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Tea phenols in bulk and nanoparticle form modify DNA damage in human lymphocytes from colon cancer patients and healthy individuals treated in vitro with platinum-based chemotherapeutic drugs

机译:散装和纳米颗粒形式的茶酚可改善结肠癌患者和健康个体体外用铂类化疗药物治疗后人淋巴细胞的DNA损伤

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Background: Tea catechin epigallocatechin-3-gallate (EGCG) and other polyphenols, such as theaflavins (TFs), are increasingly proving useful as chemopreventives in a number of human cancers. They can also affect normal cells. The polyphenols in tea are known to have antioxidant properties that can quench free radical species, and pro-oxidant activities that appear to be responsible for the induction of apoptosis in tumor cells. The bioavailability of these natural compounds is an important factor that determines their efficacy. Nanoparticle (NP)-mediated delivery techniques of EGCG and TFs have been found to improve their bioavailability to a level that could benefit their effectiveness as chemopreventives. Aim: The present study was conducted to compare the effects of TFs and EGCG, when used in the bulk form and in the polymer (poly[lactic-co-glycolic acid])-based NP form, in oxaliplatin- and satraplatin-treated lymphocytes as surrogate cells from colorectal cancer patients and healthy volunteers. Materials & methods: NPs were examined for their size distribution, surface morphology, entrapment efficiency and release profile. Lymphocytes were treated in the Comet assay with oxaliplatin and satraplatin, washed and treated with bulk or NP forms of tea phenols, washed and then treated with hydrogen peroxide to determine single-strand breaks after crosslinking. Results: The results of DNA damage measurements by the Comet assay revealed opposite trends in bulk and NP forms of TFs, as well as EGCG. Both the compounds in the bulk form produced statistically significant concentration-dependent reductions in DNA damage in oxaliplatin- or satraplatin-treated lymphocytes. In contrast, when used in the NP form both TFs and EGCG, although initially causing a reduction, produced a concentration-dependent statistically significant increase in DNA damage in the lymphocytes. Discussion: These observations support the notion that TFs and EGCG act as both antioxidants and pro-oxidants, depending on the form in which they are administered under the conditions of investigation.
机译:背景:儿茶素表没食子儿茶素-3-没食子酸酯(EGCG)和其他茶多酚(茶黄素)(TFs)已被证明在许多人类癌症中作为化学预防剂有用。它们也会影响正常细胞。众所周知,茶中的多酚具有抗氧化剂特性,可以淬灭自由基,并具有促氧化活性,这似乎是导致肿瘤细胞凋亡的原因。这些天然化合物的生物利用度是决定其功效的重要因素。已经发现,纳米颗粒(NP)介导的EGCG和TF的递送技术可将其生物利用度提高到有益于其作为化学预防剂的功效的水平。目的:进行本研究以比较以草酸铂和沙铂处理的淋巴细胞以大容量形式和基于聚合物(聚乳酸-乙醇酸)的NP形式使用时,TFs和EGCG的作用作为大肠癌患者和健康志愿者的替代细胞。材料和方法:检查NP的大小分布,表面形态,截留效率和释放曲线。在彗星试验中,用奥沙利铂和沙铂处理淋巴细胞,洗涤并用散装或NP形式的茶酚处理,洗涤,然后用过氧化氢处理,以确定交联后的单链断裂。结果:通过彗星分析的DNA损伤测量结果显示,TF和EGCG的体积和NP形式呈现相反的趋势。在奥沙利铂或沙铂处理的淋巴细胞中,两种散装形式的化合物均产生统计学上显着的浓度依赖性的DNA损伤减少。相反,当以NP形式使用TFs和EGCG时,尽管最初会引起减少,但淋巴细胞中DNA损伤的浓度依赖性的统计学显着增加。讨论:这些观察结果支持以下观点:TFs和EGCG既可以作为抗氧化剂,也可以作为促氧化剂,这取决于在研究条件下施用它们的形式。

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