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首页> 外文期刊>Translational Oncology >PI3K Inhibition Augments the Therapeutic Efficacy of a 3a-aza-Cyclopenta[α]indene Derivative in Lung Cancer Cells
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PI3K Inhibition Augments the Therapeutic Efficacy of a 3a-aza-Cyclopenta[α]indene Derivative in Lung Cancer Cells

机译:PI3K抑制增强3a-氮杂-环戊[α]茚满衍生物在肺癌细胞中的治疗功效。

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摘要

The synergistic targeting of DNA damage and DNA repair is a promising strategy for the development of new chemotherapeutic agents for human lung cancer. The DNA interstrand cross-linking agent BO-1509, a derivative of 3a-aza-cyclopenta[α]indene, was synthesized and combined with the phosphoinositide 3-kinase (PI3K) inhibitor LY294002 to treat human lung cancer cells. Our results showed that the BO-1509 and LY294002 combination synergistically killed lung cancer cells in culture and also suppressed the growth of lung cancer xenografts in mice, including those derived from gefitinib-resistant cells. We also found that LY294002 suppressed the induction of several DNA repair proteins by BO-1509 and inhibited the nuclear translocation of Rad51. On the basis of the results of the γH2AX foci formation assays, LY294002 apparently inhibited the repair of DNA damage that was induced by BO-1509. According to the complete blood profile, biochemical enzyme analysis, and histopathologic analysis of major organs, no apparent toxicity was observed in mice treated with BO-1509 alone or in combination with LY294002. Our results suggest that the combination of a DNA cross-linking agent with a PI3K inhibitor is a feasible strategy for the treatment of patients with lung cancer.
机译:DNA损伤和DNA修复的协同靶向是开发用于人类肺癌的新化学治疗剂的有前途的策略。合成了DNA链交联剂BO-1509,它是3a-氮杂-环戊达[α]茚的衍生物,并与磷酸肌醇3-激酶(PI3K)抑制剂LY294002结合使用,可治疗人肺癌细胞。我们的结果表明,BO-1509和LY294002组合可协同杀死培养中的肺癌细胞,并且还抑制了小鼠肺癌异种移植物的生长,包括那些来自吉非替尼耐药细胞的异种移植物。我们还发现LY294002抑制了BO-1509对几种DNA修复蛋白的诱导,并抑制了Rad51的核易位。根据γH2AX灶形成分析的结果,LY294002明显抑制了BO-1509诱导的DNA损伤的修复。根据完整的血液概况,主要器官的生化酶分析和组织病理学分析,在单独用BO-1509或与LY294002组合治疗的小鼠中未观察到明显的毒性。我们的结果表明,DNA交联剂与PI3K抑制剂的组合是治疗肺癌患者的可行策略。

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