阿尔茨海默病的神经元模型:对氧化应激介导的线粒体损伤机制的洞察。
A neuronal model of Alzheimer's disease: an insight into the mechanisms of oxidative stress-mediated mitochondrial injury.
作者信息
Sompol P, Ittarat W, Tangpong J, Chen Y, Doubinskaia I, Batinic-Haberle I, Abdul H M, Butterfield D A, St Clair D K
机构信息
Graduate Center for Toxicology, University of Kentucky, Lexington, KY 40536, USA.
出版信息
Neuroscience. 2008 Apr 22;153(1):120-30. doi: 10.1016/j.neuroscience.2008.01.044. Epub 2008 Feb 7.
Alzheimer's disease (AD) is associated with beta-amyloid accumulation, oxidative stress and mitochondrial dysfunction. However, the effects of genetic mutation of AD on oxidative status and mitochondrial manganese superoxide dismutase (MnSOD) production during neuronal development are unclear. To investigate the consequences of genetic mutation of AD on oxidative damages and production of MnSOD during neuronal development, we used primary neurons from new born wild-type (WT/WT) and amyloid precursor protein (APP) (NLh/NLh) and presenilin 1 (PS1) (P264L) knock-in mice (APP/PS1) which incorporated humanized mutations in the genome. Increasing levels of oxidative damages, including protein carbonyl, 4-hydroxynonenal (4-HNE) and 3-nitrotyrosine (3-NT), were accompanied by a reduction in mitochondrial membrane potential in both developing and mature APP/PS1 neurons compared with WT/WT neurons suggesting mitochondrial dysfunction under oxidative stress. Interestingly, developing APP/PS1 neurons were significantly more resistant to beta-amyloid 1-42 treatment, whereas mature APP/PS1 neurons were more vulnerable than WT/WT neurons of the same age. Consistent with the protective function of MnSOD, developing APP/PS1 neurons have increased MnSOD protein and activity, indicating an adaptive response to oxidative stress in developing neurons. In contrast, mature APP/PS1 neurons exhibited lower MnSOD levels compared with mature WT/WT neurons indicating that mature APP/PS1 neurons lost the adaptive response. Moreover, mature APP/PS1 neurons had more co-localization of MnSOD with nitrotyrosine indicating a greater inhibition of MnSOD by nitrotyrosine. Overexpression of MnSOD or addition of MnTE-2-PyP(5+) (SOD mimetic) protected against beta-amyloid-induced neuronal death and improved mitochondrial respiratory function. Together, the results demonstrate that compensatory induction of MnSOD in response to an early increase in oxidative stress protects developing neurons against beta-amyloid toxicity. However, continuing development of neurons under oxidative damage conditions may suppress the expression of MnSOD and enhance cell death in mature neurons.
阿尔茨海默病(AD)与β-淀粉样蛋白积累、氧化应激和线粒体功能障碍有关。然而,AD基因突变在神经元发育过程中对氧化状态和线粒体锰超氧化物歧化酶(MnSOD)产生的影响尚不清楚。为了研究AD基因突变在神经元发育过程中对氧化损伤和MnSOD产生的影响,我们使用了新生野生型(WT/WT)、淀粉样前体蛋白(APP)(NLh/NLh)和早老素1(PS1)(P264L)基因敲入小鼠(APP/PS1)的原代神经元,这些小鼠在基因组中引入了人源化突变。与WT/WT神经元相比,发育中和成熟的APP/PS1神经元中氧化损伤水平增加,包括蛋白质羰基、4-羟基壬烯醛(4-HNE)和3-硝基酪氨酸(3-NT),同时线粒体膜电位降低,提示氧化应激下的线粒体功能障碍。有趣的是,发育中的APP/PS1神经元对β-淀粉样蛋白1-42处理具有显著更高的抗性,而成熟的APP/PS1神经元比同年龄的WT/WT神经元更易受损。与MnSOD的保护功能一致,发育中的APP/PS1神经元中MnSOD蛋白和活性增加,表明发育中的神经元对氧化应激有适应性反应。相比之下,成熟的APP/PS1神经元与成熟的WT/WT神经元相比,MnSOD水平较低,表明成熟的APP/PS1神经元失去了适应性反应。此外,成熟的APP/PS1神经元中MnSOD与硝基酪氨酸的共定位更多,表明硝基酪氨酸对MnSOD的抑制作用更强。MnSOD的过表达或添加MnTE-2-PyP(5+)(SOD模拟物)可保护神经元免受β-淀粉样蛋白诱导的死亡,并改善线粒体呼吸功能。总之,结果表明,对氧化应激早期增加的反应中MnSOD的代偿性诱导可保护发育中的神经元免受β-淀粉样蛋白毒性。然而,在氧化损伤条件下神经元的持续发育可能会抑制MnSOD的表达并增强成熟神经元中的细胞死亡。
Zotero 插件