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Vesicular flavonoid in combating diethylnitrosamine induced hepatocarcinoma in rat model.

机译:在大鼠模型中,水泡类黄酮对抗二乙基亚硝胺诱导的肝癌。

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Reactive oxygen species (O2(*-), OH(-), H2O2) are known to play an important role in tumor initiation in hepatocarcinoma. Hepatocarcinoma was developed in the Swiss Albino rats by administration three doses of diethylnitrosamine (DEN) (200 mg/kg b. wt.) (i.p.) at 15 days interval. Quercetin (QC), herbal polyphenolic compound, is a potent anticancer drug. Clinical trials are difficult for its hydrophobic nature. To overcome this problem, our study was aimed to formulate soluble liver specific, galactosylated liposomal QC and to investigate its efficacy against hepatocarcinoma in rat model. Galactosylated liposomal QC was formulated and the suspension was introduced intravenously to rats (8.98 microM/kg) once in a week for 16 weeks. Hepatocarcinoma in rat model and its pathological improvement were evaluated histopathologically, histochemically and electron microscopically. Severe oxidative damage was noticed in the whole liver and its microsomal fraction of DEN treated rats. Huge numbers of hyperplasticnodules (HNs) with pre-neoplastic lesions appeared in rat liver by DEN administration. Galactosylated liposomal QC injections prevented DEN mediated development of hepatocarcinoma and oxidative damage in rat liver. Quercetin in liver specific galactosylated liposomal drug delivery system may be recommended as a potent therapeutic formulation against DEN-induced hepatocarcinoma.
机译:已知活性氧(O2(*-),OH(-),H2O2)在肝癌的肿瘤发生中起重要作用。在瑞士白化病大鼠中,每隔15天服用三剂二乙基亚硝胺(DEN)(200 mg / kg b。wt。)(i.p.),即可发展为肝癌。槲皮素(QC)是一种草药多酚化合物,是一种有效的抗癌药物。由于疏水性,临床试验很困难。为了克服这个问题,我们的研究旨在制定可溶性肝特异性半乳糖基化脂质体QC,并研究其在大鼠模型中抗肝癌的功效。配制半乳糖基化脂质体QC,并将悬浮液每周一次静脉内引入大鼠(8.98 microM / kg),持续16周。通过组织病理学,组织化学和电子显微镜对大鼠肝癌模型及其病理改善情况进行评估。在DEN治疗的大鼠的整个肝脏及其微粒体部分中发现了严重的氧化损伤。通过DEN给药在大鼠肝脏中出现了大量具有肿瘤前病变的增生性结节(HNs)。半乳糖基脂质体QC注射可预防DEN介导的肝癌的发展和大鼠肝脏的氧化损伤。肝脏特异性半乳糖基化脂质体药物递送系统中的槲皮素可能被推荐作为针对DEN诱导的肝癌的有效治疗剂。

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