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Early Detection of Cerebral Glucose Uptake Changes in the 5XFAD Mouse

机译:5XFAD小鼠中脑葡萄糖摄取变化的早期检测

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摘要

Brain glucose hypometabolism has been observed in Alzheimer’s disease (AD) patients, and is detected with 18F radiolabelled glucose, using positron emission tomography. A pathological hallmark of AD is deposition of brain β-amyloid plaques that may influence cerebral glucose metabolism. The five times familial AD (5XFAD) mouse is a model of brain amyloidosis exhibiting AD-like phenotypes. This study examines brain β-amyloid plaque deposition and 18FDG uptake, to search for an early biomarker distinguishing 5XFAD from wild-type mice. Thus, brain 18FDG uptake and plaque deposition was studied in these mice at age 2, 5 and 13 months. The 5XFAD mice demonstrated significantly reduced brain 18FDG uptake at 13 months relative to wild-type controls but not in younger mice, despite substantial β-amyloid plaque deposition. However, by comparing the ratio of uptake values for glucose in different regions in the same brain, 5XFAD mice could be distinguished from controls at age 2 months. This method of measuring altered glucose metabolism may represent an early biomarker for the progression of amyloid deposition in the brain. We conclude that brain 18FDG uptake can be a sensitive biomarker for early detection of abnormal metabolism in the 5XFAD mouse when alternative relative uptake values are utilized.
机译:在阿尔茨海默氏病(AD)患者中观察到脑葡萄糖代谢异常,并使用正电子发射断层扫描技术通过 18 F放射性标记的葡萄糖进行检测。 AD的病理特征是脑β淀粉样斑块的沉积,其可能影响脑葡萄糖的代谢。五次家族性AD(5XFAD)小鼠是表现出AD样表型的脑淀粉样变性的模型。本研究检查脑β-淀粉样蛋白斑块沉积和 18 FDG摄取,以寻找将5XFAD与野生型小鼠区分开的早期生物标记。因此,研究了这些小鼠在2、5、13个月大时大脑 18 FDG的摄取和斑块沉积。 5XFAD小鼠在13个月时表现出相对于野生型对照组显着降低的脑 18 FDG摄取,但是在年轻的小鼠中却没有,尽管存在大量的β-淀粉样蛋白斑块沉积。但是,通过比较同一大脑中不同区域的葡萄糖摄取值的比率,可以将2个月大的5XFAD小鼠与对照组区分开。这种测量改变的葡萄糖代谢的方法可能代表了淀粉样蛋白在脑内沉积进程的早期生物标志物。我们得出的结论是,当利用其他相对摄取值时,大脑 18 FDG摄取可能是早期检测5XFAD小鼠代谢异常的敏感生物标志物。

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