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Aspirin eugenol ester regulates cecal contents metabolomic profile and microbiota in an animal model of hyperlipidemia

机译:阿司匹林丁香酚酯在高脂血症的动物模型中调节肠含量代谢组型和微生物群

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摘要

Abstract Background Hyperlipidemia, with an increasing of prevalence, has become one of the common metabolic diseases in companion animal clinic. Aspirin eugenol ester (AEE) is a novel compound that exhibits efficacious anti-hyperlipidemia activities. However, its mechanisms are still not completely known. The objective of present study was to investigate the intervention effects of AEE on cecal contents metabonomics profile and microbiota in hyperlipidemia rats. Results Three groups of rats were fed with a control diet, or high fat diet (HFD) containing or not AEE. The results showed the beneficial effects of AEE in HFD-fed rats such as the reducing of aspartate aminotransferase (AST) and total cholesterol (TCH). Distinct changes in metabonomics profile of cecal contents were observed among control, model and AEE groups. HFD-induced alterations of eight metabolites in cecal contents mainly related with purine metabolism, linoleic acid metabolism, glycerophospholipid metabolism, sphingolipid metabolism and pyrimidine metabolism were reversed by AEE treatment. Principal coordinate analysis (PCoA) and cluster analysis of microbiota showed altered patterns with distinct differences in AEE group versus model group, indicating that AEE treatment improved the negative effects caused by HFD on cecal microbiota. In addition, the correction analysis revealed the possible link between the identified metabolites and cecal microbiota. Conclusions This study showed regulation effects of AEE on cecal contents metabonomics profile and microbiota, which could provide information to reveal the possible underlying mechanism of AEE on hyperlipidemia treatment.
机译:摘要背景高脂血症随着患病率的增加,已成为伴侣动物诊所的常见代谢疾病之一。阿司匹林丁香酚酯(AEE)是一种新型化合物,其具有有效的抗高脂血症活性。然而,其机制仍然没有完全知道。目前研究的目的是探讨AEE对高脂血症大鼠肠内含量代谢农法谱和微生物群的干预效果。结果含有三组大鼠,用对照饮食,或含有AEE的高脂饮食(HFD)。结果表明AEE在HFD喂养大鼠中的有益作用,例如还原天冬氨酸氨基转移酶(AST)和总胆固醇(TCH)。在对照,模型和AEE群体中观察到盲肠内容物的不同变化。通过AEE治疗,HFD诱导的含有嘌呤代谢,亚油酸代谢,甘油代谢和嘧啶代谢和嘧啶代谢与丙烯酸代谢,甘油磷脂代谢和嘧啶代谢的改变。 Microbiota的主坐标分析(PCOA)和微生物群的聚类分析表明,AEE群与模型组不同差异的改变模式,表明AEE治疗改善了HFD对肠髓癌患者引起的负面影响。此外,校正分析揭示了所鉴定的代谢物和肠髓微生物之间可能的联系。结论本研究表明AEE对肠内含量的调节作用,可以提供信息,揭示AEE对高脂血症治疗的可能潜在机制。

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