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首页> 外文期刊>Journal of experimental & clinical cancer research : >Potent cytotoxic effects of Calomeria amaranthoides on ovarian cancers
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Potent cytotoxic effects of Calomeria amaranthoides on ovarian cancers

机译:Cal菜花草对卵巢癌的潜在细胞毒性作用

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Background Ovarian cancer remains the leading cause of death from gynaecological malignancy. More than 60% of the patients are presenting the disease in stage III or IV. In spite of combination of chemotherapy and surgery the prognosis stays poor for therapy regimen. Methods The leaves of a plant endemic to Australia, Calomeria amaranthoides, were extracted and then fractionated by column chromatography. In vitro cytotoxicity tests were performed with fractions of the plant extract and later with an isolated compound on ovarian cancer cell lines, as well as normal fibroblasts at concentrations of 1-100 μg/mL (crude extract) and 1-10 μg/mL (compound). Cytotoxicity was measured after 24, 48 and 72 hours by using a non-fluorescent substrate, Alamar blue. In vivo cytotoxicity was tested on ascites, developed in the abdomen of nude mice after inoculation with human OVCAR3 cells intraperitoneally. The rate of change in abdomen size for the mice was determined by linear regression and statistically evaluated for significance by the unpaired t test. Results Two compounds were isolated by chromatographic fractionation and identified by 1H-NMR, 13C-NMR and mass spectrometry analyses, EPD, an α-methylene sesquiterpene lactone of the eremophilanolide subtype, and EPA, an α-methylene carboxylic acid. Cytotoxicity of EPD for normal fibroblasts at all time points IC50 was greater than 10 μg/mL, whereas, for OVCAR3 cells at 48 hours IC50 was 5.3 μg/mL (95% confidence interval 4.3 to 6.5 μg/mL). Both, the crude plant extract as well as EPD killed the cancer cells at a final concentration of 10 μg/mL and 5 μg/mL respectively, while in normal cells only 20% cell killing effect was observed. EPA had no cytotoxic effects. Changes in abdomen size for control versus Cisplatin treated mice were significantly different, P = 0.023, as were control versus EPD treated mice, P = 0.025, whereas, EPD versus Cisplatin treated mice were not significantly different, P = 0.13. Conclusions For the first time both crude plant extract from Calomeria amaranthoides and EPD have been shown to have potent anti-cancer effects against ovarian cancer.
机译:背景卵巢癌仍然是妇科恶性肿瘤死亡的主要原因。超过60%的患者在III或IV期出现疾病。尽管化学疗法和手术相结合,但是治疗方案的预后仍然很差。方法提取澳大利亚特有种mar菜(Calomeria amaranthoides)的叶子,然后通过柱色谱法分级分离。用部分植物提取物进行体外细胞毒性测试,然后使用分离的化合物对卵巢癌细胞系以及浓度为1-100μg/ mL(粗提取物)和1-10μg/ mL的正常成纤维细胞进行分离(复合)。通过使用非荧光底物Alamar蓝在24、48和72小时后测量细胞毒性。腹膜内接种人OVCAR 3 细胞后,对裸鼠腹部产生的腹水进行体内细胞毒性测试。通过线性回归确定小鼠腹部大小的变化率,并通过未配对的t检验对统计学意义的显着性进行评估。结果通过色谱分离分离出两种化合物,分别通过 1 H-NMR, 13 C-NMR和质谱分析法鉴定了EPD,艾美特罗内酯的α-亚甲基倍半萜烯内酯。亚型和EPA,一种α-亚甲基羧酸。在所有时间点IC 50 对正常成纤维细胞的EPD的细胞毒性均大于10μg/ mL,而在48小时IC 50 下对OVCAR 3 细胞的细胞毒性。 sub>为5.3μg/ mL(95%置信区间为4.3至6.5μg/ mL)。粗植物提取物和EPD分别以10μg/ mL和5μg/ mL的终浓度杀死癌细胞,而在正常细胞中仅观察到20%的细胞杀伤作用。 EPA没有细胞毒性作用。对照与顺铂处理的小鼠的腹部大小变化显着不同,P = 0.023,对照与EPD处理的小鼠的腹部大小变化,P = 0.025,而EPD与顺铂处理的小鼠,腹部大小变化无显着差异,P = 0.13。结论首次从a菜中提取的粗植物提取物和EPD均显示出对卵巢癌有效的抗癌作用。

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