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首页> 外文期刊>The Journal of Nutritional Biochemistry >The role of epoxidation and electrophile-responsive element-regulated gene transcription in the potentially beneficial and harmful effects of the coffee components cafestol and kahweol
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The role of epoxidation and electrophile-responsive element-regulated gene transcription in the potentially beneficial and harmful effects of the coffee components cafestol and kahweol

机译:环氧化和亲电子反应元件调节的基因转录在咖啡成分cafestol和kahweol的潜在有益和有害作用中的作用

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Cafestol and kahweol are diterpene compounds present in unfiltered coffees. Cafestol is known as the most potent cholesterol-raising agent that may be present in the human diet. Remarkably, the mechanisms behind this effect have only been partly resolved so far. Even less is known about the metabolic fate of cafestol and kahweol. From the structure of cafestol, carrying a furan moiety, we hypothesized that epoxidation may not only be an important biotransformation route but that this also plays a role in its effects found. In bile duct-cannulated mice, dosed with cafestol, we were able to demonstrate the presence of epoxy-glutathione (GSH) conjugates, GSH conjugates and glucuronide conjugates. In addition, it was shown that cafestol was able to induce an electrophile-responsive element (EpRE). Using a murine hepatoma cell line with a luciferase reporter gene under control of an EpRE from the human NQO1 regulatory region, we also found that metabolic activation by CYP450 enzymes is needed for EpRE induction. Furthermore, raising intracellular GSH resulted in a decrease in EpRE-mediated gene induction, whereas lowering intracellular GSH levels increased EpRE-mediated gene induction. In conclusion, evidence suggests that cafestol induces EpRE, apparently via a bioactivation process that possibly involves epoxidation of the furan ring. The epoxides themselves appear subject to conjugation with GSH. The effects on EpRE can also explain the induction of GSH which seems to be involved in the reported beneficial effects of cafestol, for example, when administered with aflatoxin B1 or other toxic or carcinogenic compounds
机译:Cafestol和kahweol是未过滤咖啡中存在的二萜化合物。 Cafestol被认为是人类饮食中可能存在的最有效的胆固醇升高剂。引人注目的是,到目前为止,这种作用背后的机制尚未得到部分解决。关于cafestol和kahweol的代谢命运知之甚少。从带有呋喃部分的cafestol的结构中,我们假设环氧化不仅可能是重要的生物转化途径,而且在发现其效果中也起作用。在给予cafestol的胆管插管小鼠中,我们能够证明环氧-谷胱甘肽(GSH)缀合物,GSH缀合物和葡糖醛酸苷缀合物的存在。另外,显示了咖啡甾醇能够诱导亲电响应元件(EpRE)。在人NQO1调节区的EpRE的控制下,使用具有荧光素酶报道基因的鼠肝癌细胞系,我们还发现CYP450酶的代谢激活对于EpRE的诱导是必需的。此外,提高细胞内GSH会导致EpRE介导的基因诱导减少,而降低细胞内GSH会增加EpRE介导的基因诱导。总之,有证据表明,咖啡甾醇显然是通过生物激活过程(可能涉及呋喃环的环氧化)诱导了EpRE。环氧化物本身似乎与GSH结合。对EpRE的影响也可以解释GSH的诱导,这似乎与咖啡酚的报道有益作用有关,例如,与黄曲霉毒素B1或其他有毒或致癌化合物一起使用时

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