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首页> 外文期刊>Journal of Applied Biomedicine >Molecular mechanisms responsible for programmed cell death-inducing attributes of terpenes from Mesua ferrea stem bark towards human colorectal carcinoma HCT 116 cells
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Molecular mechanisms responsible for programmed cell death-inducing attributes of terpenes from Mesua ferrea stem bark towards human colorectal carcinoma HCT 116 cells

机译:致使Mesua ferrea茎皮中萜烯对人结直肠癌HCT 116细胞的程序性细胞死亡诱导特性的分子机制

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The current study explored the in vitro anticancer properties of Mesua ferrea stem bark (SB) extract towards human colon carcinoma HCT116 cells. SB was successively extracted with different solvents using soxhlet apparatus. MTT assay was employed to test toxicity against different cancer and normal cell lines. Active extract (n-Hexane) was fractionated by column chromatography (CC) to get the most active fraction (F-3). Series of in vitro assays were employed to characterize cytotoxic nature of F-3. Antioxidant properties of F-3 were assessed using DPPH, ABTS and FRAP assays followed by GCa??MS analysis. Intracellular ROS levels were measured by DCFH-DA fluorescent assay. Finally, cell signalling pathways and their downstream proteins targeted by F-3 were studied using 10-cancer pathway and human apoptosis protein profilers and in silico docking studies. n-Hexane extract and its fraction (F-3) showed potent anti-proliferative effect against HCT 116. Programmed cell death (PCD) studies showed that F-3 modulated the expression of multiple proteins in HCT 116. F-3 showed weak antioxidant activity in all the models, while significant increase in ROS was observed in HCT 116. GCa??MS analysis revealed that F-3 was majorly comprised of terpenes. Data of pathway profiler and in silico studies revealed that F-3 down-regulated the expression of NF-?oB and HIF-1?± pathways. Overall these results demonstrate that anticancer effects of M. ferrea stem bark towards human colon carcinoma are mainly due to its terpenes contents.
机译:当前的研究探索了Mesua ferrea茎皮(SB)提取物对人结肠癌HCT116细胞的体外抗癌特性。使用索氏萃取仪依次用不同溶剂萃取SB。使用MTT测定法测试针对不同癌症和正常细胞系的毒性。通过柱色谱法(CC)对活性提取物(正己烷)进行分馏,以获得活性最高的馏分(F-3)。使用一系列体外测定来表征F-3的细胞毒性性质。使用DPPH,ABTS和FRAP分析,然后进行GCaβMS分析,评估F-3的抗氧化性能。通过DCFH-DA荧光测定法测量细胞内ROS水平。最后,使用10癌途径和人类凋亡蛋白分析仪以及计算机对接研究,研究了F-3靶向的细胞信号通路及其下游蛋白。正己烷提取物及其馏分(F-3)对HCT 116表现出有效的抗增殖作用。程序性细胞死亡(PCD)研究表明F-3调节HCT 116中多种蛋白质的表达。F-3显示弱的抗氧化剂HCT 116中观察到ROS显着增加。GCaMS分析表明F-3主要由萜烯组成。通路分析仪和计算机研究的数据表明,F-3下调了NF-κB和HIF-1α±通路的表达。总的来说,这些结果表明,M.ferrea茎皮对人结肠癌的抗癌作用主要是由于其萜烯含量。

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