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使用正电子发射断层扫描(PET)成像和匹兹堡化合物-B对人体淀粉样蛋白结合进行动力学建模。

Kinetic modeling of amyloid binding in humans using PET imaging and Pittsburgh Compound-B.

作者信息

Price Julie C, Klunk William E, Lopresti Brian J, Lu Xueling, Hoge Jessica A, Ziolko Scott K, Holt Daniel P, Meltzer Carolyn C, DeKosky Steven T, Mathis Chester A

机构信息

Department of Radiology, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania 15213, USA.

出版信息

J Cereb Blood Flow Metab. 2005 Nov;25(11):1528-47. doi: 10.1038/sj.jcbfm.9600146.

Abstract

A valid quantitative imaging method for the measurement of amyloid deposition in humans could improve Alzheimer's disease (AD) diagnosis and antiamyloid therapy assessment. Our group developed Pittsburgh Compound-B (PIB), an amyloid-binding radiotracer, for positron emission tomography (PET). The current study was aimed to further validate PIB PET through quantitative imaging (arterial input) and inclusion of subjects with mild cognitive impairment (MCI). Pittsburgh Compound-B studies were performed in five AD, five MCI, and five control subjects and five subjects were retested within 20 days. Magnetic resonance images were acquired for partial volume correction and region-of-interest definition (e.g., posterior cingulate: PCG; cerebellum: CER). Data were analyzed using compartmental and graphical approaches. Regional distribution volume (DV) values were normalized to the reference region (CER) to yield DV ratios (DVRs). Good agreement was observed between compartmental and Logan DVR values (e.g., PCG: r=0.89, slope=0.91); the Logan results were less variable. Nonspecific PIB retention was similar across subjects (n=15, Logan CER DV: 3.63+/-0.48). Greater retention was observed in AD cortical areas, relative to controls (P<0.05). The PIB retention in MCI subjects appeared either 'AD-like' or 'control-like'. The mean test/retest variation was approximately 6% in primary areas-of-interest. The Logan analysis was the method-of-choice for the PIB PET data as it proved stable, valid, and promising for future larger studies and voxel-based statistical analyses. This study also showed that it is feasible to perform quantitative PIB PET imaging studies that are needed to validate simpler methods for routine use across the AD disease spectrum.

摘要

一种用于测量人体淀粉样蛋白沉积的有效定量成像方法,可改善阿尔茨海默病(AD)的诊断及抗淀粉样蛋白治疗评估。我们团队开发了匹兹堡化合物B(PIB),一种用于正电子发射断层扫描(PET)的淀粉样蛋白结合放射性示踪剂。当前研究旨在通过定量成像(动脉输入)以及纳入轻度认知障碍(MCI)受试者来进一步验证PIB PET。对5名AD患者、5名MCI患者、5名对照受试者进行了PIB研究,其中5名受试者在20天内接受了重新检测。采集了磁共振图像用于部分容积校正和感兴趣区定义(例如,后扣带回:PCG;小脑:CER)。使用房室模型和图像法分析数据。将区域分布容积(DV)值标准化至参考区域(CER)以得出DV比率(DVR)。在房室模型和Logan DVR值之间观察到良好的一致性(例如,PCG:r = 0.89,斜率 = 0.91);Logan结果的变异性较小。非特异性PIB滞留情况在各受试者之间相似(n = 15,Logan CER DV:3.63±0.48)。相对于对照,在AD皮质区域观察到更高的滞留(P < 0.05)。MCI受试者的PIB滞留表现为“类似AD”或“类似对照”。在主要感兴趣区,平均重测变异约为6%。Logan分析是PIB PET数据的首选方法,因为它被证明稳定、有效,并且对未来更大规模的研究和基于体素的统计分析很有前景。这项研究还表明,进行定量PIB PET成像研究是可行的,此类研究对于验证在AD疾病谱中常规使用的更简单方法是必要的。

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