富勒烯C60与抗氧剂的作用

V. V. Marysheva, P. Shabanov
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引用次数: 0

摘要

背景:药物改良通常是在化学修饰的帮助下进行的,这些修饰可以改善受体的作用或药物向靶组织的运输。目的:本研究旨在探讨C60富勒烯与氨替唑、2-氨基-4-乙酰噻唑[5,4-b]吲哚、metaprot、metaprot碱和芦丁联合使用对急性缺氧伴高碳酸血症模型抗缺氧活性的影响。材料和方法:对几种单环、双环和三环结构的化合物分别或与C60富勒烯结合进行了研究。除芦丁外,所有化合物都是在基洛夫军事医学院药理学部合成的,并且在循环中含有活性氨基、氮和硫原子:amtizol(3,5-二氨基-1,2,4-噻二唑)、VM-606(2-氨基-4-乙酰噻唑[5,4-b]吲哚)、Metaprot(2-乙基噻吩咪唑氢溴化物)和Metaprot碱。所有化合物均表现出抗缺氧活性。在流压室中模拟低压缺氧,以50 m/s的速度将动物提升到10,000 m的高度,暴露60 min。实验前60 min给药。用海拔平均预期寿命来评价这种保护作用。研究人员对体重为2022 g的雄性白鼠进行了低氧高碳酸血症评估,将小鼠置于200毫升的密封玻璃瓶中,并将玻璃瓶放入水中以防止漏气。所研究的制剂及其与富勒烯的配合物以Tween-80的薄悬浮液的形式在缺氧前进行腹腔注射。这些动物的寿命被记录下来。结果:配合物的形成及其性质取决于药物与富勒烯之间的供受体键的发展。与C60富勒烯络合物形式的氨替唑的生物利用度增加,使混合物的抗缺氧活性增加了40%。在高碳酸缺氧模型中,首次获得了氨替唑和2-氨基-4-乙酰噻唑[5,4-b]吲哚活性随时间的动态曲线。结论:富勒烯C60增强了所研究化合物的抗缺氧活性,这是由于富勒烯C60的作用使组织膜微穿孔引起抗氧剂的生物利用度增加。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Effects of fullerene C60 with antihypoxants
BACKGROUND: Drug improvement is often carried out with the help of chemical modifications that improve the receptor action or transport of drugs to their target tissues. AIM: The aim of this study was to investigate the effect of combinations of C60 fullerene with amtizol, 2-amino-4-acetylthiazolo[5,4-b]indole, metaprot, metaprot base, and rutin on antihypoxic activities in a model of acute hypoxia with hypercapnia. MATERIALS AND METHODS: Several compounds with mono-, bi-, and tricyclic structures were examined separately or combined with C60 fullerene. All compounds, except for rutin, were synthesized at the Department of Pharmacology of the S.M. Kirov Military Medical Academy and contain active amino groups, nitrogen, and sulfur atoms in the cycles: amtizol (3,5-diamino-1,2,4-thiadiazole), VM-606 (2-amino-4-acetylthiazolo[5,4-b]indole), Metaprot (2-ethylthiobenzimidazole hydrobromide monohydrate), and Metaprot base. All compounds demonstrated antihypoxic activity. Hypobaric hypoxia was simulated in a flow pressure chamber by lifting animals to a height of 10,000 m at a speed of 50 m/s and exposure for 60 min. The preparations were administered intraperitoneally 60 min before the experiment. The protective effect was evaluated by the average life expectancy at altitude. Hypoxia with hypercapnia was assessed on male white mice weighing 2022 g, which were placed in 200 mL glass jars with hermetic lids, which were lowered under water to prevent air leakage. The studied preparations and their complexes with fullerene in the form of a thin suspension with Tween-80 were administered intraperitoneally min before hypoxia. The lifespan of the animals was recorded. RESULTS: The formation of the complex and its properties depend on the development of a donoracceptor bond between the drug and fullerene. An increase in the bioavailability of amtizol in the form of a complex with C60 fullerene increased the antihypoxic activity of the mixture by 40%. For the first time, dynamic curves of the activities of amtizol and 2-amino-4-acetylthiazolo[5,4-b]indole depending on time were obtained in a model of hypercapnic hypoxia. CONCLUSION: Fullerene C60 enhances the antihypoxic activity of the studied compounds due to an increase in the bioavailability of the antihypoxant caused by the microporation of tissue membranes due to the action of fullerene C60.
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