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首页> 外文期刊>Life sciences >In vivo biodistribution and pharmacokinetics of (18)F-labeled human C-peptide: evaluation in monkeys using positron emission tomography.
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In vivo biodistribution and pharmacokinetics of (18)F-labeled human C-peptide: evaluation in monkeys using positron emission tomography.

机译:(18)F标记的人C肽的体内生物分布和药代动力学:使用正电子发射断层扫描在猴子中进行评估。

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摘要

The recently observed beneficial effects exerted by C-peptide in insulin-dependent diabetes patients (IDDM) have instigated research into the mechanisms of C-peptide action as well as the location for it. Here we report in vivo biodistribution studies performed in monkeys using positron emission tomography (PET) and C-peptide labeled in the N-terminal with fluorine-18. Following iv injection of the radiotracer, dynamic decay data were collected over the chest and/or abdomens of the monkeys. The radioactivity distributed mainly to the kidneys, less to the heart and to some extent to the liver. Excretion of radioactivity into the urinary bladder was observed. Brain uptake was not detected in a static emission scan of the head performed at late times. Accumulation of radioactivity in the skeleton as a result of in vivo defluorination was not observed. Pharmacokinetic modeling of the regional concentrations of radioactivity over time resulted, for most organs, in two-compartment models. The organs with the highest radioactivity concentrations have been identified, enabling dose estimations for studies in humans with low or no C-peptide.
机译:最近观察到,C肽对胰岛素依赖型糖尿病患者(IDDM)发挥的有益作用已促使人们研究C肽的作用机理及其作用部位。在这里,我们报告了使用正电子发射断层扫描(PET)和在N端用氟18标记的C肽在猴子中进行的体内生物分布研究。静脉注射放射性示踪剂后,在猴子的胸部和/或腹部收集动态衰减数据。放射性主要分布于肾脏,较少分布于心脏,一定程度上分布于肝脏。观察到放射性排泄到膀胱。在后期进行的头部静态发射扫描中未检测到脑吸收。没有观察到由于体内脱氟而导致骨骼中放射性的积累。对于大多数器官,在两室模型中产生了放射性随时间变化的区域浓度的药代动力学模型。已经鉴定出具有最高放射性浓度的器官,从而能够估计剂量,从而在C肽含量低或没有的人中进行研究。

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