首页> 外文期刊>Journal of Chromatography, Biomedical Applications >Measuremetn and pharmacokinetic analysis of unbound ceftazidime inrat blood using microdialysis and microbore liquid chromatography
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Measuremetn and pharmacokinetic analysis of unbound ceftazidime inrat blood using microdialysis and microbore liquid chromatography

机译:微透析和微孔液相色谱法测定未结合的头孢他啶大鼠血的药代动力学

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摘要

To evaluate the biodisposition of ceftazidime in rat blood, a rapid and simple microbore liquid chromatographic technique together with a microdialysis sampling technique were developed. This method involves an on-line design for blood dialysate directly injected into a microbore liquid chromatographic system. The chromatographic conditions consisted of a mobile phase of methanol—acetonitrile—l00 mM monosodium phosphoric acid (pH 3.0) (10:10:80. v/Wv) pumped through a microbore reversed-phase column at a flow-rate of 0.05 mi/mm. With the detection wavelength set at 254 nra, a good linear correlation was observed between the peak area and the ceftazidime concentration at 0.1 to 50 ~xgi1 (r = 0.999). Microdialysis probes, being custom-made, were screened for acceptable in vivo recovery while chromatographic resolution and detection were validated for response linearity, as well as intra-day and inter-day variabilities. This method was then applied to the pharmacokinetic profiling of ceftazidime in blood following intravenous 50 mg/kg administration to rats. The pharmacokinetics was calculated from the corrected data for dialysate concentrations of ceftazidime versus time. This method has been used to study ceftazidime pharmacokinetics in rats and has proven to be rapid and reproducible.
机译:为了评估头孢他啶在大鼠血液中的生物分布,开发了一种快速,简单的微孔液相色谱技术以及微透析采样技术。此方法涉及直接注入微孔液相色谱系统中的血液透析液的在线设计。色谱条件包括流动相为甲醇-乙腈-100 mM磷酸一钠磷酸(pH 3.0)(10:10:80.v / Wv),流动相以0.05 mi / m的流速泵入微孔反相柱。毫米将检测波长设置为254 nra,观察到峰面积与头孢他啶浓度在0.1至50〜xg / ni1之间具有良好的线性相关性(r = 0.999)。对定制的微透析探针进行了筛选,筛选出可接受的体内回收率,同时验证了色谱分离度和检测的响应线性以及日间和日间变异性。然后将这种方法应用于对大鼠进行静脉内50 mg / kg剂量的头孢他啶的药代动力学分析。由头孢他啶透析液浓度相对于时间的校正数据计算出药代动力学。该方法已用于研究大鼠头孢他啶的药代动力学,并已证明是快速且可重现的。

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