首页> 外文期刊>The Journal of Nutritional Biochemistry >Serum metabolites of proanthocyanidin-administered rats decrease lipid synthesis in HepG2 cells.
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Serum metabolites of proanthocyanidin-administered rats decrease lipid synthesis in HepG2 cells.

机译:原花青素给药大鼠的血清代谢产物减少了HepG2细胞中的脂质合成。

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The regular consumption of flavonoids has been associated with reduced mortality and a decreased risk of cardiovascular diseases. The proanthocyanidins found in plasma are very different from the original flavonoids in food sources. The use of physiologically appropriate conjugates of proanthocyanidins is essential for the in vitro analysis of flavonoid bioactivity. In this study, the effect of different proanthocyanidin-rich extracts, which were obtained from cocoa (CCX), French maritime pine bark (Pycnogenol extract, PYC) and grape seed (GSPE), on lipid homeostasis was evaluated. Hepatic human cells (HepG2 cells) were treated with 25 mg/L of CCX, PYC or GSPE. We also performed in vitro experiments to assess the effect on lipid synthesis that is induced by the bioactive GSPE proanthocyanidins using the physiological metabolites that are present in the serum of GSPE-administered rats. For this, Wistar rats were administered 1 g/kg of GSPE, and serum was collected after 2 h. The semipurified serum of GSPE-administered rats was fully characterized by liquid chromatography tandem triple quadrupole mass spectrometry (LC-QqQ/MS2). The lipids studied in the analyses were free cholesterol (FC), cholesterol ester (CE) and triglycerides (TG). All three proanthocyanidin-rich extracts induced a remarkable decrease in the de novo lipid synthesis in HepG2 cells. Moreover, GSPE rat serum metabolites reduced the total percentage of CE, FC and particularly TG; this reduction was significantly higher than that observed in the cells directly treated with GSPE. In conclusion, the bioactivity of the physiological metabolites that are present in the serum of rats after their ingestion of a proanthocyanidin-rich extract was demonstrated in Hep G2 cells
机译:定期食用类黄酮与降低死亡率和降低心血管疾病的风险有关。血浆中的原花色素与食物中的原始类黄酮有很大不同。原花青素的生理上合适的结合物的使用对于黄酮类生物活性的体外分析至关重要。在这项研究中,评估了从可可(CCX),法国海洋松树皮(碧萝ogen提取物,PYC)和葡萄籽(GSPE)中获得的富含原花青素的不同提取物对脂质稳态的影响。肝人细胞(HepG2细胞)用25 mg / L CCX,PYC或GSPE处理。我们还进行了体外实验,以评估使用GSPE给药大鼠血清中存在的生理代谢产物对生物活性GSPE原花青素诱导的脂质合成的影响。为此,向Wistar大鼠施用1g / kg的GSPE,并在2小时后收集血清。液相色谱串联三重四极杆质谱(LC-QqQ / MS 2 )充分鉴定了GSPE给药大鼠的半纯化血清。分析中研究的脂质为游离胆固醇(FC),胆固醇酯(CE)和甘油三酸酯(TG)。所有这三种富含原花青素的提取物均诱导HepG2细胞中从头脂质合成的显着减少。此外,GSPE大鼠血清代谢产物降低了CE,FC尤其是TG的总百分比;该降低明显高于直接用GSPE处理的细胞中观察到的降低。结论是,在Hep G2细胞中,大鼠摄入富含原花青素的提取物后,其血清中存在的生理代谢物具有生物活性。

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