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The effect of ApoE ε 4 on clinical and structural MRI markers in prodromal Alzheimer’s disease

机译:Apoeε4对前西米氏症疾病临床和结构MRI标志物的影响

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Background: Apolipoprotein E (ApoE) ε 4 has been identified as the strongest genetic risk factor for Alzheimer’s disease (AD). However, the importance of ApoE ε 4 on clinical and biological heterogeneity of AD is still to be determined, particularly at the prodromal stage. Here, we evaluate the association of ApoE ε 4 with clinical cognition and neuroimaging regions in mild cognitive impairment (MCI) participants based on the AT (N) system, which is increasingly essential for developing a precise assessment of AD. Methods: We stratified 178 A+T+MCI participants (prodromal AD) into ApoE ε 4 (+) and ApoE ε 4 (?) according to ApoE genotype from the Alzheimer’s Disease Neuroimaging Initiative (ADNI). We determined Aβ-positivity (A+) by the standardized uptake values ratios (SUVR) means of florbetapir-PET-AV45 (the cutoff value of 1.1) and fibrillar tau-positivity (T+) by cerebrospinal fluid (CSF) phosphorylated-tau at threonine 181 position (p-Tau) (cut-off value of 23 pg/mL). We evaluated the effect of ApoE ε 4 status on cognitive conditions and brain atrophy from structural magnetic resonance imaging (MRI) scans. A multivariate analysis of variance was used to compare the differences of cognitive scores and brain atrophy from structural MRI regions of interest (ROIs) between both groups. Furthermore, we performed a linear regression model to assess the correlation between signature ROIs of structural MRI and cognitive scores in the prodromal AD participants. Results: ApoE ε 4 (+) prodromal AD participants had lower levels of CSF Aβ 1-42, higher levels of t-Tau, more memory and global cognitive impairment, and faster decline of global cognition, compared to ApoE ε 4 (?) prodromal AD. ApoE ε 4 (+) prodromal AD participants had a thinner cortical thickness of bilateral entorhinal, smaller subcortical volume of the left amygdala, bilateral hippocampus, and left ventral diencephalon (DC) relative to ApoE ε 4 (?) prodromal AD. Furthermore, the cortical thickness average of bilateral entorhinal was highly correlated with memory and global cognition. Conclusions: ApoE ε 4 status in prodromal AD participants has an important effect on clinical cognitive domains. After ascertaining the ApoE ε 4 status, specific MRI regions can be correlated to the cognitive domain and will be helpful for precise assessment in prodromal AD.
机译:背景:载脂蛋白E(apoe)ε4已被鉴定为阿尔茨海默病(AD)的最强遗传危险因素。然而,Apoeε4对AD的临床和生物异质性的重要性仍然是为了确定,特别是在前级。在这里,我们评估Apoeε4与轻度认知障碍(MCI)参与者的临床认知和神经影像区的关联,基于AT(n)系统,这对于开发AD的精确评估越来越重要。方法:根据来自阿尔茨海默病神经影像序(ADNI)的ApoE基因型,将178A + T + MCI参与者(前驱+ MCI参与者(前驱+ MCI参与者(前驱X)和ApoEε4(α)分析为Apoeε4(+)和apoeε4(α)。通过施塔宁(CSF)在苏氨酸的脑脊液(CSF)磷酸化 - Tau的标准化摄取值比(SUVR)的标准摄取值比(SUVR)方法(SUVR)方法(SUVR)的方法(SUVR)方法和Fibrillar Tau-Polyigy(T +)的方法确定了β-阳性(A +) 181个位置(p-tau)(截止值为23 pg / ml)。我们评估了Apoeε4状态对结构磁共振成像(MRI)扫描的认知条件和脑萎缩的影响。使用对两个组之间的结构MRI区域(ROI)的结构MRI区域的认知分数和脑萎缩的多元分析进行了比较。此外,我们执行了线性回归模型,以评估前驱广告参与者中结构MRI和认知评分的签名ROI之间的相关性。结果:Apoeε4(+)产品广告参与者的CSFAβ1-42水平较低,T-Tau的水平更高,更高的内存和全球认知障碍,以及全球认知的速度更快,与Apoeε4相比(?)相比产品广告。 Apoeε4(+)前驱的Pidromal广告参与者具有相对于Apoeε4(α)前α4(α)前Apoε4(α)前方的双侧Entorlinal,左侧肌肉,左侧腹部(DC)的双侧射孔较小的皮质厚度较薄的皮质厚度。此外,双侧梭形的皮质厚度平均与记忆和全球认知高度相关。结论:Prodromal广告参与者的Apoeε4状态对临床认知结构域具有重要影响。在确定Apoeε4状态后,特定的MRI区域可以与认知领域相关,并有助于在前驱广告中进行精确评估。

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