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首页> 外文OA文献 >Pharmacokinetics of ceftazidime in serum and suction blister fluid during continuous and intermittent infusions in healthy volunteers.
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Pharmacokinetics of ceftazidime in serum and suction blister fluid during continuous and intermittent infusions in healthy volunteers.

机译:在健康志愿者中连续和间歇输注期间,头孢他啶在血清和吸水疱液中的药代动力学。

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The pharmacokinetics of ceftazidime were investigated during intermittent (II) and continuous (CI) infusion in eight healthy male volunteers in a crossover fashion. The total daily dose was 75 mg/kg of body weight per 24 h in both regimens, given in three doses of 25 mg/kg/8 h (II) or 60 mg/kg/24 h with 15 mg/kg as a loading dose (CI). After the third dose (II) and during CI, serum and blister fluid samples were taken. Seven new blisters were raised for each timed sample by a suction blister technique. Blisters took 90 min to form. Samples were then taken from four blisters (A samples) and 1 h later were taken from the remaining three (B samples). The concentration of ceftazidime was determined using a high-performance liquid chromatography method. After II, the concentrations in serum immediately after infusion (t = 30 min) and 8 h after the start of the infusion were 137.9 (standard deviation [SD], 27.5) and 4.0 (SD, 0.7) micrograms/ml, respectively. The half-life at alpha phase (t1/2 alpha) was 9.6 min (SD, 4.6), t1/2 beta was 94.8 min (SD, 5.4), area under the concentration-time curve (AUC) was 285.4 micrograms.h/ml (SD, 22.7), total body clearance was 0.115 liter/h.kg (SD, 0.022), and volume of distribution at steady state was 0.178 liter/kg (SD, 0.023). The blister fluid (A) samples showed a decline in concentration parallel to that of the concentrations in serum during the elimination phase with a ratio of 1:1. The t1/2 of the A samples was 96.4 min (SD, 3.2). The concentration of ceftazidime in the B blister fluid samples was significantly higher (27%) than in the A samples over time. This shows that blisters may behave as a separate compartment and establishes the need to raise new blisters for each timed sample. The mean AUC/h during continuous infusion was 21.3 micrograms . h/ml (SD, 3.0). The total body clearance was 0.113 liter/h . kg (SD, 0.018), the urinary clearance was 0.105 liter/h . kg (SD, 0.012), and the ceftazidime/creatinine clearance ratio was 0.885. The mean AUC of blister fluid per hour was 84.5% (18.0 micrograms . h/liter; SD, 3.6) compared with that of serum. The A samples did not differ significantly from the B samples. The implications of continuous infusion of beta-lactams for treatment of serious infections are discussed.
机译:头孢他啶的药代动力学以交叉方式在八名健康男性志愿者的间歇(II)和连续(CI)输注期间进行了研究。在两种方案中,每日总剂量为每24小时75 mg / kg体重,分25剂量/ kg / 8 h(II)或60 mg / kg / 24 h三种剂量给予,每次负荷15 mg / kg剂量(CI)。在第三剂(II)后和CI期间,采集血清和起泡液样品。通过抽吸水泡技术为每个定时的样品培养了七个新的水泡。水泡花了90分钟形成。然后从四个水泡(A样品)中取样,并在1小时后从其余三个水泡(B样品)中取样。使用高效液相色谱法测定头孢他啶的浓度。 II后,立即输注后(t = 30分钟)和开始输注后8 h血清中的浓度分别为137.9(标准偏差[SD],27.5)和4.0(SD,0.7)微克/毫升。在α相的半衰期(t1 / 2 alpha)为9.6分钟(SD,4.6),t1 / 2 beta为94.8 min(SD,5.4),浓度-时间曲线下的面积(AUC)为285.4微克.h / ml(SD,22.7),全身清除率为0.115升/小时·千克(SD,0.022),稳态分布体积为0.178升/ kg(SD,0.023)。在消除阶段,起泡液(A)样品的浓度下降与血清中浓度平行,比率为1:1。 A样品的t1 / 2为96.4分钟(标准差,3.2)。随着时间的推移,B泡罩液样品中头孢他啶的浓度显着高于A样品(27%)。这表明水泡可能表现为一个单独的隔室,并确定了需要为每个定时样品培养新的水泡。连续输注期间的平均AUC / h为21.3微克。 h / ml(SD,3.0)。全身清除率为0.113升/小时。千克(SD,0.018),尿清除率为0.105升/小时。千克(SD,0.012),头孢他啶/肌酐清除率是0.885。与血清相比,每小时起泡液的平均AUC为84.5%(18.0微克。小时/升; SD,3.6)。 A样品与B样品没有显着差异。讨论了持续输注β-内酰胺对治疗严重感染的影响。

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