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Synergistic effects of cisplatin-caffeic acid induces apoptosis in human cervical cancer cells via the mitochondrial pathways

机译:顺铂 - 咖啡酸的协同作用通过线粒体途径诱导人宫颈癌细胞细胞凋亡

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Cervical cancer (CxCa) is a major health problem globally and is associated with the presence of human papillomavirus infection. Cisplatin (CDDP) is a platinum-based chemotherapeutic agent. Owing to its side effects and drug-resistance, novel anticancer agents with lower toxicity, including caffeic acid (CFC), are of interest. However, the effects of CDDP and CFC in combination are, to the best of our knowledge, uninvestigated. The present study investigated the effectiveness of CDDP and CFC in combination and its mechanism of action on four human cervical cancer cell lines, which were compared with the Chlorocebus sabaeus normal kidney Vero cell line. Cell viability was evaluated using a sulforhodamine B assay. Caspase-Glo assay kits, measuring the activity of caspases-3, -7, -8 and -9, were used to detect caspase activation in HeLa and CaSki cell lines in response to CDDP and CFC in combination. The results revealed that CDDP and CFC alone reduced the proliferation of HeLa, CaSki, SiHa and C33A cell lines. Treatment with CFC exhibited no significant cytotoxicity towards Vero cells. In addition, CDDP-CFC significantly inhibited cell growth of HeLa and CaSki cell lines. In HeLa and CaSki cell lines, a combination index <1 for CDDP and CFC indicated the synergistic growth inhibition; the combination of the two also significantly increased expression of caspase-3, -7 and -9. In conclusion, CFC may be a candidate anticancer agent that, when use in combination, may increase the therapeutic efficacy of CDDP.
机译:宫颈癌(CXCA)是全球的主要健康问题,与人乳头瘤病毒感染的存在有关。顺铂(CDDP)是一种基于铂的化学治疗剂。由于其副作用和耐药性,具有较低毒性的新型抗癌剂,包括咖啡酸(CFC),是感兴趣的。然而,据我们所知,CDDP和CFC组合的影响是未投用的。本研究研究了CDDP和CFC的有效性及其对四种人类宫颈癌细胞系的作用机制,与氯霉素常规肾脉络细胞系进行了比较。使用苏尔磺胺胺B测定法评估细胞活力。 Caspase-Glo测定试剂盒,测量Caspases-3,-7,-8和-9的活性,用于检测HeLa和Caski细胞系中的Caspase活化,响应CDDP和CFC组合。结果表明,CDDP和CFC单独降低了HeLa,Caski,Siha和C33a细胞系的增殖。用CFC治疗对Vero细胞没有显着的细胞毒性。此外,CDDP-CFC显着抑制了HeLa和Caski细胞系的细胞生长。在Hela和Caski细胞系中,CDDP和CFC的组合指数<1表示协同生长抑制;两者的组合也显着增加了Caspase-3,-7和-9的表达。总之,CFC可以是候选抗癌剂,即在组合使用时,可以增加CDDP的治疗效果。

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