内和体外恶性间皮瘤细胞的活力和增殖

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摘要

Malignant mesothelioma (MM) is one of the most aggressive cancer types with a patient’s life expectancy of typically less than one year upon diagnosis. The urgency of finding novel therapeutic approaches to treat mesothelioma is evident. Here we tested the effect of the plant-growth regulator forchlorfenuron (FCF), an inhibitor of septin function(s) in mammalian cells, on the viability and proliferation of MM cell lines, as well as other tumor cell lines derived from lung, prostate, colon, ovary, cervix and breast. Exposure to FCF strongly inhibited proliferation of human and mouse (most efficiently epithelioid) MM cells and all other tumor cells in a concentration-dependent manner and led to cell cycle arrest and cell death. The role of septin 7 ( ), a presumably essential target of FCF in MM cells was confirmed by an shRNA strategy. FCF was robustly inhibiting tumor cell growth at low micromolar (IC : ≈20-60µM) concentrations and more promisingly also . Initial experiments with FCF analogous revealed the importance of FCF’s chloride group for efficient cell growth inhibition. FCF’s rather low systemic toxicity might warrant for an extended search for other related and possibly more potent FCF analogues to target MM and putatively other septin-dependent tumors.
机译:恶性间皮瘤(MM)是最具侵略性的癌症类型之一,诊断后患者的平均寿命通常不到一年。寻找新颖的治疗间皮瘤的方法的迫切性是显而易见的。在这里,我们测试了氯芬脲(FCF)的植物生长调节剂,一种哺乳动物细胞中septin功能的抑制剂,对MM细胞系以及其他源自肺,前列腺的肿瘤细胞系的活力和增殖的影响,结肠,卵巢,子宫颈和乳房。暴露于FCF会以浓度依赖性方式强烈抑制人和小鼠(最有效的上皮样)MM细胞和所有其他肿瘤细胞的增殖,并导致细胞周期停滞和细胞死亡。 shRNA策略证实了Septin 7()(可能是FCF在MM细胞中的重要靶标)的作用。 FCF在低微摩尔(IC:≈20-60µM)浓度下能强有力地抑制肿瘤细胞的生长,而且也很有希望。最初的FCF类似物实验揭示了FCF的氯基对于有效抑制细胞生长的重要性。 FCF的全身毒性较低,可能需要进一步寻找其他相关且可能更有效的FCF类似物,以靶向MM和其他可能依赖Septin的肿瘤。

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