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首页> 外文期刊>British Journal of Cancer >Gene therapy with SOCS1 for gastric cancer induces G2/M arrest and has an antitumour effect on peritoneal carcinomatosis
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Gene therapy with SOCS1 for gastric cancer induces G2/M arrest and has an antitumour effect on peritoneal carcinomatosis

机译:SOCS1的胃癌基因疗法可诱导G2 / M阻滞并对腹膜癌具有抗肿瘤作用

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Background: Suppressor of cytokine signaling1 (SOCS1) is a negative regulator of various cytokines. Recently, it was investigated as a therapeutic target in various cancers. However, the observed antitumour effects of SOCS1 cannot not be fully explained without taking inhibition of proliferation signalling into account. Our aim was to discover a new mechanism of antitumour effects of SOCS1 for gastric cancer (GC). Methods: We analysed the mechanism of antitumour effect of SOCS1 in vitro. In addition, we evaluated antitumour effect for GC using a xenograft peritoneal carcinomatosis mouse model in preclinical setting. Results: We confirmed that SOCS1 suppressed proliferation in four out of five GC cell lines. SOCS1 appeared to block proliferation by a new mechanism that involves cell cycle regulation at the G2/M checkpoint. We showed that SOCS1 influenced cell cycle-associated molecules through its interaction with ataxia telangiectasia and Rad3-related protein. The significant difference in therapeutic effects was noted in terms of the post-treatment weight and total photon count of the intra-abdominal tumours. Conclusion: Forced expression of SOCS1 revealed a heretofore-unknown mechanism for regulating the cell cycle and may represent a novel therapeutic approach for the treatment of peritoneal carcinomatosis of GC.
机译:背景:细胞因子信号传导1(SOCS1)的抑制因子是各种细胞因子的负调节剂。最近,已经研究了它作为各种癌症的治疗靶标。但是,如果不考虑抑制增殖信号,就不能完全解释所观察到的SOCS1的抗肿瘤作用。我们的目的是发现SOCS1对胃癌(GC)的抗肿瘤作用的新机制。方法:我们分析了SOCS1体外抗肿瘤作用的机制。此外,我们在临床前环境中使用异种移植腹膜癌小鼠模型评估了GC的抗肿瘤作用。结果:我们确认SOCS1抑制了五分之四的GC细胞系的增殖。 SOCS1似乎是通过一种涉及G2 / M检查点的细胞周期调控的新机制来阻止增殖。我们表明SOCS1通过与共济失调毛细血管扩张和Rad3相关蛋白的相互作用影响细胞周期相关的分子。在治疗后体重和腹腔内肿瘤的总光子计数方面,注意到治疗效果的显着差异。结论:强迫表达SOCS1揭示了调控细胞周期的未知机制,可能代表了一种治疗胃癌腹膜癌的新方法。

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