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Neurobehavioral Abnormalities in the HIV-1 Transgenic Rat Do Not Correspond to Neuronal Hypometabolism on 18F-FDG-PET

机译:HIV-1转基因大鼠的神经行为异常与18F-FDG-PET上的神经元代谢分解不对应

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摘要

Motor and behavioral abnormalities are common presentations among individuals with HIV-1 associated neurocognitive disorders (HAND). We investigated whether longitudinal motor and behavioral performance in the HIV-1 transgenic rat (Tg), a commonly used neuro-HIV model, corresponded to in vivo neuronal death/dysfunction, by using rotarod and open field testing in parallel to [18F] 2-fluoro-2-deoxy-D-glucose (FDG) positron emission tomography (PET). We demonstrated that age-matched non-Tg wild type (WT) rats outperformed the HIV-1 Tg rats at most time points on rotarod testing. Habituation to rotarod occurred at 8 weeks of age (fifth weekly testing session) in the WT rats but it never occurred in the Tg rats, suggesting deficits in motor learning. Similarly, in open field testing, WT rats outperformed the Tg rats at most time points, suggesting defective exploratory/motor behavior and increased emotionality in the Tg rat. Despite the neurobehavioral abnormalities, there were no concomitant deficits in 18F-FDG uptake in Tg rats on PET compared to age-matched WT rats and no significant longitudinal loss of FDG uptake in either group. The negative PET findings were confirmed using 14C- Deoxy-D-glucose autoradiography in 32 week-old Tg and WT rats. We believe that the neuropathology in the HIV-1 Tg rat is more likely a consequence of neuronal dysfunction rather than overt neurodegenerationeuronal cell death, similar to what is seen in HIV-positive patients in the post-ART era.
机译:在具有HIV-1相关神经认知障碍(HAND)的个体中,运动和行为异常是常见的表现。通过平行于[]的旋转脚踏车和露天试验,我们调查了HIV-1转基因大鼠(Tg)(一种常用的神经-HIV模型)中的纵向运动和行为表现是否与体内神经元死亡/功能障碍相对应。 18 F] 2-氟-2-脱氧-D-葡萄糖(FDG)正电子发射断层扫描(PET)。我们证明了年龄匹配的非Tg野生型(WT)大鼠在旋转脚架测试的大多数时间点都胜过HIV-1 Tg大鼠。 WT大鼠在8周龄(第五次每周测试)时习惯于轮状动物,但在Tg大鼠中从未发生过,这表明运动学习有缺陷。同样,在野外试验中,WT大鼠在大多数时间点上都比Tg大鼠好,这表明Tg大鼠的探索性/运动行为缺陷和情绪增强。尽管存在神经行为异常,但与年龄匹配的WT大鼠相比,PET的Tg大鼠的 18 F-FDG摄取没有伴随的缺陷,并且两组的FDG摄取均没有明显的纵向损失。 PET阴性结果通过32周龄Tg和WT大鼠的 14 C-脱氧-D-葡萄糖放射自显影证实。我们认为,HIV-1 Tg大鼠的神经病理学很可能是神经元功能障碍的结果,而不是明显的神经变性/神经元细胞死亡,这与后ART时代HIV阳性患者的情况相似。

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