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首页> 外文期刊>Anti-cancer drugs >Ginsenoside Rg1 impairs homologous recombination repair by targeting CtBP-interacting protein and sensitizes hepatoblastoma cells to DNA damage
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Ginsenoside Rg1 impairs homologous recombination repair by targeting CtBP-interacting protein and sensitizes hepatoblastoma cells to DNA damage

机译:人参皂甙RG1通过靶向CTBP - 相互作用蛋白来损害同源重组修复,并使肝细胞瘤细胞敏感到DNA损伤

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摘要

The ginsenoside Rg1, the primary pharmacologically active ingredient of the traditional Chinese herb ginseng, is widely used in the clinical treatment of diseases of the immune and nervous systems. Recent studies have shown that it also has an antitumor effect. In this study, we explored the effects of Rg1 on hepatoblastoma (HB) and its underlying mechanisms. We demonstrated that Rg1 significantly inhibited HB cell growth both in vivo and in vitro . Mechanistic studies revealed that Rg1 impaired homologous recombination and triggered double-strand breaks in HB cells by directly targeting CtBP-interacting protein (CtIP), a key double-strand break repair factor, which is highly expressed in HB tissues. Moreover, we also demonstrated that Rg1 sensitized HB cells to DNA-damaging agents both in vitro and in vivo . In conclusion, our data not only demonstrate the potential clinical application of Rg1 as a novel chemotherapeutic candidate but also offer a mechanism-based therapeutic option by which DNA-damaging agents can be used in combination with Rg1 to target HB.
机译:人参皂苷Rg1,中草参的主要药理学活性成分,广泛应用于免疫和神经系统疾病的临床治疗。最近的研究表明它还具有抗肿瘤效应。在这项研究中,我们探讨了RG1对肝气肿(HB)及其潜在机制的影响。我们证明RG1显着抑制体内和体外的HB细胞生长。机械研究表明,通过直接靶向CTBP相互作用蛋白(CTIP),RG1损伤的同源重组和触发的双链在Hb细胞中断裂,键双链断裂修复因子,其在HB组织中高度表达。此外,我们还证明RG1敏化HB细胞在体外和体内致DNA损伤剂。总之,我们的数据不仅证明了RG1作为新型化学治疗性候选者的潜在临床应用,而且还提供基于机制的治疗选择,通过该方法可以与RG1组合使用DNA损伤剂来靶向HB。

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