Jing Qian, Yiding Zhang, Rebecca A Betensky, Bradley T Hyman, Alberto Serrano-Pozo
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In this study, we tested the hypothesis that the <i>APOE</i> alleles differentially affect the rate of cognitive decline at the normal aging-early AD continuum and that this association is independent of their effects on classical ADNC and copathologies.</p><p><strong>Methods: </strong>We analyzed <i>APOE</i> associations with the cognitive trajectories (Clinical Dementia Rating scale Sum of Boxes [CDR-SOB] and Mini-Mental State Examination [MMSE]) of more than 1,000 individuals from a national clinicopathologic sample who had either no, mild (sparse neuritic plaques and the Braak neurofibrillary tangle [NFT] stage I/II), or intermediate (moderate neuritic plaques and the Braak NFT stage III/IV) ADNC levels at autopsy via 2 latent classes reverse-time longitudinal modeling.</p><p><strong>Results: </strong>Carrying the <i>APOE</i>ε4 allele was associated with a faster rate of cognitive decline by both CDR-SOB and MMSE relative to <i>APOE</i>ε3 homozygotes. This association remained statistically significant after adjusting for ADNC severity, comorbid pathologies, and the effects of ADNC on the slope of cognitive decline. Our modeling strategy identified 2 latent classes in which <i>APOE</i>ε4 carriers declined faster than <i>APOE</i>ε3 homozygotes, with latent class 1 members representing slow decliners (CDR-SOB: 76.7% of individuals, 0.195 vs 0.146 points/y in <i>APOE</i>ε4 vs <i>APOE</i>ε3/ε3; MMSE: 88.6% of individuals, -0.303 vs -0.153 points/y in <i>APOE</i>ε4 vs <i>APOE</i>ε3/ε3), whereas latent class 2 members were fast decliners (CDR-SOB: 23.3% of participants, 1.536 vs 1.487 points/y in <i>APOE</i>ε4 vs <i>APOE</i>ε3/ε3; MMSE: 11.4% of participants, -2.538 vs -2.387 points/y in <i>APOE</i>ε4 vs <i>APOE</i>ε3/ε3). Compared with slow decliners, fast decliners were more likely to carry the <i>APOE</i>ε4 allele, younger at initial visit and death, more impaired at initial and last visits, and more likely to have intermediate (vs none or mild) ADNC levels, as well as concurrent Lewy bodies and hippocampal sclerosis at autopsy.</p><p><strong>Discussion: </strong>In a large national sample selected to represent the normal aging-early AD continuum, the <i>APOE</i>ε4 allele is associated with a modest but statistically significant acceleration of the cognitive decline rate even after controlling for its effects on ADNC and comorbid pathologies.</p>","PeriodicalId":48613,"journal":{"name":"Neurology-Genetics","volume":"9 1","pages":"e200055"},"PeriodicalIF":3.0000,"publicationDate":"2023-01-20","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://ftp.ncbi.nlm.nih.gov/pub/pmc/oa_pdf/a7/2c/NXG-2022-200058.PMC9869750.pdf","citationCount":"0","resultStr":"{\"title\":\"Neuropathology-Independent Association Between <i>APOE</i> Genotype and Cognitive Decline Rate in the Normal Aging-Early Alzheimer Continuum.\",\"authors\":\"Jing Qian, Yiding Zhang, Rebecca A Betensky, Bradley T Hyman, Alberto Serrano-Pozo\",\"doi\":\"10.1212/NXG.0000000000200055\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><strong>Background and objectives: </strong>We previously found that the <i>APOE</i> genotype affects the rate of cognitive decline in mild-to-moderate Alzheimer disease (AD) dementia independently of its effects on AD neuropathologic changes (ADNC) and copathologies. In this study, we tested the hypothesis that the <i>APOE</i> alleles differentially affect the rate of cognitive decline at the normal aging-early AD continuum and that this association is independent of their effects on classical ADNC and copathologies.</p><p><strong>Methods: </strong>We analyzed <i>APOE</i> associations with the cognitive trajectories (Clinical Dementia Rating scale Sum of Boxes [CDR-SOB] and Mini-Mental State Examination [MMSE]) of more than 1,000 individuals from a national clinicopathologic sample who had either no, mild (sparse neuritic plaques and the Braak neurofibrillary tangle [NFT] stage I/II), or intermediate (moderate neuritic plaques and the Braak NFT stage III/IV) ADNC levels at autopsy via 2 latent classes reverse-time longitudinal modeling.</p><p><strong>Results: </strong>Carrying the <i>APOE</i>ε4 allele was associated with a faster rate of cognitive decline by both CDR-SOB and MMSE relative to <i>APOE</i>ε3 homozygotes. This association remained statistically significant after adjusting for ADNC severity, comorbid pathologies, and the effects of ADNC on the slope of cognitive decline. Our modeling strategy identified 2 latent classes in which <i>APOE</i>ε4 carriers declined faster than <i>APOE</i>ε3 homozygotes, with latent class 1 members representing slow decliners (CDR-SOB: 76.7% of individuals, 0.195 vs 0.146 points/y in <i>APOE</i>ε4 vs <i>APOE</i>ε3/ε3; MMSE: 88.6% of individuals, -0.303 vs -0.153 points/y in <i>APOE</i>ε4 vs <i>APOE</i>ε3/ε3), whereas latent class 2 members were fast decliners (CDR-SOB: 23.3% of participants, 1.536 vs 1.487 points/y in <i>APOE</i>ε4 vs <i>APOE</i>ε3/ε3; MMSE: 11.4% of participants, -2.538 vs -2.387 points/y in <i>APOE</i>ε4 vs <i>APOE</i>ε3/ε3). Compared with slow decliners, fast decliners were more likely to carry the <i>APOE</i>ε4 allele, younger at initial visit and death, more impaired at initial and last visits, and more likely to have intermediate (vs none or mild) ADNC levels, as well as concurrent Lewy bodies and hippocampal sclerosis at autopsy.</p><p><strong>Discussion: </strong>In a large national sample selected to represent the normal aging-early AD continuum, the <i>APOE</i>ε4 allele is associated with a modest but statistically significant acceleration of the cognitive decline rate even after controlling for its effects on ADNC and comorbid pathologies.</p>\",\"PeriodicalId\":48613,\"journal\":{\"name\":\"Neurology-Genetics\",\"volume\":\"9 1\",\"pages\":\"e200055\"},\"PeriodicalIF\":3.0000,\"publicationDate\":\"2023-01-20\",\"publicationTypes\":\"Journal Article\",\"fieldsOfStudy\":null,\"isOpenAccess\":false,\"openAccessPdf\":\"https://ftp.ncbi.nlm.nih.gov/pub/pmc/oa_pdf/a7/2c/NXG-2022-200058.PMC9869750.pdf\",\"citationCount\":\"0\",\"resultStr\":null,\"platform\":\"Semanticscholar\",\"paperid\":null,\"PeriodicalName\":\"Neurology-Genetics\",\"FirstCategoryId\":\"3\",\"ListUrlMain\":\"https://doi.org/10.1212/NXG.0000000000200055\",\"RegionNum\":3,\"RegionCategory\":\"医学\",\"ArticlePicture\":[],\"TitleCN\":null,\"AbstractTextCN\":null,\"PMCID\":null,\"EPubDate\":\"2023/2/1 0:00:00\",\"PubModel\":\"eCollection\",\"JCR\":\"Q2\",\"JCRName\":\"CLINICAL NEUROLOGY\",\"Score\":null,\"Total\":0}","platform":"Semanticscholar","paperid":null,"PeriodicalName":"Neurology-Genetics","FirstCategoryId":"3","ListUrlMain":"https://doi.org/10.1212/NXG.0000000000200055","RegionNum":3,"RegionCategory":"医学","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"2023/2/1 0:00:00","PubModel":"eCollection","JCR":"Q2","JCRName":"CLINICAL NEUROLOGY","Score":null,"Total":0}
引用次数: 0
摘要
背景和目的:我们之前发现,APOE 基因型会影响轻度至中度阿尔茨海默病(AD)痴呆患者的认知能力下降速度,而与其对 AD 神经病理学改变(ADNC)和共病理学的影响无关。在这项研究中,我们检验了 APOE 等位基因对正常衰老-早期 AD 连续过程中认知能力下降速度的不同影响,并且这种关联独立于其对经典 ADNC 和共病理学的影响这一假设:我们分析了 APOE 与认知轨迹(临床痴呆评定量表方框总和 [CDR-SOB] 和迷你精神状态检查 [MMSE])之间的关联,这些人来自全国临床病理样本,要么没有,要么有、通过 2 个潜类反向时间纵向建模,对尸检时无 ADNC、轻度 ADNC(稀疏神经纤维斑块和 Braak 神经纤维缠结[NFT]I/II 期)或中度 ADNC(中度神经纤维斑块和 Braak NFT III/IV 期)水平的 1,000 多人进行了研究。结果与APOEε3等位基因携带者相比,APOEε4等位基因携带者的CDR-SOB和MMSE认知能力下降速度更快。在调整了ADNC严重程度、合并病症以及ADNC对认知能力下降斜率的影响后,这种关联仍具有统计学意义。我们的建模策略确定了两个潜在类别,其中APOEε4携带者比APOEε3同卵双生者下降得更快,潜在类别1成员代表缓慢下降者(CDR-SOB:76.7%的个体,APOEε4 vs APOEε3/ε3为0.195 vs 0.146点/年;MMSE:88.6%的个体,-0.303 vs -0.153 points/y in APOEε4 vs APOEε3/ε3),而潜伏 2 类成员则是快速下降者(CDR-SOB:23.3% 的参与者,1.536 vs 1.487 points/y in APOEε4 vs APOEε3/ε3;MMSE:11.4% 的参与者,-2.538 vs -2.387 points/y in APOEε4 vs APOEε3/ε3)。与缓慢衰退者相比,快速衰退者更有可能携带APOEε4等位基因,在初次就诊和死亡时更年轻,在初次就诊和最后一次就诊时受损程度更严重,更有可能出现中度(vs无或轻度)ADNC水平,以及在尸检时同时出现路易体和海马硬化:讨论:在选取的代表正常衰老-早期AD连续体的大型全国样本中,APOEε4等位基因与认知能力下降率的适度加速有关,但在统计学上具有显著意义,即使在控制了其对ADNC和合并病症的影响之后也是如此。
Neuropathology-Independent Association Between APOE Genotype and Cognitive Decline Rate in the Normal Aging-Early Alzheimer Continuum.
Background and objectives: We previously found that the APOE genotype affects the rate of cognitive decline in mild-to-moderate Alzheimer disease (AD) dementia independently of its effects on AD neuropathologic changes (ADNC) and copathologies. In this study, we tested the hypothesis that the APOE alleles differentially affect the rate of cognitive decline at the normal aging-early AD continuum and that this association is independent of their effects on classical ADNC and copathologies.
Methods: We analyzed APOE associations with the cognitive trajectories (Clinical Dementia Rating scale Sum of Boxes [CDR-SOB] and Mini-Mental State Examination [MMSE]) of more than 1,000 individuals from a national clinicopathologic sample who had either no, mild (sparse neuritic plaques and the Braak neurofibrillary tangle [NFT] stage I/II), or intermediate (moderate neuritic plaques and the Braak NFT stage III/IV) ADNC levels at autopsy via 2 latent classes reverse-time longitudinal modeling.
Results: Carrying the APOEε4 allele was associated with a faster rate of cognitive decline by both CDR-SOB and MMSE relative to APOEε3 homozygotes. This association remained statistically significant after adjusting for ADNC severity, comorbid pathologies, and the effects of ADNC on the slope of cognitive decline. Our modeling strategy identified 2 latent classes in which APOEε4 carriers declined faster than APOEε3 homozygotes, with latent class 1 members representing slow decliners (CDR-SOB: 76.7% of individuals, 0.195 vs 0.146 points/y in APOEε4 vs APOEε3/ε3; MMSE: 88.6% of individuals, -0.303 vs -0.153 points/y in APOEε4 vs APOEε3/ε3), whereas latent class 2 members were fast decliners (CDR-SOB: 23.3% of participants, 1.536 vs 1.487 points/y in APOEε4 vs APOEε3/ε3; MMSE: 11.4% of participants, -2.538 vs -2.387 points/y in APOEε4 vs APOEε3/ε3). Compared with slow decliners, fast decliners were more likely to carry the APOEε4 allele, younger at initial visit and death, more impaired at initial and last visits, and more likely to have intermediate (vs none or mild) ADNC levels, as well as concurrent Lewy bodies and hippocampal sclerosis at autopsy.
Discussion: In a large national sample selected to represent the normal aging-early AD continuum, the APOEε4 allele is associated with a modest but statistically significant acceleration of the cognitive decline rate even after controlling for its effects on ADNC and comorbid pathologies.
期刊介绍:
Neurology: Genetics is an online open access journal publishing peer-reviewed reports in the field of neurogenetics. Original articles in all areas of neurogenetics will be published including rare and common genetic variation, genotype-phenotype correlations, outlier phenotypes as a result of mutations in known disease-genes, and genetic variations with a putative link to diseases. This will include studies reporting on genetic disease risk and pharmacogenomics. In addition, Neurology: Genetics will publish results of gene-based clinical trials (viral, ASO, etc.). Genetically engineered model systems are not a primary focus of Neurology: Genetics, but studies using model systems for treatment trials are welcome, including well-powered studies reporting negative results.
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