1 Department of Pharmacology and Therapeutics, McGill University, 3655 Sir-William-Osler Promenade, Montreal, H3G1Y6, Canada.
Brain. 2014 Mar;137(Pt 3):860-72. doi: 10.1093/brain/awt372. Epub 2014 Feb 11.
Basal forebrain cholinergic neurons play a key role in cognition. This neuronal system is highly dependent on NGF for its synaptic integrity and the phenotypic maintenance of its cell bodies. Basal forebrain cholinergic neurons progressively degenerate in Alzheimer's disease and Down's syndrome, and their atrophy contributes to the manifestation of dementia. Paradoxically, in Alzheimer's disease brains, the synthesis of NGF is not affected and there is abundance of the NGF precursor, proNGF. We have shown that this phenomenon is the result of a deficit in NGF's extracellular metabolism that compromises proNGF maturation and exacerbates its subsequent degradation. We hypothesized that a similar imbalance should be present in Down's syndrome. Using a combination of quantitative reverse transcription-polymerase chain reaction, enzyme-linked immunosorbent assay, western blotting and zymography, we investigated signs of NGF metabolic dysfunction in post-mortem brains from the temporal (n = 14), frontal (n = 34) and parietal (n = 20) cortex obtained from subjects with Down's syndrome and age-matched controls (age range 31-68 years). We further examined primary cultures of human foetal Down's syndrome cortex (17-21 gestational age weeks) and brains from Ts65Dn mice (12-22 months), a widely used animal model of Down's syndrome. We report a significant increase in proNGF levels in human and mouse Down's syndrome brains, with a concomitant reduction in the levels of plasminogen and tissue plasminogen activator messenger RNA as well as an increment in neuroserpin expression; enzymes that partake in proNGF maturation. Human Down's syndrome brains also exhibited elevated zymogenic activity of MMP9, the major NGF-degrading protease. Our results indicate a failure in NGF precursor maturation in Down's syndrome brains and a likely enhanced proteolytic degradation of NGF, changes which can compromise the trophic support of basal forebrain cholinergic neurons. The alterations in proNGF and MMP9 were also present in cultures of Down's syndrome foetal cortex; suggesting that this trophic compromise may be amenable to rescue, before frank dementia onset. Our study thus provides a novel paradigm for cholinergic neuroprotection in Alzheimer's disease and Down's syndrome.
基底前脑胆碱能神经元在认知中起着关键作用。这个神经元系统高度依赖于神经生长因子(NGF)来维持其突触完整性和细胞体的表型维持。基底前脑胆碱能神经元在阿尔茨海默病和唐氏综合征中逐渐退化,其萎缩导致痴呆的表现。矛盾的是,在阿尔茨海默病大脑中,NGF 的合成不受影响,并且存在丰富的 NGF 前体,即 proNGF。我们已经表明,这种现象是 NGF 细胞外代谢缺陷的结果,这种缺陷会损害 proNGF 的成熟,并加剧其随后的降解。我们假设在唐氏综合征中也应该存在类似的失衡。我们使用定量逆转录聚合酶链反应、酶联免疫吸附测定、Western blot 和酶谱分析的组合,研究了从唐氏综合征患者(年龄范围为 31-68 岁)和年龄匹配的对照组(n = 14)颞叶(n = 34)、额叶(n = 34)和顶叶(n = 20)皮层获得的死后大脑中 NGF 代谢功能障碍的迹象。我们进一步检查了人类胎儿唐氏综合征皮层(17-21 孕周)和 Ts65Dn 小鼠(12-22 个月)的原代培养物,Ts65Dn 小鼠是唐氏综合征的广泛使用的动物模型。我们报告说,人类和小鼠唐氏综合征大脑中的 proNGF 水平显著增加,同时纤溶酶原和组织纤溶酶原激活物 mRNA 水平降低,神经丝氨酸蛋白酶表达增加;这些酶参与 proNGF 的成熟。人类唐氏综合征大脑还表现出基质金属蛋白酶 9(MMP9)的酶原活性升高,MMP9 是主要的 NGF 降解蛋白酶。我们的结果表明,唐氏综合征大脑中 NGF 前体成熟失败,并且可能增强了 NGF 的蛋白水解降解,这可能会损害基底前脑胆碱能神经元的营养支持。唐氏综合征胎儿皮层培养物中也存在 proNGF 和 MMP9 的改变;这表明在出现明显痴呆之前,这种营养缺陷可能可以得到挽救。因此,我们的研究为阿尔茨海默病和唐氏综合征中的胆碱能神经保护提供了一个新的范例。
