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Validation of Parametric Methods for [C-11]UCB-J PET Imaging Using Subcortical White Matter as Reference Tissue

机译:使用皮下白质作为参考组织的[C-11] UCB-J PET成像的参数方法验证

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Purpose The aim of this study was to evaluate different non-invasive methods for generating (R)-1-((3-([C-11]methyl)pyridin-4-yl)methyl)-4-(3,4,5-trifluorophenyl)pyrrolidin-2-one) ([C-11]UCB-J) parametric maps using white matter (centrum semi-ovale-SO) as reference tissue. Procedures Ten healthy volunteers (8 M/2F; age 27.6 +/- 10.0 years) underwent a 90-min dynamic [C-11]UCB-J positron emission tomography (PET) scan with full arterial blood sampling and metabolite analysis before and after administration of a novel chemical entity with high affinity for presynaptic synaptic vesicle glycoprotein 2A (SV2A). A simplified reference tissue model (SRTM2), multilinear reference tissue model (MRTM2), and reference Logan graphical analysis (rLGA) were used to generate binding potential maps using SO as reference tissue (BPSO). Shorter dynamic acquisitions down to 50 min were also considered. In addition, standard uptake value ratios (SUVR) relative to SO were evaluated for three post-injection intervals (SUVRSO,40-70min, SUVRSO,50-80min, and SUVRSO,60-90min respectively). Regional parametric BPSO + 1 and SUVRSO were compared with regional distribution volume ratios of a 1-tissue compartment model (1TCM DVRSO) using Spearman correlation and Bland-Altman analysis. Results For all methods, highly significant correlations were found between regional, parametric BPSO + 1 (r = [0.63;0.96]) or SUVRSO (r = [0.90;0.91]) estimates and regional 1TCM DVRSO. For a 90-min dynamic scan, parametric SRTM2 and MRTM2 values presented similar small bias and variability (- 3.0 +/- 2.9 % for baseline SRTM2) and outperformed rLGA (- 10.0 +/- 5.3 % for baseline rLGA). Reducing the dynamic acquisition to 60 min had limited impact on the bias and variability of parametric SRTM2 BPSO estimates (- 1.0 +/- 9.9 % for baseline SRTM2) while a higher variability (- 1.83 +/- 10.8 %) for baseline MRTM2 was observed for shorter acquisition times. Both SUVRSO,60-90min and SUVRSO,50-80min showed similar small bias and variability (- 2.8 +/- 4.6 % bias for baseline SUVRSO,60-90min). Conclusion SRTM2 is the preferred method for a voxelwise analysis of dynamic [C-11]UCB-J PET using SO as reference tissue, while reducing the dynamic acquisition to 60 min has limited impact on [C-11]UCB-J BPSO parametric maps. For a static PET protocol, both SUVRSO,60-90min and SUVRSO,50-80min images are an excellent proxy for [C-11]UCB-J BPSO parametric maps.
机译:目的本研究的目的是评估用于产生(R)-1 - ((3 - ([C-11]甲基)吡啶-4-基)甲基)-4-(3,4, 5-三氟苯基)吡咯烷蛋白-2-一)([C-11] UCB-J)使用白体(半卵子半卵形-SO)作为参考组织的参数图。程序十个健康志愿者(8米/ 2F;年龄27.6 +/- 10.0年)经历了90分钟的动态[C-11] UCB-J正电子发射断层扫描(PET)扫描,前后全动脉血液采样和代谢物分析施用具有高亲和力的新型化学实体对突触前突触囊泡糖蛋白2A(SV2A)。简化的参考组织模型(SRTM2),多线性参考组织模型(MRTM2)和参考逻辑图形分析(RLGA)用于使用诸如参考组织(BPSO)产生绑定潜在地图。还考虑了下降到50分钟的较短动态采集。此外,相对于所以的标准摄取值比(SUVR)分别评估了三个后注射间隔(SUVRSO,40-70min,SUVRSO,50-80min和SUVRSO,60-90min)。使用Spearman相关性和Bland-Altman分析将区域参数BPSO + 1和SUVRSO与1组织隔室模型(1TCM DVRSO)的区域分布体积比进行比较。所有方法的结果,在区域,参数BPSO + 1之间发现了非常显着的相关性(R = [0.63; 0.96])或SUVRSO(r = [0.90; 0.91])估算和区域1TCM DVRSO。对于90分钟的动态扫描,参数SRTM2和MRTM2值呈现出类似的小偏差和变异性(基线SRTM2的可变性(3.0 +/- 2.9%),并且表现优于基线RLGA的RLGA( - 10.0 +/- 5.3%)。将动态采集降低到60分钟对参数SRTM2 BPSO估计的偏差和变异性有限(基线SRTM2的1.0 +/- 9.9%),而基线MRTM2的较高变化( - 1.83 +/- 10.8%)被观察到用于更短的收购时间。 Suvrso,60-90min和Suvrso都显示出类似的小偏差和变异性( - 2.8 +/- 4.6%,为基线Suvrso,60-90min)。结论SRTM2是动态[C-11] UCB-J PET的VoxelWise分析的优选方法,用于使用借鉴组织,同时将动态采集降低到60分钟对[C-11] UCB-J BPSO参数图影响有限。对于静态PET协议,SUVRSO,60-90min和SUVRSO,50-80min图像是[C-11] UCB-J BPSO参数图的优异代理。

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