载脂蛋白E克赖斯特彻奇变异体增强了疾病相关的小胶质细胞对斑块的反应,但抑制了对tau病理的反应。
APOE Christchurch enhances a disease-associated microglial response to plaque but suppresses response to tau pathology.
作者信息
Tran Kristine M, Kwang Nellie E, Butler Claire A, Gomez-Arboledas Angela, Kawauchi Shimako, Mar Cassandra, Chao Donna, Barahona Rocio A, Da Cunha Celia, Tsourmas Kate I, Shi Zechuan, Wang Shuling, Collins Sherilyn, Walker Amber, Shi Kai-Xuan, Alcantara Joshua A, Neumann Jonathan, Duong Duc M, Seyfried Nicholas T, Tenner Andrea J, LaFerla Frank M, Hohsfield Lindsay A, Swarup Vivek, MacGregor Grant R, Green Kim N
机构信息
Department of Neurobiology and Behavior, Charlie Dunlop School of Biological Sciences, University of California, Irvine, CA, 92697-4545, USA.
Institute for Memory Impairments and Neurological Disorders, University of California, Irvine, CA, 92697, USA.
出版信息
Mol Neurodegener. 2025 Jan 22;20(1):9. doi: 10.1186/s13024-024-00793-x.
BACKGROUND
Apolipoprotein E ε4 (APOE4) is the strongest genetic risk factor for late-onset Alzheimer's disease (LOAD). A recent case report identified a rare variant in APOE, APOE3-R136S (Christchurch), proposed to confer resistance to autosomal dominant Alzheimer's Disease (AD). However, it remains unclear whether and how this variant exerts its protective effects.
METHODS
We introduced the R136S variant into mouse Apoe (ApoeCh) and investigated its effect on the development of AD-related pathology using the 5xFAD model of amyloidosis and the PS19 model of tauopathy. We used immunohistochemical and biochemical analysis along with single-cell spatial omics and bulk proteomics to explore the impact of the ApoeCh variant on AD pathological development and the brain's response to plaques and tau.
RESULTS
In 5xFAD mice, ApoeCh enhances a Disease-Associated Microglia (DAM) phenotype in microglia surrounding plaques, and reduces plaque load, dystrophic neurites, and plasma neurofilament light chain. By contrast, in PS19 mice, ApoeCh suppresses the microglial and astrocytic responses to tau-laden neurons and does not reduce tau accumulation or phosphorylation, but partially rescues tau-induced synaptic and myelin loss. We compared how microglia responses differ between the two mouse models to elucidate the distinct DAM signatures induced by ApoeCh. We identified upregulation of antigen presentation-related genes in the DAM response in a PS19 compared to a 5xFAD background, suggesting a differential response to amyloid versus tau pathology that is modulated by the presence of ApoeCh. Bulk proteomics show upregulated mitochondrial protein abundance with ApoeCh in 5xFAD mice, but reductions in mitochondrial and translation associated proteins in PS19 mice.
CONCLUSIONS
These findings highlight the ability of the ApoeCh variant to modulate microglial responses based on the type of pathology, enhancing DAM reactivity in amyloid models and dampening neuroinflammation to promote protection in tau models. This suggests that the Christchurch variant's protective effects likely involve multiple mechanisms, including changes in receptor binding and microglial programming.
背景
载脂蛋白E ε4(APOE4)是晚发型阿尔茨海默病(LOAD)最强的遗传风险因素。最近的一份病例报告在APOE中鉴定出一种罕见变异体APOE3-R136S(克赖斯特彻奇变异体),该变异体被认为对常染色体显性阿尔茨海默病(AD)具有抗性。然而,尚不清楚这种变异体是否以及如何发挥其保护作用。
方法
我们将R136S变异体引入小鼠Apoe(ApoeCh)中,并使用淀粉样变性的5xFAD模型和tau蛋白病的PS19模型研究其对AD相关病理发展的影响。我们使用免疫组织化学和生化分析以及单细胞空间组学和整体蛋白质组学来探究ApoeCh变异体对AD病理发展以及大脑对斑块和tau蛋白反应的影响。
结果
在5xFAD小鼠中,ApoeCh增强了斑块周围小胶质细胞中与疾病相关的小胶质细胞(DAM)表型,并减少了斑块负荷、营养不良性神经突和血浆神经丝轻链。相比之下,在PS19小鼠中,ApoeCh抑制了小胶质细胞和星形胶质细胞对富含tau蛋白的神经元的反应,并且没有减少tau蛋白的积累或磷酸化,但部分挽救了tau蛋白诱导的突触和髓鞘丢失。我们比较了两种小鼠模型中小胶质细胞反应的差异,以阐明ApoeCh诱导的不同DAM特征。我们发现,与5xFAD背景相比,PS19背景下DAM反应中抗原呈递相关基因上调,这表明对淀粉样蛋白与tau蛋白病理的反应存在差异,且这种差异受ApoeCh的存在调节。整体蛋白质组学显示,在5xFAD小鼠中,ApoeCh使线粒体蛋白丰度上调,但在PS19小鼠中,线粒体和翻译相关蛋白减少。
结论
这些发现突出了ApoeCh变异体根据病理类型调节小胶质细胞反应的能力,在淀粉样蛋白模型中增强DAM反应性,并减轻神经炎症以在tau蛋白模型中促进保护作用。这表明克赖斯特彻奇变异体的保护作用可能涉及多种机制,包括受体结合和小胶质细胞编程的变化。
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