Early intervention anti-Aβ immunotherapy attenuates microglial activation without inducing exhaustion at residual plaques.

IF 17.5 1区医学 Q1 NEUROSCIENCES

Molecular Neurodegeneration Pub Date : 2025-08-20 DOI:10.1186/s13024-025-00878-1

Lis de Weerd, Selina Hummel, Stephan A Müller, Iñaki Paris, Thomas Sandmann, Marie Eichholtz, Robin Gröger, Amelie L Englert, Stephan Wagner, Connie Ha, Sonnet S Davis, Valerie Warkins, Dan Xia, Brigitte Nuscher, Anna Berghofer, Marvin Reich, Astrid F Feiten, Kai Schlepckow, Michael Willem, Stefan F Lichtenthaler, Joseph W Lewcock, Kathryn M Monroe, Matthias Brendel, Christian Haass

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引用次数: 0

Abstract

Anti-amyloid β-peptide (Aβ) immunotherapy was developed to reduce amyloid plaque pathology and slow cognitive decline during progression of Alzheimer's disease. Efficient amyloid clearance has been proven in clinical trials testing anti-Aβ antibodies, by their impact on cognitive endpoints correlating with the extent of amyloid removal. However, treatment is associated with adverse side effects, such as oedema and haemorrhages, which are potentially linked to the induced immune response. To improve the safety profile of these molecules, it is imperative to understand the consequences of anti-Aβ antibody treatment on immune cell function. Here, we investigated the effects of long-term chronic anti-Aβ treatment on amyloid plaque pathology and microglial response in the APP-SAA triple knock-in mouse model with an intervention paradigm early during amyloidogenesis. Long-term treatment with anti-Aβ results in a robust and dose-dependent lowering of amyloid plaque pathology, with a higher efficiency for reducing diffuse over dense-core plaque deposition. Analysis of the CSF proteome indicates a reduction of markers for neurodegeneration including Tau and α-Synuclein, as well as immune-cell-related proteins. Bulk RNA-seq revealed a dose-dependent attenuation of disease-associated microglial (DAM) and glycolytic gene expression, which is supported by a parallel decrease of glucose uptake and protein levels of Triggering Receptor Expressed on Myeloid cells 2 (Trem2) protein, a major immune receptor involved in DAM activation of microglia. In contrast, DAM activation around residual plaques remains high, regardless of treatment dose. In addition, microglia surrounding residual plaques display a dose-dependent increase in microglial clustering and a selective increase in antigen-presenting and immune signalling proteins. These findings demonstrate that chronic early intervention by an anti-amyloid immunotherapy leads to a dose-dependent decrease in plaque formation, which is associated with lower brain-wide microglial DAM activation and neurodegeneration. Microglia at residual plaques still display a combined DAM and antigen-presenting phenotype that suggests a continued treatment response.

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早期干预抗β免疫治疗减弱小胶质细胞的激活，而不诱导残余斑块的衰竭。

抗淀粉样蛋白β-肽（Aβ）免疫疗法被开发用于减少淀粉样斑块病理和减缓阿尔茨海默病进展过程中的认知能力下降。有效的淀粉样蛋白清除已在抗a β抗体的临床试验中得到证实，因为它们对认知终点的影响与淀粉样蛋白清除的程度相关。然而，治疗伴有不良副作用，如水肿和出血，这可能与诱导的免疫反应有关。为了提高这些分子的安全性，有必要了解抗a β抗体治疗对免疫细胞功能的影响。在这里，我们研究了长期慢性抗a β治疗对淀粉样斑块病理和小胶质细胞反应的影响，在APP-SAA三敲入小鼠模型中，在淀粉样变性早期进行干预。长期抗a β治疗可显著降低淀粉样斑块病理，且具有剂量依赖性，可有效减少弥漫性致密斑块沉积。脑脊液蛋白质组分析表明，神经变性标志物包括Tau和α-突触核蛋白以及免疫细胞相关蛋白减少。Bulk RNA-seq揭示了疾病相关小胶质细胞（DAM）和糖酵解基因表达的剂量依赖性衰减，这是由葡萄糖摄取和髓样细胞2触发受体表达（Trem2）蛋白水平的平行降低所支持的，Trem2蛋白是参与小胶质细胞DAM激活的主要免疫受体。相比之下，无论治疗剂量如何，残余斑块周围的DAM激活仍然很高。此外，残留斑块周围的小胶质细胞表现出剂量依赖性的小胶质聚集性增加和抗原呈递蛋白和免疫信号蛋白的选择性增加。这些发现表明，抗淀粉样蛋白免疫疗法的慢性早期干预导致斑块形成的剂量依赖性减少，这与全脑小胶质细胞DAM激活和神经退行性变有关。残留斑块处的小胶质细胞仍然显示出DAM和抗原呈递的联合表型，这表明治疗反应持续。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Molecular Neurodegeneration 医学-神经科学

CiteScore

23.00

自引率

4.60%

发文量

审稿时长

6-12 weeks

期刊介绍： Molecular Neurodegeneration, an open-access, peer-reviewed journal, comprehensively covers neurodegeneration research at the molecular and cellular levels. Neurodegenerative diseases, such as Alzheimer's, Parkinson's, Huntington's, and prion diseases, fall under its purview. These disorders, often linked to advanced aging and characterized by varying degrees of dementia, pose a significant public health concern with the growing aging population. Recent strides in understanding the molecular and cellular mechanisms of these neurodegenerative disorders offer valuable insights into their pathogenesis.