Neurobiology Program, Institute for Biological Sciences, National Research Council of Canada, Ottawa, Ontario.
Neurosci Bull. 2011 Aug;27(4):221-32. doi: 10.1007/s12264-011-1015-7.
OBJECTIVE The double transgenic mouse model (APPswe/PS1dE9) of Alzheimer's disease (AD) has been widely used in experimental studies. β-Amyloid (Aβ) peptide is excessively produced in AD mouse brain, which affects synaptic function and the development of central nervous system. However, little has been reported on characterization of this model. The present study aimed to characterize this mouse AD model and its wild-type counterparts by biochemical and functional approaches. METHODS Blood samples were collected from the transgenic and the wild-type mice, and radial arm water maze behavioral test was conducted at the ages of 6 and 12 months. The mice were sacrificed at 12-month age. One hemisphere of the brain was frozen-sectioned for immunohistochemistry and the other hemisphere was dissected into 7 regions. The levels of Aβ1-40, Aβ1-42 and 8-hydroxydeoxyguanosine (8-OHdG) in blood or/and brain samples were analyzed by ELISA. Secretase activities in brain regions were analyzed by in vitro assays. RESULTS The pre-mature death rate of transgenic mice was approximately 35% before 6-month age, and high levels of Aβ(1-40) and Aβ(1-42) were detected in these dead mice brains with a ratio of 1:10. The level of blood-borne Aβ at 6-month age was similar with that at 12-month age. Besides, Aβ(1-40) level in the blood was significantly higher than Aβ(1-42) level at the ages of 6 and 12 months (ratio 2.37:1). In contrast, the level of Aβ(1-42) in the brain (160.6 ng/mg protein) was higher than that of Aβ(1-40) (74 ng/mg protein) (ratio 2.17:1). In addition, the levels of Aβ(1-40) and Aβ(1-42) varied markedly among different brain regions. Aβ(1-42) level was significantly higher than Aβ(1-40) level in cerebellum, frontal and posterior cortex, and hippocampus. Secretase activity assays did not reveal major differences among different brain regions or between wild-type and transgenic mice, suggesting that the transgene PS1 did not lead to higher γ-secretase activity but was more efficient in producing Aβ(1-42) peptides. 8-OHdG, the biomarker of DNA oxidative damage, showed a trend of increase in the blood of transgenic mice, but with no significant difference, as compared with the wild-type mice. Behavioral tests showed that transgenic mice had significant memory deficits at 6-month age compared to wild-type controls, and the deficits were exacerbated at 12-month age with more errors. CONCLUSION These results suggest that this mouse model mimics the early-onset human AD and may represent full-blown disease at as early as 6-month age for experimental studies.
阿尔茨海默病(AD)的双转基因小鼠模型已广泛应用于实验研究。AD 小鼠脑内β-淀粉样肽(Aβ)过度产生,影响突触功能和中枢神经系统发育。然而,目前对该模型的特征描述较少。本研究旨在通过生化和功能方法对该 AD 模型及其野生型对照进行特征描述。
收集转基因和野生型小鼠的血液样本,并在 6 个月和 12 个月时进行放射臂水迷宫行为测试。12 月龄时处死小鼠。将一侧大脑冷冻切片用于免疫组织化学,另一侧大脑分为 7 个区。通过 ELISA 分析血液或/和脑组织中 Aβ1-40、Aβ1-42 和 8-羟基脱氧鸟苷(8-OHdG)的水平。通过体外测定分析脑区的分泌酶活性。
转基因小鼠在 6 月龄前的早逝率约为 35%,这些死亡小鼠的大脑中检测到高浓度的 Aβ(1-40)和 Aβ(1-42),比例为 1:10。6 月龄时的血源性 Aβ水平与 12 月龄时相似。此外,6 月龄和 12 月龄时,血液中 Aβ(1-40)水平明显高于 Aβ(1-42)水平(比值 2.37:1)。相比之下,大脑中 Aβ(1-42)(160.6 ng/mg 蛋白)的水平高于 Aβ(1-40)(74 ng/mg 蛋白)(比值 2.17:1)。此外,不同脑区之间 Aβ(1-40)和 Aβ(1-42)的水平差异明显。小脑、额皮质和后皮质以及海马区 Aβ(1-42)水平明显高于 Aβ(1-40)水平。分泌酶活性测定未显示不同脑区或野生型和转基因小鼠之间存在明显差异,表明转 PS1 基因不会导致 γ-分泌酶活性增加,但更有效地产生 Aβ(1-42)肽。作为 DNA 氧化损伤生物标志物的 8-OHdG 在转基因小鼠的血液中呈上升趋势,但与野生型小鼠相比无显著差异。行为测试显示,转基因小鼠在 6 月龄时与野生型对照组相比存在明显的记忆缺陷,12 月龄时缺陷加剧,错误更多。
这些结果表明,该小鼠模型模拟了早发性人类 AD,并且可能在 6 月龄时就代表了完全发病状态,可用于实验研究。
