首页> 外文期刊>Brain: A journal of neurology >Ventricular enlargement as a possible measure of Alzheimer's disease progression validated using the Alzheimer's disease neuroimaging initiative database.
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Ventricular enlargement as a possible measure of Alzheimer's disease progression validated using the Alzheimer's disease neuroimaging initiative database.

机译:使用阿尔茨海默氏病神经影像主动性数据库验证了心室扩大,可以作为阿尔茨海默氏病进展的一种可能度量。

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Ventricular enlargement may be an objective and sensitive measure of neuropathological change associated with mild cognitive impairment (MCI) and Alzheimer's disease (AD), suitable to assess disease progression for multi-centre studies. This study compared (i) ventricular enlargement after six months in subjects with MCI, AD and normal elderly controls (NEC) in a multi-centre study, (ii) volumetric and cognitive changes between Apolipoprotein E genotypes, (iii) ventricular enlargement in subjects who progressed from MCI to AD, and (iv) sample sizes for multi-centre MCI and AD studies based on measures of ventricular enlargement. Three dimensional T(1)-weighted MRI and cognitive measures were acquired from 504 subjects (NEC n = 152, MCI n = 247 and AD n = 105) participating in the multi-centre Alzheimer's Disease Neuroimaging Initiative. Cerebral ventricular volume was quantified at baseline and after six months using semi-automated software. For the primary analysis of ventricle and neurocognitive measures, between group differences were evaluated using an analysis of covariance, and repeated measures t-tests were used for within group comparisons. For secondary analyses, all groups were dichotomized for Apolipoprotein E genotype based on the presence of an epsilon 4 polymorphism. In addition, the MCI group was dichotomized into those individuals who progressed to a clinical diagnosis of AD, and those subjects that remained stable with MCI after six months. Group differences on neurocognitive and ventricle measures were evaluated by independent t-tests. General sample size calculations were computed for all groups derived from ventricle measurements and neurocognitive scores. The AD group had greater ventricular enlargement compared to both subjects with MCI (P = 0.0004) and NEC (P < 0.0001), and subjects with MCI had a greater rate of ventricular enlargement compared to NEC (P = 0.0001). MCI subjects that progressed to clinical AD after six months had greater ventricular enlargement than stable MCI subjects (P = 0.0270). Ventricular enlargement was different between Apolipoprotein E genotypes within the AD group (P = 0.010). The number of subjects required to demonstrate a 20% change in ventricular enlargement was substantially lower than that required to demonstrate a 20% change in cognitive scores. Ventricular enlargement represents a feasible short-term marker of disease progression in subjects with MCI and subjects with AD for multi-centre studies.
机译:心室扩大可能是与轻度认知障碍(MCI)和阿尔茨海默氏病(AD)相关的神经病理变化的客观和敏感指标,适用于评估多中心研究的疾病进展。这项研究在一项多中心研究中比较了(i)具有MCI,AD和正常老年人对照(NEC)的受试者六个月后的心室增大,(ii)载脂蛋白E基因型之间的体积和认知变化,(iii)受试者的心室增大从MCI到AD的研究者;以及(iv)基于心室扩大量度的多中心MCI和AD研究的样本量。从参与多中心阿尔茨海默氏病神经影像学计划的504名受试者(NEC n = 152,MCI n = 247和AD n = 105)中获得了三维T(1)加权MRI和认知测量。使用半自动化软件在基线和六个月后对脑室体积进行定量。对于心室和神经认知测量的初步分析,使用协方差分析评估组之间的差异,并使用重复测量的t检验进行组内比较。对于次要分析,基于存在ε4多态性,将所有组二分载脂蛋白E基因型。此外,将MCI组分为进行AD临床诊断的个体和六个月后仍保持MCI稳定的受试者。通过独立的t检验评估神经认知和心室测量的组差异。从心室测量值和神经认知评分得出所有组的常规样本量计算。与MCI(P = 0.0004)和NEC(P <0.0001)的受试者相比,AD组的心室增大更大,与NEC(P = 0.0001)相比,MCI的心室增大率更高。在六个月后发展为临床AD的MCI受试者的心室扩张比稳定的MCI受试者更大(P = 0.0270)。 AD组中载脂蛋白E基因型之间的心室增大是不同的(P = 0.010)。表现出心室扩大20%变化所需的受试者人数明显少于表现出认知分数变化20%所需的受试者数量。在多中心研究中,MCI患者和AD患者的心室扩大是疾病进展的可行的短期标记。

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