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A method to estimate dispersion in sampling catheters and to calculate dispersion-free blood time-activity curves.

机译:一种估计采样导管中的离散度并计算无离散度血液时间-活动曲线的方法。

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The authors developed a transmission-dispersion model to estimate dispersion in blood sampling systems and to calculate dispersion-free input functions needed for kinetic analysis. Transport of molecules through catheters was considered in two parts: a central part with convective transmission of molecules and a stagnant layer that molecules may enter and leave. The authors measured dispersion caused by automatic and manual blood sampling using three PET tracers that distribute differently in blood (C15O, H2(15)O, and 11C-methylglucose). For manual sampling, dispersion was negligible. For the automated sampling procedure, characteristic parameters were calibrated for each tracer, and subsequently used in calculating dispersion-free input functions following real bolus injections. This led to shapes of dispersion-free input functions C(i)(t) that had sharper peaks than the measured C(o)(t), and the authors quantified the effect of correcting for dispersion before kinetic modeling. The transmission-dispersion model quantitatively takes apart effects of transmission and dispersion, it has transparent noise properties associated with each component, and it does not require deconvolution to calculate dispersion-free input functions. Once characteristic parameters are estimated, input functions can be corrected before applying kinetic models. This allows bias-free estimation of kinetic parameters such as blood flow.
机译:作者开发了一种传输-分散模型,以估计血液采样系统中的分散并计算动力学分析所需的无分散输入函数。分子通过导管的运输分为两个部分:分子对流传输的中心部分和分子可能进入和离开的停滞层。这组作者使用三种在血液中分布不同的PET示踪剂(C150,H2(15)O和11C-甲基葡萄糖)测量了自动和手动采血引起的分散。对于手动采样,色散可以忽略不计。对于自动采样程序,将为每个示踪剂校准特征参数,然后将其用于计算真实推注后的无色散输入函数。这导致了无色散输入函数C(i)(t)的形状,其峰值比所测得的C(o)(t)尖锐,并且作者在动力学建模之前量化了校正色散的效果。传输色散模型定量地分离了传输和色散的影响,它具有与每个组件相关的透明噪声属性,并且不需要解卷积即可计算无色散输入函数。一旦估计了特征参数,就可以在应用动力学模型之前校正输入函数。这允许对动力学参数(例如血流)进行无偏估计。

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