Cheng Gerald Wai-Yeung, Ma Iris Wai-Ting, Huang Jianpan, Yeung Sunny Hoi-Sang, Ho Paolo, Chen Zilin, Mak Henry Ka Fung, Herrup Karl, Chan Kannie Wai Yan, Tse Kai-Hei
bioRxiv. 2023 Jul 25:2023.07.24.547147. doi: 10.1101/2023.07.24.547147.
Myelin degradation is a normal feature of brain aging that accelerates in Alzheimer's disease (AD). To date, however, the underlying biological basis of this correlation remains elusive. The amyloid cascade hypothesis predicts that demyelination is caused by increased levels of the β-amyloid (Aβ) peptide. Here we report on work supporting the alternative hypothesis that early demyelination is upstream of amyloid. We challenged two different mouse models of AD (R1.40 and APP/PS1) using cuprizone-induced demyelination and tracked the responses with both neuroimaging and neuropathology. In oppose to amyloid cascade hypothesis, R1.40 mice, carrying only a single human mutant APP (Swedish; APP ) transgene, showed a more abnormal changes of magnetization transfer ratio and diffusivity than in APP/PS1 mice, which carry both APP and a second PSEN1 transgene (delta exon 9; PSEN1 ). Although cuprizone targets oligodendrocytes (OL), magnetic resonance spectroscopy and targeted RNA-seq data in R1.40 mice suggested a possible metabolic alternation in axons. In support of alternative hypotheses, cuprizone induced significant intraneuronal amyloid deposition in young APP/PS1, but not in R1.40 mice, and it suggested the presence of PSEN deficiencies, may accelerate Aβ deposition upon demyelination. In APP/PS1, mature OL is highly vulnerable to cuprizone with significant DNA double strand breaks (53BP1 ) formation. Despite these major changes in myelin, OLs, and Aβ immunoreactivity, no cognitive impairment or hippocampal pathology was detected in APP/PS1 mice after cuprizone treatment. Together, our data supports the hypothesis that myelin loss can be the cause, but not the consequence, of AD pathology.
The causal relationship between early myelin loss and the progression of Alzheimer's disease remains unclear. Using two different AD mouse models, R1.40 and APP/PS1, our study supports the hypothesis that myelin abnormalities are upstream of amyloid production and deposition. We find that acute demyelination initiates intraneuronal amyloid deposition in the frontal cortex. Further, the loss of oligodendrocytes, coupled with the accelerated intraneuronal amyloid deposition, interferes with myelin tract diffusivity at a stage before any hippocampus pathology or cognitive impairments occur. We propose that myelin loss could be the cause, not the consequence, of amyloid pathology during the early stages of Alzheimer's disease.
髓鞘降解是大脑衰老的正常特征,在阿尔茨海默病(AD)中会加速。然而,迄今为止,这种相关性的潜在生物学基础仍不清楚。淀粉样蛋白级联假说预测脱髓鞘是由β-淀粉样蛋白(Aβ)肽水平升高引起的。在此,我们报告支持另一种假说的研究工作,即早期脱髓鞘在淀粉样蛋白上游。我们使用铜螯合剂诱导的脱髓鞘对两种不同的AD小鼠模型(R1.40和APP/PS1)进行挑战,并通过神经影像学和神经病理学追踪其反应。与淀粉样蛋白级联假说相反,仅携带单个人类突变APP(瑞典型;APP )转基因的R1.40小鼠,比同时携带APP 和第二个PSEN1转基因(第9外显子缺失;PSEN1 )的APP/PS1小鼠表现出更异常的磁化传递率和扩散率变化。尽管铜螯合剂靶向少突胶质细胞(OL),但R1.40小鼠的磁共振波谱和靶向RNA测序数据表明轴突可能存在代谢改变。为支持另一种假说,铜螯合剂在年轻的APP/PS1小鼠中诱导了显著的神经元内淀粉样蛋白沉积,但在R1.40小鼠中未诱导,这表明PSEN缺陷的存在可能会加速脱髓鞘后的Aβ沉积。在APP/PS1小鼠中,成熟的OL对铜螯合剂高度敏感,会形成显著的DNA双链断裂(53BP1 )。尽管髓鞘、OL和Aβ免疫反应性发生了这些重大变化,但在铜螯合剂处理后的APP/PS1小鼠中未检测到认知障碍或海马病理改变。总之,我们的数据支持髓鞘丢失可能是AD病理的原因而非结果这一假说。
早期髓鞘丢失与阿尔茨海默病进展之间的因果关系仍不清楚。我们使用两种不同的AD小鼠模型R1.40和APP/PS1进行研究,支持髓鞘异常在淀粉样蛋白产生和沉积上游的假说。我们发现急性脱髓鞘会引发额叶皮质的神经元内淀粉样蛋白沉积。此外,少突胶质细胞的丢失,加上神经元内淀粉样蛋白沉积加速,在任何海马病理或认知障碍出现之前的阶段就会干扰髓鞘束的扩散率。我们提出,在阿尔茨海默病早期,髓鞘丢失可能是淀粉样蛋白病理的原因而非结果。
