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Myricetin Abrogates Cisplatin-Induced Oxidative Stress Inflammatory Response and Goblet Cell Disintegration in Colon of Wistar Rats

机译:杨梅素消除Wistar大鼠结肠中顺铂诱导的氧化应激炎症反应和杯状细胞分解。

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摘要

Cisplatin [cis-diamminedichloroplatinum II] is an extensively prescribed drug in cancer chemotherapy; it is also useful for the treatment of diverse types of malignancies. Conversely, cisplatin is associated with a range of side effects such as nephrotoxicity, hepatotoxicity, gastrointestinal toxicity, and so on. Myricetin (3,5,7-trihydroxy-2-(3,4,5-trihydroxyphenyl)-4chromenone) is a very common natural flavonoid found in fruits, tea, and plants. It has been found to have high-value pharmacological properties and strong health benefits. To examine the role of myricetin in colon toxicity induced by cisplatin, we conducted a concurrent prophylactic study in experimental animals that were treated orally with myricetin for 14 days at two doses—25 and 50 mg/kg of body weight. On the 14th day, a single intraperitoneal injection of cisplatin (7.5 mg/kg body weight) was administered in all groups except control. The effects of myricetin in cisplatin-induced toxicity in the colon were assessed in terms of antioxidant status, phase-II detoxification enzymes, the level of inflammatory markers, and goblet cell disintegration. Myricetin was found to restore the level of all the antioxidant enzymes analyzed in the study. In addition, the compound ameliorated cisplatin-induced lipid peroxidation, increase in xanthine oxidase activity, and phase-II detoxifying enzyme activity. Myricetin also attenuated deteriorative effects induced by cisplatin by regulating the level of molecular markers of inflammation (NF-κB, Nrf-2, IL-6, and TNF-α), restoring Nrf-2 levels, and controlling goblet cell disintegration. The current study reinforces the conclusion that myricetin exerts protection in colon toxicity via up-regulation of inflammatory markers, improving anti-oxidant status, and protecting tissue damage.
机译:顺铂[cis-diamminedichloroplatinum II]是癌症化疗中广泛使用的药物;它也可用于治疗多种类型的恶性肿瘤。相反,顺铂与一系列副作用相关,例如肾毒性,肝毒性,胃肠道毒性等。杨梅素(3,5,7-三羟基-2-(3,4,5-三羟基苯基)-4chromenone)是一种非常常见的天然黄酮类化合物,存在于水果,茶和植物中。已经发现它具有高价值的药理特性和强大的健康益处。为了检查杨梅素在顺铂诱导的结肠毒性中的作用,我们在以25和50 mg / kg体重的两种剂量口服杨梅素治疗14天的实验动物中进行了一项并行的预防性研究。在第14天,除对照组外,所有组均腹膜内注射顺铂(7.5mg / kg体重)。根据抗氧化剂状态,II期解毒酶,炎性标志物的水平和杯状细胞的分解,评估了杨梅素在顺铂诱导的结肠毒性中的作用。发现杨梅素可以恢复研究中分析的所有抗氧化酶的水平。此外,该化合物改善了顺铂诱导的脂质过氧化作用,提高了黄嘌呤氧化酶活性和II期解毒酶活性。杨梅素还通过调节炎症分子标志物的水平(NF-κB,Nrf-2,IL-6和TNF-α),恢复Nrf-2的水平并控制杯状细胞的分解,来减轻顺铂引起的恶化作用。当前的研究进一步证实了杨梅素通过上调炎症标志物,改善抗氧化剂状态和保护组织损伤而在结肠毒性中起到保护作用的结论。

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