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Ibopamine (SKF 100168) pharmacokinetics in relation to the timing of meals.

机译:伊波巴明(SK&F 100168)与进餐时间有关的药代动力学。

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摘要

The effect of the timing of a standard meal relative to a single oral dose of 200 mg ibopamine, on the appearance of its pharmacologically active metabolite, epinine, in plasma was investigated in a randomised crossover study in 12 healthy volunteers. After a 12 h fast, ibopamine was administered either in the fasting state (no meal), or 1 h before, 0.5 h before, immediately after, 2 h after or 3 h after a standardised meal. Blood samples taken immediately before and at intervals for 3 h after dosing were analysed for free epinine. Maximum concentration (Cmax), time to Cmax(tmax), and area under the concentration-time curve (AUC) for free epinine in plasma were calculated. When compared with the fasting state, Cmax and AUC0-3h were significantly reduced when ibopamine was given immediately after or 2 h after a meal. AUC was also reduced for ibopamine given 0.5 h before a meal. tmax was significantly delayed when ibopamine was given immediately after, or 2 or 3 h after a meal. Thus, administration of ibopamine with or shortly after a meal reduced the rate and extent of appearance of free epinine in plasma. The clinical significance of reduced epinine levels on acute dosing in the presence of food is unknown.
机译:在一项针对12名健康志愿者的随机交叉研究中,研究了相对于单次口服200 mg ibopamine相对于血浆其药理活性代谢物epinine而言,标准进餐时间的影响。禁食12小时后,以禁食状态(不进餐)或在标准化餐前1小时,0.5小时之前,0.5小时后,紧随其后,2小时后或3小时后给予伊巴巴明。在给药前和给药后3小时的间隔中采集的血液样品中分析了游离表皮胺。计算血浆中游离游离胺的最大浓度(Cmax),达到Cmax的时间(tmax)和浓度-时间曲线下的面积(AUC)。与禁食状态相比,饭后立即或饭后2小时给予伊巴巴明可明显降低Cmax和AUC0-3h。饭前0.5小时给予伊巴胺,AUC也降低。饭后或饭后2或3小时服用ibopamine时,tmax明显延迟。因此,在饭后或饭后不久服用伊巴巴明降低了血浆中游离表皮胺的出现速率和程度。在有食物的情况下,急性剂量降低的表皮胺水平的临床意义尚不清楚。

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