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首页> 外文期刊>Bioorganic and medicinal chemistry >Novel limonene phosphonate and farnesyl diphosphate analogues: design, synthesis, and evaluation as potential protein-farnesyl transferase inhibitors.
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Novel limonene phosphonate and farnesyl diphosphate analogues: design, synthesis, and evaluation as potential protein-farnesyl transferase inhibitors.

机译:新型柠檬烯膦酸酯和法呢基二磷酸类似物:设计,合成和评估为潜在的蛋白质-法呢基转移酶抑制剂。

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摘要

Limonene and its metabolite perillyl alcohol are naturally-occurring isoprenoids that block the growth of cancer cells both in vitro and in vivo. This cytostatic effect appears to be due, at least in part, to the fact that these compounds are weak yet selective and non-toxic inhibitors of protein prenylation. Protein-farnesyl transferase (FTase), the enzyme responsible for protein farnesylation, has become a key target for the rational design of cancer chemotherapeutic agents. Therefore, several alpha-hydroxyphosphonate derivatives of limonene were designed and synthesized as potentially more potent FTase inhibitors. A noteworthy feature of the synthesis was the use of trimethylsilyl triflate as a mild, neutral deprotection method for the preparation of sensitive phosphonates from the corresponding tert-butyl phosphonate esters. Evaluation of these compounds demonstrates that they are exceptionally poor FTase inhibitors in vitro (IC50 > or = 3 mM) and they have no effect on protein farnesylation in cells. In contrast, farnesyl phosphonyl(methyl)phosphinate, a diphosphate-modified derivative of the natural substrate farnesyl diphosphate, is a very potent FTase inhibitor in vitro (Ki=23 nM).
机译:柠檬烯及其代谢产物紫苏醇是天然存在的类异戊二烯,可在体外和体内阻滞癌细胞的生长。这种细胞抑制作用似乎至少部分是由于以下事实:这些化合物是弱的,选择性的且无毒的蛋白质异戊二烯化抑制剂。蛋白质法呢基转移酶(FTase)是负责蛋白质法呢基化的酶,已成为合理设计癌症化疗药物的关键目标。因此,设计并合成了柠檬烯的几种α-羟基膦酸酯衍生物,作为可能更有效的FTase抑制剂。合成的一个值得注意的特征是使用三氟甲磺酸三甲基甲硅烷基酯作为温和的中性脱保护方法,用于从相应的叔丁基膦酸酯制备敏感的膦酸酯。对这些化合物的评估表明,它们在体外是异常差的FTase抑制剂(IC50>或= 3 mM),并且对细胞中的蛋白质法呢基化没有影响。相反,法呢基膦酰基(甲基)次膦酸酯是天然底物法呢基二磷酸的二磷酸酯改性的衍生物,在体外是非常有效的FTase抑制剂(Ki = 23 nM)。

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