首页> 美国卫生研究院文献>Molecules >Anticancer Activities of the Quinone-Methide Triterpenes Maytenin and 22-β-hydroxymaytenin Obtained from Cultivated Maytenus ilicifolia Roots Associated with Down-Regulation of miRNA-27a and miR-20a/miR-17-5p
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Anticancer Activities of the Quinone-Methide Triterpenes Maytenin and 22-β-hydroxymaytenin Obtained from Cultivated Maytenus ilicifolia Roots Associated with Down-Regulation of miRNA-27a and miR-20a/miR-17-5p

机译:从miRNA-27a和miR-20a / miR-17-5p的下调获得的栽培的Maytenus ilicifolia根获得的甲基间苯二酚三萜烯Maytenin和22-β-羟基maytenin的抗癌活性。

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摘要

Natural triterpenes exhibit a wide range of biological activities. Since this group of secondary metabolites is structurally diverse, effects may vary due to distinct biochemical interactions within biological systems. In this work, we investigated the anticancer-related activities of the quinone-methide triterpene maytenin and its derivative compound 22-β-hydroxymaytenin, obtained from roots cultivated in vitro. Their antiproliferative and pro-apoptotic activities were evaluated in monolayer and three-dimensional cultures of immortalized cell lines. Additionally, we investigated the toxicity of maytenin in SCID mice harboring tumors derived from a squamous cell carcinoma cell line. Both isolated molecules presented pronounced pro-apoptotic activities in four cell lines derived from head and neck squamous cell carcinomas, including a metastasis-derived cell line. The molecules also induced reactive oxygen species (ROS) and down-regulated microRNA-27a and microRNA-20a/miR-17-5p, corroborating with the literature data for triterpenoids. Intraperitoneal administration of maytenin to tumor-bearing mice did not lead to pronounced histopathological changes in kidney tissue, suggesting low nephrotoxicity. The wide-ranging activity of maytenin and 22-β-hydroxymaytenin in head and neck cancer cells indicates that these molecules should be further explored in plant biochemistry and biotechnology for therapeutic applications.
机译:天然三萜烯具有广泛的生物活性。由于这组次生代谢物在结构上是多种多样的,因此效果可能会由于生物系统内不同的生化相互作用而有所不同。在这项工作中,我们研究了从体外培养的根获得的醌-甲基三萜烯美登汀及其衍生物化合物22-β-羟基美登汀的抗癌相关活性。在永生化细胞系的单层和三维培养中评估了它们的抗增殖和促凋亡活性。此外,我们调查了美登素对SCID小鼠的毒性,该小鼠具有来自鳞状细胞癌细胞系的肿瘤。两种分离的分子在源自头颈部鳞状细胞癌的四个细胞系中均表现出明显的促凋亡活性,包括转移衍生的细胞系。这些分子还诱导了活性氧(ROS)并下调了microRNA-27a和microRNA-20a / miR-17-5p,与三萜类化合物的文献数据相符。向荷瘤小鼠腹膜内给予美登汀并没有导致肾脏组织的明显组织病理学改变,提示其肾毒性较低。美登汀和22-β-羟基美登素在头颈癌细胞中的广泛活性表明,这些分子应在植物生物化学和生物技术中进行进一步研究以用于治疗应用。

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