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Factors Influencing the Antifolate Activity of Synthetic Tea-Derived Catechins

机译:影响合成茶衍生儿茶素类抗叶酸活性的因素

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Novel tea catechin derivatives have been synthesized, and a structure-activity study, related to the capacity of these and other polyphenols to bind dihydrofolate reductase (DHFR), has been performed. The data showed an effective binding between all molecules and the free enzyme, and the dissociation constants of the synthetic compounds and of the natural analogues were on the same order. Polyphenols with a catechin configuration were better DHFR inhibitors than those with an epicatechin configuration. Antiproliferative activity was also studied in cultured tumour cells, and the data showed that the activity of the novel derivatives was higher in catechin isomers. Derivatives with a hydroxyl group para on the ester-bonded gallate moiety presented a high in vitro binding to DHFR, but exhibited transport problems in cell culture due to ionization at physiologic pHs. The impact of the binding of catechins to serum albumin on their biological activity was also evaluated. The information provided in this study could be important for the design of novel medicinal active compounds derived from tea catechins. The data suggest that changes in their structure to avoid serum albumin interactions and to facilitate plasmatic membrane transport are essential for the intracellular functions of catechins.
机译:已经合成了新型茶儿茶素衍生物,并且已经进行了与这些酚和其他多酚结合二氢叶酸还原酶(DHFR)的能力有关的结构活性研究。数据显示所有分子与游离酶之间有效结合,并且合成化合物和天然类似物的解离常数处于相同的数量级。具有儿茶素构型的多酚比具有表儿茶素构型的多酚更好。还研究了在培养的肿瘤细胞中的抗增殖活性,数据表明该新型衍生物的活性在儿茶素异构体中较高。在酯键合的没食子酸酯部分上具有羟基对位的衍生物在体外与DHFR具有很高的结合力,但由于在生理pH值下的电离,在细胞培养中显示出运输问题。还评估了儿茶素与血清白蛋白结合对其生物学活性的影响。这项研究中提供的信息对于设计衍生自茶儿茶素的新型药物活性化合物可能很重要。数据表明,改变其结构以避免血清白蛋白相互作用并促进质膜转运对儿茶素的细胞内功能至关重要。

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