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蓝斑核损毁增加了tg-2576转基因小鼠而非野生型小鼠的氧化应激。

Ablation of the locus coeruleus increases oxidative stress in tg-2576 transgenic but not wild-type mice.

作者信息

Hurko Orest, Boudonck Kurt, Gonzales Cathleen, Hughes Zoe A, Jacobsen J Steve, Reinhart Peter H, Crowther Daniel

机构信息

Biologics Consulting Group, Inc., 400 N. Washington Street, Suite 100, Alexandria, VA 22314, USA.

出版信息

Int J Alzheimers Dis. 2010 Oct 11;2010:864625. doi: 10.4061/2010/864625.

Abstract

Mice transgenic for production of excessive or mutant forms of beta-amyloid differ from patients with Alzheimer's disease in the degree of inflammation, oxidative damage, and alteration of intermediary metabolism, as well as the paucity or absence of neuronal atrophy and cognitive impairment. Previous observers have suggested that differences in inflammatory response reflect a discrepancy in the state of the locus coeruleus (LC), loss of which is an early change in Alzheimer's disease but which is preserved in the transgenic mice. In this paper, we extend these observations by examining the effects of the LC on markers of oxidative stress and intermediary metabolism. We compare four groups: wild-type or Tg2576 Aβ transgenic mice injected with DSP4 or vehicle. Of greatest interest were metabolites different between ablated and intact transgenics, but not between ablated and intact wild-type animals. The Tg2576_DSP4 mice were distinguished from the other three groups by oxidative stress and altered energy metabolism. These observations provide further support for the hypothesis that Tg2576 Aβ transgenic mice with this ablation may be a more congruent model of Alzheimer's disease than are transgenics with an intact LC.

摘要

产生过量或突变形式β-淀粉样蛋白的转基因小鼠在炎症程度、氧化损伤、中间代谢改变以及神经元萎缩和认知障碍的缺乏或不存在方面与阿尔茨海默病患者有所不同。先前的观察家认为,炎症反应的差异反映了蓝斑(LC)状态的差异,蓝斑的丧失是阿尔茨海默病的早期变化,但在转基因小鼠中得以保留。在本文中,我们通过研究蓝斑对氧化应激和中间代谢标志物的影响来扩展这些观察结果。我们比较了四组:注射了DSP4或赋形剂的野生型或Tg2576 Aβ转基因小鼠。最令人感兴趣的是在切除和完整的转基因小鼠之间不同,但在切除和完整的野生型动物之间没有差异的代谢物。Tg2576_DSP4小鼠在氧化应激和能量代谢改变方面与其他三组不同。这些观察结果进一步支持了这样的假设,即与具有完整蓝斑的转基因小鼠相比,这种切除后的Tg2576 Aβ转基因小鼠可能是更符合阿尔茨海默病的模型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ee62/2958341/1318f29ac63a/IJAD2010-864625.001.jpg

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