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Neurite orientation dispersion and density imaging (NODDI) and free‐water imaging in Parkinsonism

机译:神经痛取向弥散和密度成像(NODDI)和帕金森病中的自由水成像

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摘要

Neurite orientation dispersion and density imaging (NODDI) uses a three‐compartment model to probe brain tissue microstructure, whereas free‐water (FW) imaging models two‐compartments. It is unknown if NODDI detects more disease‐specific effects related to neurodegeneration in Parkinson's disease (PD) and atypical Parkinsonism. We acquired multi‐ and single‐shell diffusion imaging at 3 Tesla across two sites. NODDI (using multi‐shell; isotropic volume [Viso]; intracellular volume [Vic]; orientation dispersion [ODI]) and FW imaging (using single‐shell; FW; free‐water corrected fractional anisotropy [FAt]) were compared with 44 PD, 21 multiple system atrophy Parkinsonian variant (MSAp), 26 progressive supranuclear palsy (PSP), and 24 healthy control subjects in the basal ganglia, midbrain/thalamus, cerebellum, and corpus callosum. There was elevated Viso in posterior substantia nigra across Parkinsonisms, and Viso, Vic, and ODI were altered in MSAp and PSP in the striatum, globus pallidus, midbrain, thalamus, cerebellum, and corpus callosum relative to controls. The mean effect size across regions for Viso was 0.163, ODI 0.131, Vic 0.122, FW 0.359, and FAt 0.125, with extracellular compartments having the greatest effect size. A key question addressed was if these techniques discriminate PD and atypical Parkinsonism. Both NODDI (AUC: 0.945) and FW imaging (AUC: 0.969) had high accuracy, with no significant difference between models. This study provides new evidence that NODDI and FW imaging offer similar discriminability between PD and atypical Parkinsonism, and FW had higher effect sizes for detecting Parkinsonism within regions across the basal ganglia and cerebellum.
机译:神经元定向弥散和密度成像(NODDI)使用三室模型来探测脑组织的微观结构,而自由水(FW)成像则对两个室进行建模。尚不清楚NODDI是否能检测到更多与帕金森氏病(PD)和非典型帕金森病有关的神经变性相关疾病。我们在两个站点的3 Tesla处获得了多壳和单壳扩散成像。比较了NODDI(使用多壳;各向同性体积[Viso];细胞内体积[Vic];取向分散[ODI])和FW成像(使用单壳; FW;自由水校正分数各向异性[FAt])与44 PD,基底节,中脑/丘脑,小脑和call体中的21个多系统萎缩性帕金森氏变种(MSAp),26个进行性核上性麻痹(PSP)和24个健康对照组。在整个帕金森病中,黑质后部的Viso升高,相对于对照组,纹状体,苍白球,中脑,丘脑,小脑和call体的MSAp和PSP中的Viso,Vic和ODI发生了改变。 Viso跨区域的平均效应大小为0.163,ODI 0.131,Vic 0.122,FW 0.359和FAt 0.125,其中胞外区室的效应大小最大。解决的关键问题是这些技术是否能够区分PD和非典型帕金森病。 NODDI(AUC:0.945)和FW成像(AUC:0.969)都具有很高的准确性,并且模型之间没有显着差异。这项研究提供了新的证据,即NODDI和FW成像可在PD和非典型帕金森病之间提供相似的可分辨性,并且FW在基底神经节和小脑区域内检测帕金森病的效果更大。

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