Fitz Nicholas F, Wolfe Cody M, Playso Brittany E, Biedrzycki Richard J, Lu Yi, Nam Kyong Nyon, Lefterov Iliya, Koldamova Radosveta
Department of Environmental & Occupational Health, University of Pittsburgh, 130 De Soto Street, Pittsburgh, PA, 15261, USA.
Mol Neurodegener. 2020 Jul 23;15(1):41. doi: 10.1186/s13024-020-00394-4.
Alzheimer's Disease (AD) is a neurodegenerative disorder influenced by aging and genetic risk factors. The inheritance of APOEε4 and variants of Triggering Receptor Expressed on Myeloid cells 2 (TREM2) are major genetic risk factors for AD. Recent studies showed that APOE binds to TREM2, thus raising the possibility of an APOE-TREM2 interaction that can modulate AD pathology.
The aim of this study was to investigate this interaction using complex AD model mice - a crossbreed of Trem2 and APP/PSEN1dE9 mice expressing human APOE3 or APOE4 isoforms (APP/E3 and APP/E4 respectively), and their WT littermates (E3 and E4), and evaluate cognition, steady-state amyloid load, plaque compaction, plaque growth rate, glial response, and brain transcriptome.
In both, APP/E3 and APP/E4 mice, Trem2 deletion reduced plaque compaction but did not significantly affect steady-state plaque load. Importantly, the lack of TREM2 increased plaque growth that negatively correlated to the diminished microglia barrier, an effect most pronounced at earlier stages of amyloid deposition. We also found that Trem2 deficiency significantly decreased plaque-associated APOE protein in APP/E4 but not in APP/E3 mice in agreement with RNA-seq data. Interestingly, we observed a significant decrease of Apoe mRNA expression in plaque-associated microglia of APP/E4/Trem2 vs APP/E4 mice. The absence of TREM2, worsened cognitive performance in APP transgenic mice but not their WT littermates. Gene expression analysis identified Trem2 signature - a cluster of highly connected immune response genes, commonly downregulated as a result of Trem2 deletion in all genotypes including APP and WT littermates. Furthermore, we identified sets of genes that were affected in TREM2- and APOE isoform-dependent manner. Among them were Clec7a and Csf1r upregulated in APP/E4 vs APP/E3 mice, a result further validated by in situ hybridization analysis. In contrast, Tyrobp and several genes involved in the C1Q complement cascade had a higher expression level in APP/E3 versus their APP/E4 counterparts.
Our data demonstrate that lack of Trem2 differentially impacts the phenotype and brain transcriptome of APP mice expressing human APOE isoforms. The changes probably reflect the different effect of APOE isoforms on amyloid deposition.
阿尔茨海默病(AD)是一种受衰老和遗传风险因素影响的神经退行性疾病。APOEε4的遗传以及髓样细胞2上表达的触发受体(TREM2)变体是AD的主要遗传风险因素。最近的研究表明,APOE与TREM2结合,因此增加了APOE - TREM2相互作用调节AD病理的可能性。
本研究的目的是使用复杂的AD模型小鼠来研究这种相互作用,该模型小鼠是Trem2和表达人类APOE3或APOE4异构体(分别为APP/E3和APP/E4)的APP/PSEN1dE9小鼠的杂交种,以及它们的野生型同窝小鼠(E3和E4),并评估认知、稳态淀粉样蛋白负荷、斑块压实、斑块生长速率、神经胶质反应和脑转录组。
在APP/E3和APP/E4小鼠中,Trem2缺失均降低了斑块压实,但未显著影响稳态斑块负荷。重要的是,TREM2的缺失增加了斑块生长,这与小胶质细胞屏障减弱呈负相关,这种效应在淀粉样蛋白沉积的早期阶段最为明显。我们还发现,与RNA测序数据一致,Trem2缺陷在APP/E4小鼠中显著降低了斑块相关的APOE蛋白,但在APP/E3小鼠中未降低。有趣的是,我们观察到APP/E4/Trem2小鼠与APP/E4小鼠相比,斑块相关小胶质细胞中Apoe mRNA表达显著降低。TREM2的缺失使APP转基因小鼠的认知能力恶化,但未影响其野生型同窝小鼠。基因表达分析确定了Trem2特征——一组高度连接的免疫反应基因,在包括APP和野生型同窝小鼠在内的所有基因型中,由于Trem2缺失通常下调。此外,我们确定了以TREM2和APOE异构体依赖性方式受影响的基因集。其中,Clec7a和Csf1r在APP/E4小鼠中相对于APP/E3小鼠上调,原位杂交分析进一步验证了这一结果。相反,Tyrobp和几个参与C1Q补体级联反应的基因在APP/E3小鼠中的表达水平高于其APP/E4对应物。
我们的数据表明,Trem2的缺失对表达人类APOE异构体的APP小鼠的表型和脑转录组有不同影响。这些变化可能反映了APOE异构体对淀粉样蛋白沉积的不同作用。
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