首页> 外文会议>Nuclear Science Symposium Conference Record, 2007 IEEE; Honolulu,HI >Comparison of brain pet and sequential and simultaneous dual-isotope spect for estimation tasks in normal and parkinson subjects
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Comparison of brain pet and sequential and simultaneous dual-isotope spect for estimation tasks in normal and parkinson subjects

机译:正常人和帕金森病患者评估任务时脑宠物和连续双同位素同时同位素的比较

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Parkinson''s disease (PD) is a widespread neurodegenerative disorder characterized primarily by changes in motor function. It affects the dopamine transporter (DAT) system, and results in a reduction of DAT specific binding and volume of active dopamine transporters, in the striata. Early detection of PD, before the onset of clinical symptoms, has great potential in improving patient management. Dual-isotope SPECT allows the assessment of different brain functions under identical physiological conditions. Simultaneous dual-isotope studies have a further advantage over sequential studies as they provide perfect image registration and reduce imaging time for the same total collected counts. These advantages are limited however by cross-talk and downscatter between the two isotopes, especially in the case of 123I and 99mTc where the emission energies are very close (i.e., 159 and 140 keV). We compare DAT brain PET with sequential and simultaneous pre- and post-synaptic dual-isotope SPECT for the task of estimating striatal activity concentration and striatal size for a normal brain and for three early stages of PD. We used the Cramer-Rao lower bound, representing the theoretical best performance achievable, as our performance metric to objectively compare these modalities, and determine their performance in identifying early disease stages. Our findings show that PET and simultaneous and sequential SPECT can successfully identify the early stages of PD when estimating both pre-synaptic activity concentration and size. Post-synaptic SPECT imaging was not able to separate disease stages. PET and simultaneous SPECT perform well when estimating only activity concentration or size, but sequential SPECT has significantly degraded performance due to lower statistics.
机译:帕金森氏病(PD)是一种广泛的神经退行性疾病,其主要特征是运动功能改变。它会影响多巴胺转运蛋白(DAT)系统,并导致纹状体中DAT特异性结合的减少以及活性多巴胺转运蛋白的体积减少。在临床症状发作之前及早发现PD,具有改善患者管理的巨大潜力。双同位素SPECT可以在相同的生理条件下评估不同的大脑功能。同时进行的双同位素研究比顺序研究具有更多优势,因为它们可以提供完美的图像配准并减少相同总采集计数的成像时间。但是,这些优势受到两个同位素之间的串扰和向下散射的限制,尤其是在发射能量非常接近的 123 I和 99m Tc的情况下(即, 159和140 keV)。我们比较DAT脑PET与突触前和突触后双同位素SPECT的顺序和同步,以评估正常大脑和PD的三个早期阶段的纹状体活性浓度和纹状体大小。我们使用表示理论上可实现的最佳性能的Cramer-Rao下限作为我们的性能指标,以客观地比较这些模式,并确定其在识别早期疾病阶段中的性能。我们的发现表明,在估计突触前活性浓度和大小时,PET以及同时和顺序的SPECT可以成功地识别PD的早期阶段。突触后SPECT成像不能区分疾病阶段。仅估计活动浓度或大小时,PET和同时SPECT表现良好,但由于统计量较低,顺序SPECT的性能明显下降。

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