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A randomized, double-blind, dose-ranging, pilot trial of piperine with resveratrol on the effects on serum levels of resveratrol.一项关于胡椒碱与白藜芦醇对血清白藜芦醇水平影响的随机、双盲、剂量范围探索性试验。
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一项关于胡椒碱与白藜芦醇对血清白藜芦醇水平影响的随机、双盲、剂量范围探索性试验。

A randomized, double-blind, dose-ranging, pilot trial of piperine with resveratrol on the effects on serum levels of resveratrol.

作者信息

Bailey Howard H, Johnson Jeremy J, Lozar Taja, Scarlett Cameron O, Wollmer Barbara W, Kim KyungMann, Havinghurst Thomas, Ahmad Nihal

机构信息

University of Wisconsin, Carbone Cancer Center.

Analytical Instrumentation Center, University of Wisconsin, School of Pharmacy, Madison, Wisconsin.

出版信息

Eur J Cancer Prev. 2021 May 1;30(3):285-290. doi: 10.1097/CEJ.0000000000000621.

DOI:10.1097/CEJ.0000000000000621
PMID:32868637
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7910313/
Abstract

Resveratrol (3,4,5-trihydroxystilbene) is a naturally occurring phytoalexin with purported health-promoting effects, but with limited oral bioavailability. Our prior murine modeling research observed enhanced resveratrol bioavailability with piperine co-administration. In this study, single-dose pharmacokinetics of resveratrol with or without piperine and the associated toxicities were studied on a cohort of healthy volunteers. We performed a double-blind, randomized, three-arm pilot study. Participants were randomized to receive a single dose of resveratrol 2.5 g, with piperine in 0 mg, 5 mg, or 25 mg dose. An improved liquid chromatography/mass spectrometry assay was used to determine serum levels of resveratrol and resveratrol-glucuronide. Baseline through 24 h post-study drug serum analyses were performed and adverse events were followed for 30 days. Twenty-four participants were enroled. No significant relationship between dose and pharmacokinetic values were found. In the sex stratified analysis, Cmax for resveratrol in women showed a trend (P = 0.057) toward an increase with piperine. Pharmacokinetic values for resveratrol were: Cmax - 18.5 ± 16 ng/mL resveratrol alone, 29 ± 29 resveratrol + 5 mg piperine, 16 ± 13 resveratrol + 25 mg piperine; area under the concentration × time curve - 1270 ± 852 ng/h/mL resveratrol alone, 2083 ± 2284 resveratrol + 5 mg piperine, 1132 ± 222 resveratrol + 25 mg piperine. All subjects tolerated their protocol therapy with minimal to no toxicity and no evidence of differences between the three groups. The co-administration of resveratrol with piperine at 5 and 25 mg doses did not sufficiently alter the pharmacokinetics of resveratrol or resveratrol-glucuronide to demonstrate the significant enhancement observed in murine modeling.

摘要

白藜芦醇(3,4,5 - 三羟基茋)是一种天然存在的植物抗毒素,据称具有促进健康的作用,但口服生物利用度有限。我们之前的小鼠模型研究观察到,联合使用胡椒碱可提高白藜芦醇的生物利用度。在本研究中,我们对一组健康志愿者研究了单独使用或联合使用胡椒碱时白藜芦醇的单剂量药代动力学及相关毒性。我们进行了一项双盲、随机、三臂试点研究。参与者被随机分配接受单剂量2.5 g白藜芦醇,分别联合0 mg、5 mg或25 mg剂量的胡椒碱。采用改进的液相色谱/质谱分析法测定血清中白藜芦醇和白藜芦醇 - 葡萄糖醛酸苷的水平。在研究药物给药后,进行了从基线到24小时的血清分析,并对不良事件进行了30天的跟踪。共招募了24名参与者。未发现剂量与药代动力学值之间存在显著关系。在按性别分层分析中,女性白藜芦醇的Cmax显示出随着胡椒碱剂量增加而升高的趋势(P = 0.057)。白藜芦醇的药代动力学值为:单独使用白藜芦醇时,Cmax为18.5±16 ng/mL;白藜芦醇 + 5 mg胡椒碱时,Cmax为29±29 ng/mL;白藜芦醇 + 25 mg胡椒碱时,Cmax为16±13 ng/mL;浓度×时间曲线下面积:单独使用白藜芦醇时为1270±852 ng/h/mL;白藜芦醇 + 5 mg胡椒碱时为2083±2284 ng/h/mL;白藜芦醇 + 25 mg胡椒碱时为1132±222 ng/h/mL。所有受试者对其方案治疗耐受性良好且毒性极小或无毒性,且未发现三组之间存在差异的证据。联合使用5 mg和25 mg剂量的胡椒碱与白藜芦醇并未充分改变白藜芦醇或白藜芦醇 - 葡萄糖醛酸苷的药代动力学,未能证明在小鼠模型中观察到的显著增强效果。