首页> 美国卫生研究院文献>Antimicrobial Agents and Chemotherapy >Heat Treatment of Amphotericin B Modifies Its Serum Pharmacokinetics Tissue Distribution and Renal Toxicity following Administration of a Single Intravenous Dose to Rabbits
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Heat Treatment of Amphotericin B Modifies Its Serum Pharmacokinetics Tissue Distribution and Renal Toxicity following Administration of a Single Intravenous Dose to Rabbits

机译:对兔子进行单一静脉给药后两性霉素B的热处理会改变其血清药代动力学组织分布和肾脏毒性。

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摘要

The purpose of this investigation was to determine the serum pharmacokinetics, tissue distribution, and renal toxicity of amphotericin B (AmpB) following administration of a single intravenous dose (1 mg/kg of body weight) of Fungizone (FZ) and a heat-treated form of FZ (HFZ) to New Zealand White female rabbits. FZ solutions were heated at 70°C for 20 min to produce HFZ. Blood samples were obtained before drug administration and serially thereafter. After collection of the 48-h blood sample, each rabbit was humanely sacrificed and the right kidney, spleen, lungs, liver, and heart were harvested for AmpB analysis. Serum creatinine levels were measured before and 10 h after drug administration. AmpB concentrations in the serum and tissues were analyzed using high-performance liquid chromatography. FZ administration to rabbits resulted in a greater-than-50% increase in serum creatinine concentrations compared to baseline. However, HFZ administration resulted in no difference in serum creatinine concentrations compared to baseline. The AmpB area under the concentration-time curve (AUC) after HFZ administration was significantly lower than the AmpB AUC in rabbits administered FZ. However, AmpB systemic total body clearance was significantly greater in rabbits administered HFZ than in rabbits administered FZ without any differences in volume of distribution at steady state. Kidney tissue AmpB concentrations, although not significantly different, were greater in rabbits administered FZ than in rabbits administered HFZ. Likewise, lung and spleen AmpB concentrations, although not significantly different, were greater in rabbits administered FZ than in rabbits administered HFZ. However, liver AmpB concentrations were significantly lower in rabbits administered FZ than in rabbits administered HFZ. No significant differences in heart AmpB concentration between rabbits administered FZ and those given HFZ were found. These findings suggest that the pharmacokinetics, tissue distribution, and renal toxicity of AmpB are modified following administration of HFZ. HFZ could be an improved low-cost AmpB drug delivery system that has a potentially higher therapeutic index than FZ.
机译:这项研究的目的是确定单次静脉注射剂量(1 mg / kg体重)的真菌区(FZ)和热处理后的两性霉素B(AmpB)的血清药代动力学,组织分布和肾毒性FZ(HFZ)的形式对新西兰白母兔。将FZ溶液在70°C加热20分钟以生产HFZ。在给药之前和之后连续采集血液样品。收集48小时血液样本后,将每只兔子人道处死,并采集右肾,脾,肺,肝和心脏进行AmpB分析。在给药前和给药后10小时测量血清肌酐水平。使用高效液相色谱法分析血清和组织中的AmpB浓度。与基线相比,对兔进行FZ给药可使血清肌酐浓度增加超过50%。但是,与基线相比,HFZ给药导致血清肌酐浓度无差异。 HFZ给药后,浓度-时间曲线下的AmpB面积显着低于FZ给药的兔子中的AmpB AUC。但是,HFZ兔的AmpB全身总清除率明显高于FZ兔,稳态时分布体积无任何差异。给予FZ的兔子的肾脏组织AmpB浓度虽然没有显着差异,但高于给予HFZ的兔子。同样,给予FZ的兔子的肺和脾AmpB浓度虽然没有显着差异,但高于给予HFZ的兔子。但是,给予FZ的兔子的肝脏AmpB浓度明显低于给予HFZ的兔子。在给予FZ的兔子和给予HFZ的兔子之间,心脏AmpB浓度没有显着差异。这些发现表明,HFZ给药后,AmpB的药代动力学,组织分布和肾毒性得到改善。 HFZ可能是一种改进的低成本AmpB药物递送系统,其治疗指数可能高于FZ。

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