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Inhibitory Effects of Yuzu and Its Components on Human Platelet Aggregation
Authors:Tae-Ho Kim  Hye-Min Kim  Se Won Park  Yi-Sook Jung
Affiliation:1.College of Pharmacy, Ajou University, Suwon 443-749, Republic of Korea;2.Department of Molecular Biotechnology, College of Life and Environmental Sciences, Konkuk University, Seoul 143-701, Republic of Korea;3.College of Pharmacy, Research Institute of Pharmaceutical Sciences and Technology, Ajou University, Suwon 443-749, Republic of Korea
Abstract:Our previous study demonstrated that yuzu has an anti-platelet effect in rat blood. In the present study, we examined whether the anti-platelet effect of yuzu can be extended to human blood by investigating its ability to inhibit aggregations induced by various agonists in human platelet rich plasma (PRP). This study also investigated the underlying mechanism of yuzu focusing on ADP granule secretion, TXB2 formations, and PLCγ/Akt signaling. The results from this study showed that ethanolic yuzu extract (YE), and its components, hesperidin and naringin, inhibited human platelet aggregation in a concentration-dependent manner. YE, hesperidin and naringin also inhibited TXB2 formation and ADP release. The phosphorylation of PLCγ and Akt was significantly inhibited by YE, heperidin and naringin. Furthermore, we demonstrated that YE, heperidin and naringin has anti-platelet effects in rat ex vivo studies, and lower side effects in mice tail bleeding time studies. The results from this study suggest that YE, hesperidin and naringin can inhibit human platelet aggregation, at least partly through the inhibition of PLCγ and Akt, leading to a decrease in TXB2 formation and granule secretion.
Keywords:Yuzu   Hesperidin   Naringin   Platelet   Aggregation
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