首页> 美国卫生研究院文献>Antimicrobial Agents and Chemotherapy >Pharmacokinetics of intravenous cefetamet (Ro 15-8074) and oral cefetamet pivoxil (Ro 15-8075) in young and elderly subjects.
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Pharmacokinetics of intravenous cefetamet (Ro 15-8074) and oral cefetamet pivoxil (Ro 15-8075) in young and elderly subjects.

机译:静脉注射头孢他美特(Ro 15-8074)和口服头孢他美酯(左15-8075)在年轻和老年受试者中的药代动力学。

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摘要

The purpose of this investigation was to evaluate the effect of advanced age on the pharmacokinetics of cefetamet and its prodrug, cefetamet pivoxil. A secondary objective of this study was to assess the effect of food on the absorption of cefetamet pivoxil in the elderly. Twenty-four healthy subjects (twelve young and twelve elderly) received (in a Latin square design) a single-dose, 515-mg infusion of cefetamet, a single 1,000-mg oral dose of cefetamet pivoxil during fasted conditions, and a single 1,000-mg oral dose of cefetamet pivoxil 10 min after a standardized low-fat breakfast. Serial blood and urine samples were collected over a 36-h period and analyzed by high-performance liquid chromatography. Intravenous and oral pharmacokinetic parameters were obtained by using model-independent techniques. The systemic clearance and renal clearance of cefetamet were significantly lower (P less than 0.05) in elderly subjects compared with in young controls after intravenous administration. No significant difference was observed in the apparent volumes of distribution at steady state between the two groups. Consequently, half-life and mean residence time were prolonged. A trend toward a lower renal clearance/creatinine clearance ratio was observed in our elderly population. Oral clearance of cefetamet was only slightly reduced in our elderly subjects, consistent with an increase in plasma half-life. Otherwise, oral pharmacokinetic parameters were comparable between elderly and young subjects. Additionally, the same effects of food were observed on the absorption characteristics of cefetamet (no change in maximum concentration of drug in plasma and an increase in both time to maximum concentration of drug in plasma and bioavailability) in our elderly subjects as in our young volunteers. Age did not appear to alter the deesterification and bioavailability of cefetamet pivoxil. We conclude that the small reduction in the elimination of cefetamet in the elderly would not require dose adjustment for this population.
机译:这项研究的目的是评估高龄对头孢他美及其前体药物头孢他美匹伏昔的药代动力学的影响。这项研究的第二个目的是评估食物对老年人头孢他美酯吸收的影响。 24名健康受试者(十二岁和十二岁的老人)(按拉丁方设计)接受了单剂量515 mg的头孢他美特输注,在禁食期间口服1,000毫克的头孢他美酯的口服剂量和1,000例标准化的低脂早餐后10分钟服用-mg的头孢他美酯口服剂量。在36小时内收集了一系列血液和尿液样本,并通过高效液相色谱进行了分析。通过使用与模型无关的技术获得静脉和口服药代动力学参数。与静脉注射后的年轻对照组相比,老年受试者的头孢他美的全身清除率和肾脏清除率显着降低(P小于0.05)。两组之间在稳态下的表观分布量没有观察到显着差异。因此,延长了半衰期和平均停留时间。在我们的老年人群中,观察到肾脏清除率/肌酐清除率降低的趋势。在我们的老年受试者中,头孢他美的口服清除率仅略微降低,这与血浆半衰期的增加相一致。否则,老年和青年受试者的口服药代动力学参数相当。此外,在老年受试者中,食物对头孢他美的吸收特性具有相同的影响(血浆中最大药物浓度无变化,血浆中最大药物浓度的时间和生物利用度均增加) 。年龄似乎没有改变头孢他美酯的脱酯作用和生物利用度。我们得出的结论是,老年人中消除头孢他美的少量减少将不需要对该人群进行剂量调整。

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