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首页> 外文期刊>Pharmacology: International Journal of Experimental and Clinical Pharmacology >SRS06, a New Semisynthetic Andrographolide Derivative with Improved Anticancer Potency and Selectivity, Inhibits Nuclear Factor-kappa B Nuclear Binding in the A549 Non-Small Cell Lung Cancer Cell Line
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SRS06, a New Semisynthetic Andrographolide Derivative with Improved Anticancer Potency and Selectivity, Inhibits Nuclear Factor-kappa B Nuclear Binding in the A549 Non-Small Cell Lung Cancer Cell Line

机译:SRS06,具有改进的抗癌潜能和选择性的新型半合成穿心莲内酯衍生物,可抑制A549非小细胞肺癌细胞系中的核因子-κB核结合。

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Background: Andrographolide has been reported with anticancer and anti-inflammatory properties through the inhibition of the activity of signaling molecules such as v-Src, nuclear factor-kappa B (NF-kappa B), STAT3, and PI3K. NF-kappa B has been proven to promote cancer cell survival, and targeting this pathway will halt the growth of cancer cells. Efforts have been made to produce semisynthetic derivatives of andrographolide with improved anticancer potency and selectivity. Subsequently, the effect of a selected derivative, 3,14,19-tripropionylandrographolide (SRS06), was tested for its action against NF-kappa B. Methods: Screening against 60 US National Cancer Institute (NCI) human cancer cell lines representing leukemia and non-small cell lung (NSCL), colon, CNS, melanoma, ovarian, renal, prostate, and breast cancers was performed to determine the tumor type selectivity and potency of SRS06. Microculture tetrazolium, 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyl tetrazolium bromide and sulforhodamine B assays were used to determine the in vitro anticancer activity, while Western blot studies were performed to ascertain the inhibitory effect of SRS06 on the NF-kappa B signaling cascade. The TransAM (TM) p65 assay kit was used to determine NF-kappa B p65 DNA binding activity in the NSCL cancer cell line A549. Results: From the NCI screening, SRS06 was found to exhibit potent growth-inhibitory effects on multiple cancer cell lines with 10-fold lower 50% growth inhibition (GI 50) compared with andrographolide. It was also discerned that the compound preferentially targeted melanoma, CNS, renal, colon, ovarian, prostate, and NSCL cancer cell lines. The DNA fragmentation assay indicated that the main mode of cell death of SRS06-treated A549 cells was via apoptosis. At 5 mu mol/l the compound decreased NF-kappa B protein expression and caused a significant reduction in the nuclear p65 DNA binding activity. Conclusion: SRS06 displayed improved anticancer selectivity and potency when compared with andrographolide. We alluded its anticancer activity to its effect of inhibiting NF-kappa B nuclear binding. (C) 2015 S. Karger AG, Basel
机译:背景:穿心莲内酯据报道具有通过抑制信号分子(例如v-Src,核因子-κB(NF-κB),STAT3和PI3K)的活性而具有的抗癌和抗炎特性。 NF-κB已被证明可以促进癌细胞的存活,靶向该途径将阻止癌细胞的生长。已经努力生产具有改进的抗癌效力和选择性的穿心莲内酯的半合成衍生物。随后,测试了一种选定的衍生物3,14,19-三丙炔酸内酯(SRS06)对NF-κB的作用。方法:针对60种代表白血病和白血病的美国国家癌症研究所(NCI)人癌细胞株进行筛选进行非小细胞肺癌(NSCL),结肠癌,中枢神经系统,黑色素瘤,卵巢癌,肾癌,前列腺癌和乳腺癌的研究,以确定SRS06的肿瘤类型选择性和效力。微培养四唑,3-(4,5-二甲基噻唑-2-基)-2,5-二苯基溴化四唑和磺基罗丹明B测定法测定体外抗癌活性,同时进行Western印迹研究以确定NF-κB信号级联上的SRS06。 TransAM TM p65分析试剂盒用于确定NSCL癌细胞系A549中的NF-κB p65 DNA结合活性。结果:从NCI筛选中,发现SRS06对多种癌细胞具有有效的生长抑制作用,与​​穿心莲内酯相比,其50%的生长抑制(GI 50)低10倍。还发现该化合物优先靶向黑色素瘤,CNS,肾,结肠,卵巢,前列腺和NSCL癌细胞系。 DNA片段化分析表明,经SRS06处理的A549细胞的主要细胞死亡方式是通过凋亡。在5μmol / l的浓度下,该化合物降低了NF-κB蛋白的表达,并导致核p65 DNA结合活性显着降低。结论:与穿心莲内酯相比,SRS06具有更高的抗癌选择性和效力。我们将其抗癌活性提到抑制NF-κB核结合的作用。 (C)2015 S.Karger AG,巴塞尔

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