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首页> 外文期刊>In Vitro Cellular and Developmental Biology. Animal: Journal of the Tissues Culture Association >In vitro evaluation of combination of EGCG and Erlotinib with classical chemotherapeutics on JAR cells
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In vitro evaluation of combination of EGCG and Erlotinib with classical chemotherapeutics on JAR cells

机译:在罐细胞上对古典化学治疗剂EGCG和ERLOTINIB结合的体外评价

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摘要

Gestational Trophoblastic Neoplasia (GTN) is a term used for a group of malignant gynecological tumors including choriocarcinoma. Low-risk neoplasias can be cured using single agents Methotrexate (MTX) and actinomycin-D(ACD), but in certain cases, decreased responsiveness and serious side effects occur. Therefore, researchers have been attempting to find new treatment modalities. One of the most popular way for increasing cancer patient survival rates is supporting treatment with adjuvant molecules or chemosensitizers. For this purpose, we investigated epigallocatechin-3-gallate (EGCG), a green tea cathecin, and Erlotinib, an EGFR tyrosine kinase inhibitor, as single agents and combined with MTX or ACD. In accordance with this, JAR (human placenta choriocarcinoma) cell line was used as an in vitro model and MTT, LDH, caspase-3 activation, RT-PCR, and Western Blot analyses were performed to investigate the effects of the test materials. Our studies demonstrate that combination of Erlotinib and EGCG with MTX and ACD decreases JAR cell proliferation and metastatic HER2 protein synthesis and increases caspase-3 activation compared to ACD orMTX alone. In addition, significant increase was observed in the apoptotic Bax gene, but no notable protein synthesis occurred in the Western Blot analysis, which suggests that combination of Erlotinib and EGCG with classical chemotherapeutics ACD or MTX may lead the JAR cells to apoptosis, but not by a mitochondrial pathway. All the results indicate that the synergetic effect of Erlotinib and EGCG with classical chemotherapeutics may help to increase patient survival rates of choriocarcinoma, but the detailed mechanism needs further investigation.
机译:妊娠滋养细胞瘤形成(GTN)是用于一组恶性妇科肿瘤,包括胆碱癌的术语。低风险的肿瘤可以使用单一剂甲氨蝶呤(MTX)和放线霉素-D(ACD)来治愈,但在某些情况下,发生响应性和严重副作用。因此,研究人员一直试图找到新的治疗方式。增加癌症患者存活率的最受欢迎的方式之一是用佐剂分子或化学化剂支持治疗。为此目的,我们研究了EpigallocaTechin-3-gallate(EGCG),绿茶料中和厄洛替尼,EGFR酪氨酸激酶抑制剂,作为单一剂,并与MTX或ACD合并。根据此,进行罐(人胎盘胆碱瘤)细胞系用作体外模型和MTT,LDH,Caspase-3活化,RT-PCR和Western印迹分析以研究测试材料的影响。我们的研究表明,Erlotinib和EGCG与MTX和ACD的组合降低了罐细胞增殖和转移性HER2蛋白合成,并与单独的ACD OrmTX相比增加了Caspase-3活化。此外,在凋亡BAX基因中观察到显着增加,但Western印迹分析中没有出现显着的蛋白质合成,这表明Erlotinib和EGCG与古典化学治疗剂ACD或MTX的组合可以引导罐细胞对细胞凋亡,但不是通过线粒体途径。所有结果表明,Erlotinib和EGCG与古典化学治疗剂的协同作用可能有助于提高患者的胆管癌的存活率,但细化机制需要进一步调查。

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