首页> 美国卫生研究院文献>Biomolecules >The Phytochemical Indicaxanthin Synergistically Enhances Cisplatin-Induced Apoptosis in HeLa Cells via Oxidative Stress-Dependent p53/p21waf1 Axis
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The Phytochemical Indicaxanthin Synergistically Enhances Cisplatin-Induced Apoptosis in HeLa Cells via Oxidative Stress-Dependent p53/p21waf1 Axis

机译:通过氧化应激依赖性P53 / P21WAF1轴协同增强HeLa细胞中的顺铂诱导的顺铂诱导的细胞凋亡

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摘要

Combining phytochemicals with chemotherapics is an emerging strategy to treat cancer to overcome drug toxicity and resistance with natural compounds. We assessed the effects of indicaxanthin (Ind), a pigment obtained from (L. Mill) fruit, combined with cisplatin (CDDP) against cervical cancer cells (HeLa). Measured cell viability via Trypan blue assay; cell morphology via fluorescence microscopy; apoptosis, cell cycle, mitochondrial membrane potential (MMP) and cell redox balance via flow-cytometry; expression levels of apoptosis-related proteins via western blot. Cell viability assays and Chou-Talalay plot demonstrated that the combination of CDDP and Ind had synergistic cytotoxic effects. Combined treatment had significant effects ( < 0.05) on phosphatidylserine externalization, cell morphological changes, cell cycle arrest, fall in MMP, ROS production and GSH decay compared with the individual treatment groups. Bax, cytochrome c, p53 and p21 were over-expressed, while Bcl-2 was downregulated. Pre-treatment with N-acetyl-l-cysteine abolished the observed synergistic effects. We also demonstrated potentiation of CDDP anticancer activity by nutritionally relevant concentrations of Ind. Oxidative stress-dependent mitochondrial cell death is the basis of the chemosensitizing effect of Ind combined with CDDP against HeLa cancer cells. ROS act as upstream signaling molecules to initiate apoptosis via p53/p21 axis. Ind can be a phytochemical of interest in combo-therapy.
机译:将植物化学物质与化疗结合起来是一种治疗癌症的新出现策略,以克服药物毒性和耐受天然化合物的抗性。我们评估了籼迷(IND)的效果,从(L. Mill)果实中获得的颜料,与顺铂(CDDP)联合对宫颈癌细胞(HELA)。通过台盼蓝测定测量的细胞活力;通过荧光显微镜的细胞形态;通过流式细胞术,细胞凋亡,细胞周期,线粒体膜电位(MMP)和细胞氧化还原平衡;通过蛋白质印迹表达相关蛋白的表达水平。细胞活力测定和Chou-talalay曲线表明CDDP和IND的组合具有协同细胞毒性作用。结合治疗对磷脂酰丝氨酸外化具有显着影响(<0.05),细胞形态学变化,细胞周期骤停,下降与个体治疗组相比,MMP,ROS生产和GSH衰减。 BAX,细胞色素C,P53和P21被过度表达,而BCL-2下调。用N-乙酰基-1-半胱氨酸预处理废除了观察到的协同作用。我们还通过营养相关浓度呈现CDDP抗癌活性的增强。氧化应激依赖性线粒体细胞死亡是IND与CDDP对HELA癌细胞的化学溶解作用的基础。 ROS充当上游信号分子,通过P53 / P21轴启动细胞凋亡。 IND可以是在组合治疗中兴趣的植物化学。

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