Morales-Corraliza Jose, Wong Harrison, Mazzella Matthew J, Che Shaoli, Lee Sang Han, Petkova Eva, Wagner Janice D, Hemby Scott E, Ginsberg Stephen D, Mathews Paul M
Nathan Kline Institute for Psychiatric Research, Orangeburg, New York 10962, Departments of Psychiatry.
Nathan Kline Institute for Psychiatric Research, Orangeburg, New York 10962.
J Neurosci. 2016 Apr 13;36(15):4248-58. doi: 10.1523/JNEUROSCI.4640-14.2016.
Epidemiological findings suggest that diabetic individuals are at a greater risk for developing Alzheimer's disease (AD). To examine the mechanisms by which diabetes mellitus (DM) may contribute to AD pathology in humans, we examined brain tissue from streptozotocin-treated type 1 diabetic adult male vervet monkeys receiving twice-daily exogenous insulin injections for 8-20 weeks. We found greater inhibitory phosphorylation of insulin receptor substrate 1 in each brain region examined of the diabetic monkeys when compared with controls, consistent with a pattern of brain insulin resistance that is similar to that reported in the human AD brain. Additionally, a widespread increase in phosphorylated tau was seen, including brain areas vulnerable in AD, as well as relatively spared structures, such as the cerebellum. An increase in active ERK1/2 was also detected, consistent with DM leading to changes in tau-kinase activity broadly within the brain. In contrast to these widespread changes, we found an increase in soluble amyloid-β (Aβ) levels that was restricted to the temporal lobe, with the greatest increase seen in the hippocampus. Consistent with this localized Aβ increase, a hippocampus-restricted decrease in the protein and mRNA for the Aβ-degrading enzyme neprilysin (NEP) was found, whereas various Aβ-clearing and -degrading proteins were unchanged. Thus, we document multiple biochemical changes in the insulin-controlled DM monkey brain that can link DM with the risk of developing AD, including dysregulation of the insulin-signaling pathway, changes in tau phosphorylation, and a decrease in NEP expression in the hippocampus that is coupled with a localized increase in Aβ.
Given that diabetes mellitus (DM) appears to increase the risk of developing Alzheimer's disease (AD), understanding the mechanisms by which DM promotes AD is important. We report that DM in a nonhuman primate brain leads to changes in the levels or posttranslational processing of proteins central to AD pathobiology, including tau, amyloid-β (Aβ), and the Aβ-degrading protease neprilysin. Additional evidence from this model suggests that alterations in brain insulin signaling occurred that are reminiscent of insulin signaling pathway changes seen in human AD. Thus, in an in vivo model highly relevant to humans, we show multiple alterations in the brain resulting from DM that are mechanistically linked to AD risk.
流行病学研究结果表明,糖尿病患者患阿尔茨海默病(AD)的风险更高。为了研究糖尿病(DM)可能导致人类AD病理的机制,我们检查了接受链脲佐菌素治疗的1型糖尿病成年雄性绿猴的脑组织,这些猴子每天接受两次外源性胰岛素注射,持续8 - 20周。我们发现,与对照组相比,糖尿病猴子每个检查脑区的胰岛素受体底物1的抑制性磷酸化程度更高,这与人类AD脑报道的脑胰岛素抵抗模式一致。此外,还观察到磷酸化tau广泛增加,包括AD中易损脑区以及相对未受影响的结构,如小脑。还检测到活性ERK1/2增加,这与DM导致大脑中tau激酶活性广泛变化一致。与这些广泛变化形成对比的是,我们发现可溶性淀粉样β蛋白(Aβ)水平增加仅限于颞叶,在海马体中增加最为明显。与这种局部Aβ增加一致,发现Aβ降解酶中性内肽酶(NEP)的蛋白质和mRNA在海马体中特异性降低,而各种Aβ清除和降解蛋白未发生变化。因此,我们记录了胰岛素控制的糖尿病猴子脑中的多种生化变化,这些变化可将DM与患AD的风险联系起来,包括胰岛素信号通路失调、tau磷酸化变化以及海马体中NEP表达降低并伴有局部Aβ增加。
鉴于糖尿病(DM)似乎会增加患阿尔茨海默病(AD)的风险,了解DM促进AD的机制很重要。我们报告,非人类灵长类动物脑中的DM会导致AD病理生物学核心蛋白的水平或翻译后加工发生变化,包括tau、淀粉样β蛋白(Aβ)和Aβ降解蛋白酶中性内肽酶。该模型的其他证据表明,大脑胰岛素信号发生了改变,这让人联想到在人类AD中看到的胰岛素信号通路变化。因此,在一个与人类高度相关的体内模型中,我们展示了DM导致的大脑中多种与AD风险有机制联系的改变。
