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Positron emission tomography in Alzheimer’s disease: early prediction and differentiation

机译:正电子发射断层扫描在阿尔茨海默氏病中的作用:早期预测和鉴别

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摘要

The development of biomarkers for the preclinical detection of neurodegenerative diseases such as Alzheimer’s disease (AD) is a vital step in developing prevention therapies. One consistent feature of AD is a reduction in the cerebral metabolic rate of glucose (CMRglc), a measure of neuronal function. In vivo brain 2-[18F]fluoro-2-deoxy-D-glucose-PET imaging demonstrates consistent and progressive CMRglc reductions in AD patients, the extent and topography of which correlate with symptom severity. There is increasing evidence that CMRglc reductions occur at the preclinical stages of AD and predict decline years in advance of clinical symptoms. This review will give an overview of FDG-PET results in individuals at risk for developing dementia, including: presymptomatic individuals carrying mutations responsible for early-onset familial AD; patients with mild cognitive impairment, often a prodrome to late-onset sporadic AD; nondemented carriers of the ApoE ε4 allele, a strong genetic risk factor for late-onset AD; cognitively normal subjects with a family history of AD; subjects with subjective memory complaints; and normal elderly who were followed longitudinally until they expressed the clinical symptoms and later received postmortem confirmation of AD. We will then review the most recent studies using FDG-PET as an early differential diagnostic tool in AD.
机译:在临床上检测神经退行性疾病(例如阿尔茨海默氏病(AD))的生物标记物是开发预防疗法的重要步骤。 AD的一个一致特征是降低了葡萄糖的脑代谢速率(CMRglc),这是神经元功能的一种度量。体内脑2- [18F]氟-2-脱氧-D-葡萄糖-PET成像显示AD患者CMRglc持续一致且进行性降低,其程度和地形与症状严重程度相关。越来越多的证据表明CMRglc的降低发生在AD的临床前阶段,并且可以预测临床症状提前数年下降。这篇综述将概述FDG-PET在有患痴呆症风险的个体中的结果,包括:症状突变的个体,其携带导致家族性早发性AD的突变;有轻度认知障碍的患者,通常是迟发性散发性AD的前兆; ApoEε4等位基因的非痴呆型携带者,这是晚期AD的强大遗传危险因素;具有AD家族史的认知正常受试者;有主观记忆障碍的受试者;纵向随访的正常老年人,直到他们表现出临床症状并随后接受AD验尸确认。然后,我们将回顾使用FDG-PET作为AD中早期鉴别诊断工具的最新研究。

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