18F-FDG PET 诊断和预后模式在轻度认知障碍(MCI)阶段的阿尔茨海默病(AD)患者中没有重叠。
18F-FDG PET diagnostic and prognostic patterns do not overlap in Alzheimer's disease (AD) patients at the mild cognitive impairment (MCI) stage.
机构信息
Nuclear Medicine Unit, IRCCS AOU San Martino, IST and Department of Health Sciences, University of Genoa, Largo R. Benzi 10, 16132, Genoa, Italy.
Clinical Neurology, Department of Neuroscience (DINOGMI), University of Genoa and IRCCS AOU San Martino-IST, Genoa, Italy.
出版信息
Eur J Nucl Med Mol Imaging. 2017 Nov;44(12):2073-2083. doi: 10.1007/s00259-017-3790-5. Epub 2017 Aug 7.
PURPOSE
We aimed to identify the cortical regions where hypometabolism can predict the speed of conversion to dementia in mild cognitive impairment due to Alzheimer's disease (MCI-AD).
METHODS
We selected from the clinical database of our tertiary center memory clinic, eighty-two consecutive MCI-AD that underwent 18F-fluorodeoxyglucose (FDG) PET at baseline during the first diagnostic work-up and were followed up at least until their clinical conversion to AD dementia. The whole group of MCI-AD was compared in SPM8 with a group of age-matched healthy controls (CTR) to verify the presence of AD diagnostic-pattern; then the correlation between conversion time and brain metabolism was assessed to identify the prognostic-pattern. Significance threshold was set at p < 0.05 False-Discovery-Rate (FDR) corrected at peak and at cluster level. Each MCI-AD was then compared with CTR by means of a SPM single-subject analysis and grouped according to presence of AD diagnostic-pattern and prognostic-pattern. Kaplan-Meier-analysis was used to evaluate if diagnostic- and/or prognostic-patterns can predict speed of conversion to dementia.
RESULTS
Diagnostic-pattern corresponded to typical posterior hypometabolism (BA 7, 18, 19, 30, 31 and 40) and did not correlate with time to conversion, which was instead correlated with metabolic levels in right middle and inferior temporal gyri as well as in the fusiform gyrus (prognostic-pattern, BA 20, 21 and 38). At Kaplan-Meier analysis, patients with hypometabolism in the prognostic pattern converted to AD-dementia significantly earlier than patients not showing significant hypometabolism in the right middle and inferior temporal cortex (9 versus 19 months; Log rank p < 0.02, Breslow test: p < 0.003, Tarone-Ware test: p < 0.007).
CONCLUSION
The present findings support the role of FDG PET as a robust progression biomarker even in a naturalist population of MCI-AD. However, not the AD-typical diagnostic-pattern in posterior regions but the middle and inferior temporal metabolism captures speed of conversion to dementia in MCI-AD since baseline. The highlighted prognostic pattern is a further, independent source of heterogeneity in MCI-AD and affects a primary-endpoint on interventional clinical trials (time of conversion to dementia).
目的
我们旨在确定皮质区域,在这些区域中代谢功能降低可以预测轻度认知障碍(MCI-AD)患者向痴呆转化的速度。
方法
我们从我们的三级中心记忆诊所的临床数据库中选择了 82 例连续的 MCI-AD 患者,这些患者在首次诊断性检查期间在基线时接受了 18F-氟脱氧葡萄糖(FDG)PET 检查,并至少随访至他们的临床诊断为 AD 痴呆。我们将 MCI-AD 整组与年龄匹配的健康对照组(CTR)在 SPM8 中进行比较,以验证 AD 诊断模式的存在;然后评估转换时间与脑代谢之间的相关性,以确定预后模式。采用 SPM 单个体分析将每个 MCI-AD 与 CTR 进行比较,并根据 AD 诊断模式和预后模式进行分组。采用 Kaplan-Meier 分析评估诊断模式和/或预后模式是否可以预测向痴呆的转化速度。
结果
诊断模式与典型的后部代谢功能降低相对应(BA7、18、19、30、31 和 40),但与转换时间无关,而与右侧中颞和下颞回以及梭状回的代谢水平相关(预后模式,BA20、21 和 38)。在 Kaplan-Meier 分析中,代谢功能降低的患者比未出现右侧中颞和下颞皮质明显代谢功能降低的患者更早转化为 AD 痴呆(9 个月与 19 个月;对数秩检验 p<0.02,Breslow 检验:p<0.003,Tarone-Ware 检验:p<0.007)。
结论
目前的研究结果支持 FDG PET 作为一种强大的进展生物标志物的作用,即使在 MCI-AD 的自然人群中也是如此。然而,在 MCI-AD 中,并不是后区的 AD 典型诊断模式,而是中颞和下颞代谢,自基线以来就可以捕获向痴呆的转化速度。突出的预后模式是 MCI-AD 异质性的另一个独立来源,并影响干预临床试验的主要终点(向痴呆的转化时间)。
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