首页> 美国卫生研究院文献>ACS Medicinal Chemistry Letters >In Vitro Metabolic Stability and in Vivo Biodistribution of 3-Methyl-4-furoxancarbaldehydeUsing PET Imaging in Rats
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In Vitro Metabolic Stability and in Vivo Biodistribution of 3-Methyl-4-furoxancarbaldehydeUsing PET Imaging in Rats

机译:3-甲基-4-呋喃呋喃甲醛的体外代谢稳定性和体内生物分布在大鼠中使用PET成像

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摘要

Painful diabetic neuropathy (PDN) is a type of peripheral neuropathic pain that is currently difficult to treat using clinically available analgesics. Recent work suggests a progressive depletion of nitric oxide (NO) in nerve cells may be responsible for the pathobiology of PDN. The nitric oxide donor, 3-methyl-4-furoxancarbaldehyde (PRG150), has been shown to produce dose-dependent analgesia in a rat model of PDN. To gain insight into the mechanism of analgesia, methods to radiolabel PRG150 were developed to assess the in vivo biodistribution in rats. The furoxan ring was labeled with 13N to follow any nitric oxide release and the 3-methyl substituent was labeled with 11C to track the metabolite using PET imaging. The in vitro metabolic stability of PRG150 was assessed in rat liver microsomes and compared to in vivo metabolism of the synthesized radiotracers. PET images revealed a higher uptake of 13N over 11C radioactivity in the spinal cord. The differences in radioactive uptake could indicate that a NO release in the spinal cord and other components of the somatosensory nervous system may be responsible for the analgesic effects of PRG150 seen in the rat model of PDN.
机译:疼痛性糖尿病性神经病(PDN)是一种周围神经性疼痛,目前难以使用临床上可用的镇痛药进行治疗。最近的工作表明,神经细胞中一氧化氮(NO)的逐渐消耗可能与PDN的病理生物学有关。一氧化氮供体3-甲基-4-呋喃呋喃甲醛(PRG150)已显示在PDN大鼠模型中产生剂量依赖性镇痛作用。为了深入了解镇痛机理,开发了放射性标记PRG150的方法来评估大鼠体内的生物分布。用 13 N标记呋喃喃环以追踪一氧化氮的释放,并使用 11 C标记3-甲基取代基以使用PET成像跟踪代谢物。在大鼠肝微粒体中评估PRG150的体外代谢稳定性,并将其与合成的放射性示踪剂的体内代谢进行比较。 PET图像显示脊髓中 13 C放射性比 11 C更高。放射性吸收的差异可能表明,在PDN大鼠模型中看到的PRG150的镇痛作用可能是脊髓和体感神经系统其他组件中NO释放的原因。

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