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首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Plaque-associated disruption of CSF and plasma amyloid-beta (Abeta) equilibrium in a mouse model of Alzheimer's disease.
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Plaque-associated disruption of CSF and plasma amyloid-beta (Abeta) equilibrium in a mouse model of Alzheimer's disease.

机译:在阿尔茨海默氏病小鼠模型中与斑块相关的CSF破坏和血浆淀粉样β(Abeta)平衡。

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摘要

To better understand amyloid-beta (Abeta) metabolism in vivo, we assessed the concentration of Abeta in the CSF and plasma of APP(V717F) (PDAPP) transgenic mice, a model that develops age-dependent Alzheimer's disease (AD)-like pathology. In 3-month-old mice, prior to the development of Abeta deposition in the brain, there was a highly significant correlation between Abeta levels in CSF and plasma. In 9-month-old-mice, an age at which some but not all mice have developed Abeta deposition, there was also a significant correlation between CSF and plasma Abeta; however, the correlation was not as strong as that present in young mice. In further exploring CSF and plasma Abeta levels in 9-month-old mice, levels of CSF Abeta were found to correlate highly with Abeta burden. Analysis of the CSF: plasma Abeta ratio revealed a selective two-fold increase in plaque versus non-plaque bearing mice, strongly suggesting a plaque-mediated sequestration of soluble Abeta in brain. Interestingly, in 9-month-old mice, a significant correlation between CNS and plasma Abeta was limited to mice lacking Abeta deposition. These findings suggest that there is a dynamic equilibrium between CNS and plasma Abeta, and that plaques create a new equilibrium because soluble CNS Abeta not only enters the plasma but also deposits onto amyloid plaques in the CNS.
机译:为了更好地了解体内的淀粉样β(Abeta)代谢,我们评估了APP(V717F)(PDAPP)转基因小鼠CSF和血浆中Abeta的浓度,该模型发展出年龄依赖性的阿尔茨海默氏病(AD)样病理。在3个月大的小鼠中,在大脑中出现Abeta沉积之前,CSF和血浆中的Abeta水平之间存在高度显着的相关性。在9个月大的小鼠中,部分但不是全部小鼠都已形成Abeta沉积,在这一年龄中,CSF与血浆Abeta之间也存在显着相关性。但是,这种相关性不如年轻小鼠强。在进一步探索9个月大小鼠的CSF和血浆Abeta水平时,发现CSF Abeta水平与Abeta负担高度相关。对脑脊液:血浆Abeta比率的分析显示,斑块轴承小鼠比无斑块的小鼠选择性增加了2倍,有力地暗示了斑块介导的大脑中可溶性Abe​​ta螯合。有趣的是,在9个月大的小鼠中,CNS与血浆Abeta之间的显着相关仅限于缺乏Abeta沉积的小鼠。这些发现表明,CNS和血浆Abeta之间存在动态平衡,并且噬菌斑形成了新的平衡,因为可溶性CNS Abeta不仅进入血浆,而且沉积在CNS中的淀粉样蛋白斑上。

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