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Pyranocoumarin tissue distribution and plasma metabolome and prostate transcriptome impacts of sub-chronic exposure to Korean Angelica supplement in mice

机译:亚慢性暴露于韩国当归补充品的小鼠吡喃香豆素组织分布以及血浆代谢组和前列腺转录组的影响

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摘要

Herbal products containing Korean Angelica gigas Nakai (AGN) root extract are marketed as dietary supplements for memory enhancement, pain killing, and female menopausal symptom relief. We have shown anti-cancer activity of AGN supplement in mouse models. To facilitate human anti-cancer translational research, we characterized the tissue distribution of AGN marker pyranocoumarin compounds decursin (D) and decursinol angelate (DA) (~50% in AGN) and their metabolite decursinol (DOH), assessed safety of sub-chronic AGN dietary exposure in mice, and explored the impacts on the plasma aqueous metabolites and prostate transcriptome. The data show that after a gavage dose, plasma contained readily detectable DOH, but little D and DA, mirroring patterns in the liver. Extra-hepatic tissues retained greater level of DA and D than liver. For sub-chronic exposures, male mice were provided ad libitum AIN93M-pellet diet with 0.5 and 1% AGN for 6 weeks. No adverse effect was observed on plasma biochemistry markers of liver and kidney integrity in spite of their enlargement. Histopathological examination of liver, kidney and other visceral organs did not reveal tissue abnormalities. Metabolomic assessment of plasma from the mice fed 1%-AGN diet suggested metabolic shifts of key amino acids especially methionine-cysteine cycle, purine cycle and glycolysis-citrate cycle. Prostate transcriptomic profiling identified gene signature changes of metabolisms of drugs, lipids and cellular energetics, neuro-muscular features, immunity and inflammation, and tumor suppressor/oncogene balance. The safety profile was corroborated with daily i.p. injection of AGN extract (200 mg/kg) for 4 weeks, which resulted in much greater systemic pyranocoumarin exposure than dietary route.
机译:含有韩国当归中根(AGN)根提取物的草药产品可作为膳食补充剂销售,以增强记忆力,止痛和缓解女性更年期症状。我们已经在小鼠模型中显示了AGN补充剂的抗癌活​​性。为促进人类抗癌转化研究,我们表征了AGN标记吡香香豆素化合物decursin(D)和decursinol angelate(DA)(在AGN中约为50%)及其代谢物decursinol(DOH)的组织分布,评估了亚慢性的安全性AGN在小鼠中的饮食暴露,并探讨了其对血浆含水代谢产物和前列腺转录组的影响。数据显示,在强饲后,血浆中的DOH易于检测,但D和DA很少,在肝脏中呈镜像状。肝外组织保留的DA和D水平高于肝脏。对于亚慢性暴露,为雄性小鼠提供0.5和1%AGN的随意AIN93M颗粒饲料6周。尽管肝脏和肾脏完整性有所增加,但对血浆生化指标没有发现不良影响。肝,肾和其他内脏器官的组织病理学检查未发现组织异常。饲喂1%-AGN饮食的小鼠血浆的代谢组学评估表明关键氨基酸的代谢变化,特别是蛋氨酸-半胱氨酸循环,嘌呤循环和糖酵解-柠檬酸盐循环。前列腺转录组谱分析确定了药物代谢,脂质和细胞能量,神经肌肉特征,免疫力和炎症以及肿瘤抑制因子/癌基因平衡的基因标志变化。每天的腹膜内注射证实了安全性。注射AGN提取物(200 mg / kg)4周,与饮食途径相比,全身吡喃香豆素暴露量高得多。

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