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Dark chocolate modulates platelet function with a mechanism mediated by flavan-3-ol metabolites

机译:黑巧克力通过黄烷-3-醇代谢物介导的机制调节血小板功能

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摘要

Cocoa is a rich source bioactive compounds, i.e., flavan-3-ols, and its consumption has been associated with several beneficial effects, such as the positive modulation of the hemostasis targeted by the platelet function. However, these phenolic compounds have a very low bioavailability and extensively undergo phase I and II metabolism, with the appearing into the bloodstream of (epi)catechin conjugates and phenyl-γ-valerolactones and their conjugates, at different times.The aims of this study were to explore the effect of dark chocolate on platelet function and to investigate the relationship between this interplay and flavan-3-ol derived metabolites.Eighteen healthy male volunteers ingested 50 g of 90% cocoa chocolate within 5 minutes. Blood samples were collected immediately before chocolate ingestion (T0) and 4 hours afterwards (T1). Platelet function analyzer (PFA)-100 closure time was assessed using collagen/adenosine-5′-diphosphate (COL/ADP) and collagen/epinephrine (COL/EPI) cartridges. Plasma flavan-3-ol metabolites were identified and quantified by means of liquid chromatography coupled to a triple quadrupole mass spectrometer (UHPLC-ESI-MS/MS).Results evidenced a significant increase of COL/ADP-induced PFA-100 closure time, but not COL/EPI, 4 hours after ingestion of dark chocolate. Total plasma structurally-related (epi)catechin metabolite (SREM) concentration significantly increased at T1, together with 4 out of the 6 detected metabolites. Total phenyl-γ-valerolactone concentrations remained unchanged. Spearman correlations evidenced a strong correlation between COL/ADP closure time and SREMs, mainly led by (epi)catechin-sulfate isomers.These data confirm that the potential beneficial effect of dark chocolate on primary hemostasis may be mediated by flavan-3-ol circulating metabolites.
机译:可可是一种来源丰富的生物活性化合物,即黄烷-3-醇,其消费与多种有益作用有关,例如对血小板功能靶向止血的积极调节。但是,这些酚类化合物的生物利用度非常低,并且广泛经历I和II期代谢,并在不同时间出现在(epi)儿茶素结合物和苯基-γ-戊内酯及其结合物的血流中。旨在探讨黑巧克力对血小板功能的影响,并探讨这种相互作用与黄烷-3-醇衍生代谢产物之间的关系。十八名健康男性志愿者在5分钟内摄入了50微克90%可可巧克力。在刚摄入巧克力之前(T0)和之后4个小时(T1)采集血液样本。使用胶原蛋白/腺苷-5'-二磷酸(COL / ADP)和胶原蛋白/肾上腺素(COL / EPI)柱评估血小板功能分析仪(PFA)-100的关闭时间。通过液相色谱-三重四极杆质谱仪(UHPLC-ESI-MS / MS)对血浆flavan-3-ol代谢产物进行鉴定和定量,结果表明COL / ADP诱导的PFA-100闭合时间显着增加,摄入黑巧克力4小时后,但未检测到COL / EPI。 T1时血浆总结构相关的(epi)儿茶素代谢物(SREM)的浓度显着增加,在6种检测到的代谢物中有4种显着增加。总苯基-γ-戊内酯浓度保持不变。 Spearman相关性表明COL / ADP闭合时间与SREM之间存在很强的相关性,主要是由(epi)儿茶素硫酸盐异构体引起的,这些数据证实了黑巧克力对原发止血的潜在有益作用可能是由flavan-3-ol循环介导的代谢产物。

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