Pharmacokinetic interaction between indoramin and ethanol.

Human toxicology Pub Date : 1989-05-01 DOI:10.1177/096032718900800306

S M Abrams, D M Pierce, A Johnston, A Hedges, R A Franklin, P Turner

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引用次数: 3

Abstract

1. The effect of ethanol consumption (0.5 g/kg) on the pharmacokinetics of the alpha adrenoceptor antagonist indoramin, administered orally (50 mg) or intravenously (0.175 mg/kg) has been investigated in young volunteers. Sedation was also assessed using a visual analogue scale. 2. After oral indoramin administration, ethanol caused increases of 58% (P less than 0.01) in Cpmax, and 25% (P less than 0.05) in AUC. There was no effect of alcohol on elimination half-life. The combination of ethanol and indoramin was more sedative than indoramin alone. 3. Ethanol did not alter the pharmacokinetics of an intravenous dose of indoramin. However indoramin caused a small but statistically significant increase (26%) in blood ethanol concentrations during the first 1.25 h after dosing. Both indoramin and ethanol caused sedation. 4. The increased bioavailability of oral indoramin in the presence of ethanol may reflect some enhanced absorption, but it is also consistent with inhibition of first-pass metabolism of a flow-limited drug. The clinical implications are discussed.

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吲哚胺与乙醇的药动学相互作用。

1. 在年轻志愿者中研究了乙醇消耗量(0.5 g/kg)对α肾上腺素受体拮抗剂吲哚明的药代动力学影响，分别口服(50 mg)或静脉注射(0.175 mg/kg)。镇静也用视觉模拟量表进行评估。2. 口服吲哚胺后，乙醇使Cpmax升高58% (P < 0.01)， AUC升高25% (P < 0.05)。酒精对消除半衰期没有影响。乙醇与吲哚胺联用比单用具有更强的镇静作用。3.乙醇不改变静脉注射吲哚明的药代动力学。然而，在给药后的前1.25小时内，吲哚明引起了血液乙醇浓度的小幅但有统计学意义的增加(26%)。吲哚胺和乙醇都能起到镇静作用。4. 在乙醇的存在下，口服吲哚胺的生物利用度增加可能反映了一些吸收增强，但这也与血流受限药物的首过代谢抑制一致。并讨论了临床意义。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Human toxicology

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