Taub Institute for Research on Alzheimer's Disease and the Aging Brain, College of Physicians and Surgeons, Columbia University, 630 West 168th Street, New York 10032, NY, USA.
Acta Neuropathol Commun. 2014 Aug 17;2:83. doi: 10.1186/s40478-014-0083-0.
Alzheimer's disease (AD) is the most common neurodegenerative disease and the leading cause of dementia. In addition to grey matter pathology, white matter changes are now recognized as an important pathological feature in the emergence of the disease. Despite growing recognition of the importance of white matter abnormalities in the pathogenesis of AD, the causes of white matter degeneration are still unknown. While multiple studies propose Wallerian-like degeneration as the source of white matter change, others suggest that primary white matter pathology may be due, at least in part, to other mechanisms, including local effects of toxic Aβ peptides. In the current study, we investigated levels of soluble amyloid-beta (Aβ) in white matter of AD patients (n=12) compared with controls (n=10). Fresh frozen white matter samples were obtained from anterior (Brodmann area 9) and posterior (Brodmann area 1, 2 and 3) areas of post-mortem AD and control brains. ELISA was used to examine levels of soluble Aβ -42 and Aβ -40. Total cortical neuritic plaque severity rating was derived from individual ratings in the following areas of cortex: mid-frontal, superior temporal, pre-central, inferior parietal, hippocampus (CA1), subiculum, entorhinal cortex, transentorhinal cortex, inferior temporal, amygdala and basal forebrain. Compared with controls, AD samples had higher white matter levels of both soluble Aβ -42 and Aβ -40. While no regional white matter differences were found in Aβ -40, Aβ -42 levels were higher in anterior regions than in posterior regions across both groups. After statistically controlling for total cortical neuritic plaque severity, differences in both soluble Aβ -42 and Aβ -40 between the groups remained, suggesting that white matter Aβ peptides accumulate independent of overall grey matter fibrillar amyloid pathology and are not simply a reflection of overall amyloid burden. These results shed light on one potential mechanism through which white matter degeneration may occur in AD. Given that white matter degeneration may be an early marker of disease, preceding grey matter atrophy, understanding the mechanisms and risk factors that may lead to white matter loss could help to identify those at high risk and to intervene earlier in the pathogenic process.
阿尔茨海默病(AD)是最常见的神经退行性疾病,也是痴呆症的主要病因。除了灰质病变外,现在人们已经认识到白质变化是疾病发生的一个重要病理特征。尽管人们越来越认识到 AD 发病机制中白质异常的重要性,但白质退化的原因仍不清楚。虽然多项研究提出沃勒氏变性是白质变化的来源,但也有研究认为原发性白质病变至少部分是由于其他机制引起的,包括有毒 Aβ 肽的局部影响。在目前的研究中,我们比较了 AD 患者(n=12)和对照组(n=10)的白质中可溶性淀粉样蛋白-β(Aβ)的水平。从 AD 和对照组死后大脑的前(Brodmann 区 9)和后(Brodmann 区 1、2 和 3)区域获得新鲜冷冻白质样本。ELISA 用于检测可溶性 Aβ-42 和 Aβ-40 的水平。皮质神经突斑块严重程度总评分源自皮质以下各区域的单独评分:中额、上颞、中央前、下顶叶、海马(CA1)、下托、内嗅皮质、穿通内嗅皮质、下颞叶、杏仁核和基底前脑。与对照组相比,AD 样本的白质中可溶性 Aβ-42 和 Aβ-40 水平均较高。虽然在 Aβ-40 中未发现区域白质差异,但在两组中,前区的 Aβ-42 水平均高于后区。在对皮质神经突斑块严重程度进行统计学控制后,两组间可溶性 Aβ-42 和 Aβ-40 的差异仍然存在,这表明白质 Aβ 肽的积累与整体灰质纤维状淀粉样蛋白病理学无关,而不仅仅是整体淀粉样蛋白负担的反映。这些结果揭示了 AD 中白质退化可能发生的一个潜在机制。鉴于白质退化可能是疾病的早期标志物,早于灰质萎缩,了解可能导致白质丢失的机制和风险因素,可能有助于识别高风险人群,并在发病过程中更早地进行干预。
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