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正电子发射断层扫描数据分析中的简化:对结果指标的影响。

Simplifications in analyzing positron emission tomography data: effects on outcome measures.

作者信息

Logan Jean, Alexoff David, Kriplani Aarti

机构信息

Medical Department, Brookhaven National Laboratory, Upton, NY 11973, USA.

出版信息

Nucl Med Biol. 2007 Oct;34(7):743-56. doi: 10.1016/j.nucmedbio.2007.06.003. Epub 2007 Aug 27.

Abstract

Initial validation studies of new radiotracers generally involve kinetic models that require a measured arterial input function. This allows for the separation of tissue binding from delivery and blood flow effects. However, when using a tracer in a clinical setting, it is necessary to eliminate arterial blood sampling due to its invasiveness and the extra burden of counting and analyzing the blood samples for metabolites. In some cases, it may also be necessary to replace dynamic scanning with a shortened scanning period some time after tracer injection, as is done with FDG (F-18 fluorodeoxyglucose). These approximations represent loss of information. In this work, we considered several questions related to this: (1) Do differences in experimental conditions (drug treatments) or populations affect the input function, and what effect, if any, does this have on the final outcome measure? (2) How do errors in metabolite measurements enter into results? (3) What errors are incurred if the uptake ratio is used in place of the distribution volume ratio? (4) Is one- or two-point blood sampling any better for FDG data than the standardized uptake value? and (5) If blood sampling is necessary, what alternatives are there to arterial blood sampling? The first three questions were considered in terms of data from human dynamic positron emission tomography (PET) studies under conditions of baseline and drug pretreatment. Data from [11C]raclopride studies and those from the norepinephrine transporter tracer (S,S)-[11C]O-methyl reboxetine were used. Calculation of a metabolic rate for FDG using the operational equation requires a measured input function. We tested a procedure based on two blood samples to estimate the plasma integral and convolution that occur in the operational equation. There are some tracers for which blood sampling is necessary. Strategies for brain studies involve using the internal carotids in estimating the radioactivity after correcting for partial volume and spillover in order to eliminate arterial sampling. Some venous blood samples are still required for metabolite measurements. The ultimate solution to the problem of arterial sampling may be a wrist scanner, which acts as a small PET camera for imaging the arteries in the wrist. This is currently under development.

摘要

新放射性示踪剂的初始验证研究通常涉及需要测量动脉输入函数的动力学模型。这有助于将组织结合与输送及血流效应区分开来。然而,在临床环境中使用示踪剂时,由于动脉血采样具有侵入性,且对血样进行代谢物计数和分析会带来额外负担,因此有必要避免动脉血采样。在某些情况下,可能还需要在示踪剂注射后的某个时间用缩短的扫描期取代动态扫描,就像使用氟代脱氧葡萄糖(FDG,F - 18氟代脱氧葡萄糖)时那样。这些近似方法意味着信息的丢失。在这项工作中,我们考虑了与此相关的几个问题:(1)实验条件(药物治疗)或人群的差异是否会影响输入函数,以及这对最终结果测量有何影响(如有影响)?(2)代谢物测量中的误差如何影响结果?(3)如果用摄取比代替分布容积比会产生哪些误差?(4)对于FDG数据,单点或两点血样采集是否比标准化摄取值更好?以及(5)如果有必要进行血样采集,除了动脉血采样还有哪些替代方法?前三个问题是根据人类动态正电子发射断层扫描(PET)研究在基线和药物预处理条件下的数据来考虑的。使用了来自[11C]雷氯必利研究的数据以及去甲肾上腺素转运体示踪剂(S,S)-[11C]O-甲基瑞波西汀的数据。使用运算方程计算FDG的代谢率需要测量输入函数。我们测试了一种基于两个血样来估计运算方程中出现的血浆积分和卷积的方法。对于某些示踪剂,血样采集是必要的。脑部研究的策略包括在校正部分容积和溢出后,利用颈内动脉来估计放射性,以便消除动脉采样。为了进行代谢物测量,仍需要采集一些静脉血样。动脉采样问题的最终解决方案可能是手腕扫描仪,它可作为一台小型PET相机用于对手腕动脉进行成像。目前该设备正在研发中。

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