Hannon Eilis, Shireby Gemma L, Brookes Keeley, Attems Johannes, Sims Rebecca, Cairns Nigel J, Love Seth, Thomas Alan J, Morgan Kevin, Francis Paul T, Mill Jonathan
College of Medicine and Health, University of Exeter, Exeter, Devon, EX2 5DW, UK.
School of Science & Technology, Nottingham Trent University, Nottingham, NG11 8NF, UK.
Brain Commun. 2020 Oct 12;2(2):fcaa167. doi: 10.1093/braincomms/fcaa167. eCollection 2020.
Alzheimer's disease is a highly heritable, common neurodegenerative disease characterized neuropathologically by the accumulation of β-amyloid plaques and tau-containing neurofibrillary tangles. In addition to the well-established risk associated with the locus, there has been considerable success in identifying additional genetic variants associated with Alzheimer's disease. Major challenges in understanding how genetic risk influences the development of Alzheimer's disease are clinical and neuropathological heterogeneity, and the high level of accompanying comorbidities. We report a multimodal analysis integrating longitudinal clinical and cognitive assessment with neuropathological data collected as part of the Brains for Dementia Research study to understand how genetic risk factors for Alzheimer's disease influence the development of neuropathology and clinical performance. Six hundred and ninety-three donors in the Brains for Dementia Research cohort with genetic data, semi-quantitative neuropathology measurements, cognitive assessments and established diagnostic criteria were included in this study. We tested the association of genotype and Alzheimer's disease polygenic risk score-a quantitative measure of genetic burden-with survival, four common neuropathological features in Alzheimer's disease brains (neurofibrillary tangles, β-amyloid plaques, Lewy bodies and transactive response DNA-binding protein 43 proteinopathy), clinical status (clinical dementia rating) and cognitive performance (Mini-Mental State Exam, Montreal Cognitive Assessment). The ε4 allele was significantly associated with younger age of death in the Brains for Dementia Research cohort. Our analyses of neuropathology highlighted two independent pathways from ε4, one where β-amyloid accumulation co-occurs with the development of tauopathy, and a second characterized by direct effects on tauopathy independent of β-amyloidosis. Although we also detected association between ε4 and dementia status and cognitive performance, these were all mediated by tauopathy, highlighting that they are a consequence of the neuropathological changes. Analyses of polygenic risk score identified associations with tauopathy and β-amyloidosis, which appeared to have both shared and unique contributions, suggesting that different genetic variants associated with Alzheimer's disease affect different features of neuropathology to different degrees. Taken together, our results provide insight into how genetic risk for Alzheimer's disease influences both the clinical and pathological features of dementia, increasing our understanding about the interplay between genotype and other genetic risk factors.
阿尔茨海默病是一种高度可遗传的常见神经退行性疾病,其神经病理学特征为β-淀粉样蛋白斑块和含tau蛋白的神经原纤维缠结的积累。除了与该基因座相关的已确定风险外,在识别与阿尔茨海默病相关的其他遗传变异方面也取得了相当大的成功。理解遗传风险如何影响阿尔茨海默病发展的主要挑战在于临床和神经病理学异质性以及伴随的高共病率。我们报告了一项多模态分析,将纵向临床和认知评估与作为痴呆症研究大脑计划一部分收集的神经病理学数据相结合,以了解阿尔茨海默病的遗传风险因素如何影响神经病理学发展和临床表现。痴呆症研究队列中的693名有遗传数据、半定量神经病理学测量、认知评估和既定诊断标准的捐赠者被纳入本研究。我们测试了该基因型和阿尔茨海默病多基因风险评分(一种遗传负担的定量测量)与生存率、阿尔茨海默病大脑中的四种常见神经病理学特征(神经原纤维缠结、β-淀粉样蛋白斑块、路易体和反应性DNA结合蛋白43蛋白病)、临床状态(临床痴呆评定量表)和认知表现(简易精神状态检查表、蒙特利尔认知评估)之间的关联。在痴呆症研究队列中,ε4等位基因与较年轻的死亡年龄显著相关。我们对神经病理学的分析突出了来自ε4的两条独立途径,一条是β-淀粉样蛋白积累与tau病变发展同时发生,另一条的特征是对tau病变有直接影响,独立于β-淀粉样变性。尽管我们还检测到ε4与痴呆状态和认知表现之间的关联,但这些都由tau病变介导,突出表明它们是神经病理学变化的结果。对多基因风险评分的分析确定了与tau病变和β-淀粉样变性的关联,这似乎既有共同贡献也有独特贡献,表明与阿尔茨海默病相关的不同遗传变异对神经病理学的不同特征有不同程度的影响。总之,我们的结果为阿尔茨海默病的遗传风险如何影响痴呆症的临床和病理特征提供了见解,增进了我们对该基因型与其他遗传风险因素之间相互作用的理解。
