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Water-soluble polyphenol-rich clove extract lowers pre- and post-prandial blood glucose levels in healthy and prediabetic volunteers: an open label pilot study

机译:富含水溶性多酚的丁香提取物降低了健康和前脂肪的血糖水平和伪造的血糖水平:开放标签试验研究

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摘要

Abstract Background/objectives Type 2 diabetes (T2D) is a global pandemic, and contributes significantly to the increasing incidence of conditions such as cardiovascular disease (CVD). Postprandial plasma glucose measured 2-h after the start of a meal is a good indicator of the overall status of glucose homeostasis. Clove (Syzygium aromaticum L.) and its essential oils (eugenol and acetyl eugenol) have been shown in preclinical studies to modulate pathways involved in glucose homeostasis. In addition, a water-soluble polyphenolic extract of unopened clove buds was recently shown to benefit liver function and redox status. Therefore, we conducted an open-label pilot study to test whether this polyphenolic clove extract (PCE) could influence glucose metabolism. Methods We evaluated the effect of PCE supplementation (250 mg once daily for 30 days) on preprandial glucose levels and 2-h postprandial glucose levels in 13 otherwise healthy volunteers who were stratified into two groups according to their initial preprandial glucose levels: Group I (n = 7) ≤100 mg/dL, Group II (n = 6) – between 101 and 125 mg/dL. In an effort to elucidate the molecular mechanisms of PCE action, we tested in vitro the effects of PCE on glucose uptake, hepatocyte glucose production, and carbohydrate hydrolyzing enzymes. Results At day 12 of supplementation, we observed statistically significant reductions in mean postprandial glucose levels in both groups [(Group I: Initial - Day 12 PPG = 13.29 mg/dL, 95% CI: 3.329–23.24) (Group II: Initial – Day 12 PPG = 16.67 mg/dL, 95% CI: 4.687–28.65, P = 0.0159)], which continued through study completion at day 30. PCE supplementation significantly decreased mean preprandial glucose levels only in Group II at Days 24 (Initial – Day 24 = 13.00 mg/dL, 95% CI: 1.407–24.59, P = 0.0345) and 30 (Initial – Day 30 = 13.67 mg/dL, 95% CI: 5.766–21.57, P = 0.0067). In cell-based assays, PCE enhanced glucose uptake in L6 myocytes and inhibited hepatocyte glucose production HepG2 cells. In cell-free assays, PCE inhibited α-amylase activity and α-glucosidase activity. Conclusions These findings underscore the therapeutic utility of PCE for maintaining healthy glucose metabolism and warrant further larger-scale clinical trials. Trial registration This trial was retrospectively registered in the ISRCTN registry on September 29, 2018 (ISRCTN15680985).
机译:抽象背景/目标2型糖尿病(T2D)是全球性大流行,并对心血管疾病(CVD)等病症的发病率显着贡献。餐后血浆葡萄糖在膳食开始后测量2-H是葡萄糖稳态的总体状态的良好指标。丁香(Syzygium aromaticum L.)及其精油(丁香酚和乙酰丁醇)已在临床前研究中显示,以调节葡萄糖稳态的途径。此外,最近显示了未开封的瓣芽芽的水溶性多酚提取物,以益处肝功能和氧化还原状态。因此,我们进行了一个开放标签的试验研究以测试这种多酚丁香提取物(PCE)是否可以影响葡萄糖代谢。方法评估PCE补充剂(每日250毫克每天服用30天)的效果,在13个健康的志愿者中,根据其初始预葡萄糖水平分为两组的另一种健康的志愿者:I组( n = 7)≤100mg/ dl,II族(n = 6) - 在101和125mg / dl之间。为了阐明PCE作用的分子机制,我们在体外测试了PCE对葡萄糖摄取,肝细胞葡萄糖生产和碳水化合物水解酶的影响。结果在补充的第12天,我们观察到两组的平均餐后葡萄糖水平的统计学显着减少[(第I组:初始 - 第12天PPG = 13.29 mg / dL,95%CI:3.329-23.24)(II组:初始 - 第12天ppg = 16.67mg / dl,95%CI:4.687-28.65,p = 0.0159)],通过第30天进行研究完成.PCE补充在第24天(第24天)仅在第II组中显着降低了平均预葡萄糖水平(初始 - 第24天= 13.00 mg / dl,95%CI:1.407-24.59,P = 0.0345)和30(首字母 - 第30天= 13.67mg / DL,95%CI:5.766-21.57,P = 0.0067)。在基于细胞的测定中,PCE在L6肌细胞中增强葡萄糖摄取并抑制肝细胞葡萄糖生产HepG2细胞。在无细胞测定中,PCE抑制α-淀粉酶活性和α-葡糖苷酶活性。结论这些发现强调了PCE治疗健康葡萄糖新陈代谢的治疗效用,并提供进一步的大规模临床试验。试用注册本试验在2018年9月29日(ISRCTN15680985)的ISRCTN登记处回顾性地注册。

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