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体内生物利用度、吸收、排泄和 [14C]原花青素 B2 在雄性大鼠中的药代动力学。

In vivo bioavailability, absorption, excretion, and pharmacokinetics of [14C]procyanidin B2 in male rats.

机构信息

Division of Nutritional Sciences, Faculty of Health and Medical Sciences, University of Surrey, Guildford, Surrey, United Kingdom.

出版信息

Drug Metab Dispos. 2010 Feb;38(2):287-91. doi: 10.1124/dmd.109.030304. Epub 2009 Nov 12.

DOI:10.1124/dmd.109.030304
PMID:19910517
Abstract

Procyanidins are important biologically active compounds, but the pathway and extent of absorption and metabolism are controversial. We conducted a mass balance study to evaluate the total radioactivity excreted in urine and feces after oral administration of [(14)C]procyanidin B2 to male rats (n = 5). Urine and feces were collected daily from 0 to 96 h. Absolute bioavailability of (14)C from [(14)C]procyanidin B2 was calculated as approximately 82% using the values for total urinary (14)C. A pharmacokinetic study measured total radioactivity in the blood (n = 9). Blood samples were collected at designated time intervals (0.5-24 h) after administration. Three treatments were used: 1) intravenous, 2) oral higher dose (21 mg/kg b.wt.), and 3) oral lower dose (10.5 mg/kg). Blood concentration of total (14)C reached a maximum at approximately 6 h after ingestion of [(14)C]procyanidin B2 (groups II and III), and area under the curve (AUC) was dependent on oral dose. After intravenous or oral administration the terminal half-lives were similar, whereas 8-fold larger values were obtained after oral dosing for total clearance and the apparent volumes of distribution. These pharmacokinetic differences explain the apparently lower (14)C bioavailability (8-11%) for [(14)C]procyanidin calculated from blood [AUC((0-24))] values. After oral administration of [(14)C]procyanidin B2, 63% was excreted via urine within 4 days. The data suggest that much of the parent compound administered orally is degraded by the gut microflora before absorption and that these microbial metabolites have a different distribution from the compounds circulating after the intravenous dose.

摘要

原花青素是重要的生物活性化合物,但它们的吸收和代谢途径和程度存在争议。我们进行了一项质量平衡研究,以评估雄性大鼠口服[(14)C]原花青素 B2 后尿液和粪便中总放射性的排泄量(n = 5)。从 0 到 96 小时每天收集尿液和粪便。使用总尿(14)C 值计算[(14)C]原花青素 B2 的(14)C 绝对生物利用度约为 82%。一项药代动力学研究测量了血液中的总放射性(n = 9)。在给药后指定的时间间隔(0.5-24 小时)采集血样。使用了三种处理方法:1)静脉内,2)口服高剂量(21 mg/kg b.wt.),3)口服低剂量(10.5 mg/kg)。口服[(14)C]原花青素 B2 后约 6 小时,血液中总(14)C 浓度达到峰值(组 II 和 III),曲线下面积(AUC)取决于口服剂量。静脉内或口服给药后,终末半衰期相似,而口服给药后总清除率和表观分布容积的倍数增加 8 倍。这些药代动力学差异解释了从血液[AUC((0-24))]值计算得出的[(14)C]原花青素的生物利用度(8-11%)似乎较低的原因。口服[(14)C]原花青素 B2 后,63%在 4 天内通过尿液排泄。数据表明,口服给予的大部分母体化合物在吸收前被肠道微生物群降解,并且这些微生物代谢物的分布与静脉内剂量后循环的化合物不同。

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