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Regionally specific changes in the hippocampal circuitry accompany progression of cerebrospinal fluid biomarkers in preclinical Alzheimer's disease

机译:海马电路的区域特异性变化伴随脑脊液生物标志物在临床前阿尔茨海默病中的进展

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Neuropathological and in vivo brain imaging studies agree that the cornu ammonis 1 and subiculum subfields of the hippocampus are most vulnerable to atrophy in the prodromal phases of Alzheimer's disease (AD). However, there has been limited investigation of the structural integrity of the components of the hippocampal circuit, including subfields and extra-hippocampal white matter structure, in relation to the progression of well-accepted cerebrospinal fluid (CSF) biomarkers of AD, amyloid-beta 1-42 (A beta) and total-tau (tau). We investigated these relationships in 88 aging asymptomatic individuals with a parental or multiple-sibling familial history of AD. Apolipoprotein (APOE) epsilon 4 risk allele carriers were identified, and all participants underwent cognitive testing, structural magnetic resonance imaging, and lumbar puncture for CSF assays of tau, phosphorylated-tau (p-tau) and A beta. Individuals with a reduction in CSF A beta levels (an indicator of amyloid accretion into neuritic plaques) as well as evident tau pathology (believed to be linked to neurodegeneration) exhibited lower subiculum volume, lower fornix microstructural integrity, and a trend towards lower cognitive score than individuals who showed only reduction in CSF A beta. In contrast, persons with normal levels of tau showed an increase in structural MR markers in relation to declining levels of CSF A beta. These results suggest that hippocampal subfield volume and extra-hippocampal white matter microstructure demonstrate a complex pattern where an initial volume increase is followed by decline among asymptomatic individuals who, in some instances, may be a decade or more away from onset of cognitive or functional impairment.
机译:神经病理学和体内脑成像研究同意,海马的玉米氨氨1和次粒子子场最容易受到阿尔茨海默病(AD)的前阶段的萎缩。然而,关于海马电路组分的结构完整性有限调查,包括子场和超海豚白质结构,相对于广告良好的脑脊液(CSF)生物标志物的进展,淀粉样蛋白β 1-42(β)和Total-Tau(Tau)。我们调查了88名衰老无症状的人际关系,具有父母或多个兄弟的广告家族史。鉴定载脂蛋白(APOE)ε4风险等位基因载体,并且所有参与者接受了对TAU,磷酸化 - TAU(P-TAU)和β的CSF测定的认知测试,结构磁共振成像和腰椎穿刺。具有降低CSF的β水平(淀粉样蛋白斑块的指标)以及明显的Tau病理学(认为与神经变性相关)表现出较低的粒度,较低的腹膜微观结构完整性,以及降低认知得分的趋势而不是只表现出CSF A测试版的个人。相比之下,具有正常水平的Tau水平的人表现出与CSFAβ水平的下降相关的结构MR标记的增加。这些结果表明,海马子场体积和超海豚白质微结构表明了一种复杂的模式,其中初始体积增加之后,在某些情况下,在某些情况下可能是十年或更长时间的认知或功能障碍。 。

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