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肝脏加工决定了α-生育酚琥珀酸酯的双重活性:一种因维生素原向维生素转化而导致生物活性转变的新范例。

Hepatic processing determines dual activity of alpha-tocopheryl succinate: a novel paradigm for a shift in biological activity due to pro-vitamin-to-vitamin conversion.

作者信息

Neuzil Jiri, Massa Helen

机构信息

Apoptosis Research Group, School of Medical Sciences, Griffith University, Southport, Qld., Australia.

出版信息

Biochem Biophys Res Commun. 2005 Feb 25;327(4):1024-7. doi: 10.1016/j.bbrc.2004.12.115.

Abstract

Redox-silent vitamin E analogues, represented by alpha-tocopheryl succinate, are potent anti-cancer drugs with potential secondary bioactivity due to their processing in vivo. Here we verified the hypothesis that hepatic processing of these agents determines the secondary effect. Mice were repeatedly injected with alpha-tocopheryl succinate, and their systemic and hepatic vein blood was assessed for alpha-tocopheryl succinate and its hydrolysis product, vitamin E (alpha-tocopherol). While levels of alpha-tocopherol doubled compared to control mice and alpha-tocopheryl succinate accumulated in the systemic blood, no alpha-tocopheryl succinate was detected in blood draining the liver. We conclude that hepatic processing endows compounds like alpha-tocopheryl succinate with a secondary, anti-oxidant/anti-inflammatory activity due to converting it to the redox-active alpha-tocopherol. Our finding epitomises a novel, general paradigm, according to which a drug can be converted in the liver into a product that has a different beneficial bioactivity.

摘要

以α-生育酚琥珀酸酯为代表的氧化还原沉默型维生素E类似物是具有潜在二次生物活性的强效抗癌药物,这是由于它们在体内的代谢过程。在此,我们验证了这样一个假设,即这些药物在肝脏中的代谢决定了其二次效应。给小鼠反复注射α-生育酚琥珀酸酯,并对其体循环血液和肝静脉血液进行评估,检测其中α-生育酚琥珀酸酯及其水解产物维生素E(α-生育酚)的含量。与对照小鼠相比,α-生育酚的水平增加了一倍,且α-生育酚琥珀酸酯在体循环血液中积累,但在从肝脏流出的血液中未检测到α-生育酚琥珀酸酯。我们得出结论,肝脏代谢赋予了α-生育酚琥珀酸酯这类化合物一种二次抗氧化/抗炎活性,因为它将其转化为了具有氧化还原活性的α-生育酚。我们的发现体现了一种新的通用模式,即一种药物可以在肝脏中转化为具有不同有益生物活性的产物。

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