Tir M, Delmaire C, Besson P, Defebvre L
Service de neurologie et pathologie du mouvement, hôpital Salengro, CHRU de Lille, EA 1046, département de pharmacologie médicale, université Lille Nord de France, 1, place de Verdun, 59045 Lille cedex, France; Service de neurologie, CHU d'Amiens, EA 4559, SFR CAP-Santé (FED 4231), université de Picardie-Jules-Verne, chemin du Thil, 80000 Amiens, France.
Service de neuroradiologie, hôpital Salengro, CHRU de Lille, EA 4559, université Lille Nord de France, rue Prof.-Émile-Laine, 59037 Lille cedex, France.
Rev Neurol (Paris). 2014 Apr;170(4):266-76. doi: 10.1016/j.neurol.2013.10.013. Epub 2014 Mar 20.
Conventional MRI is a well-described, highly useful tool for the differential diagnosis of degenerative parkinsonian syndromes. Nevertheless, the observed abnormalities may only appear in late-stage disease. Diffusion tensor imaging (DTI) can identify microstructural changes in brain tissue integrity and connectivity. The technique has proven value in the differential diagnosis of multiple system atrophy (MSA), progressive supranuclear palsy (PSP) and Parkinson's disease (PD). Here, we performed a systematic review of the literature on the main corticosubcortical DTI abnormalities identified to date in the context of the diagnosis of MSA and PSP with diffusion-weighted imaging, diffusion tensor imaging and anatomical connectivity studies. In good agreement with the histological data, increased diffusivity in the putamen (in MSA and PSP), in the middle cerebellar peduncles (in MSA) and in the upper cerebellar peduncles (in PSP) has been reported. Motor pathway involvement is characterized by low fraction anisotropy (FA) in the primary motor cortex in MSA-P and PSP, a high apparent diffusion coefficient (ADC) and low FA in the supplementary motor area in PSP. We then outline the value of these techniques in differential diagnosis (especially with respect to PD). Anatomical connectivity studies have revealed a lower number of fibers in the corticospinal tract in MSA and PSP (relative to PD and controls) and fewer tracked cortical projection fibers in patients with PSP or late-stage MSA (relative to patients with early MSA or PD and controls). Lastly, we report the main literature data concerning the value of DTI parameters in monitoring disease progression. The observed correlations between DTI parameters on one hand and clinical scores and/or disease duration on the other constitute strong evidence of the value of DTI in monitoring disease progression. In MSA, the ataxia score was correlated with ADC values in the pons and the upper cerebellar peduncles, whereas both the motor score and the disease duration were correlated with putaminal ADC values. In conclusion, DTI and connectivity studies constitute promising tools for differentiating between "Parkinson-plus" syndromes.
传统磁共振成像(MRI)是一种描述详尽且非常有用的工具,用于退行性帕金森综合征的鉴别诊断。然而,观察到的异常可能仅在疾病晚期出现。扩散张量成像(DTI)能够识别脑组织完整性和连通性的微观结构变化。该技术在多系统萎缩(MSA)、进行性核上性麻痹(PSP)和帕金森病(PD)的鉴别诊断中已被证明具有价值。在此,我们对迄今为止在MSA和PSP诊断背景下通过扩散加权成像、扩散张量成像和解剖连通性研究确定的主要皮质 - 皮质下DTI异常的文献进行了系统综述。与组织学数据高度一致的是,已有报道称壳核(在MSA和PSP中)、小脑中脚(在MSA中)和小脑上脚(在PSP中)的扩散率增加。运动通路受累的特征表现为,在MSA - P和PSP中初级运动皮层的各向异性分数(FA)较低,在PSP中辅助运动区的表观扩散系数(ADC)较高且FA较低。然后我们概述了这些技术在鉴别诊断中的价值(特别是相对于PD而言)。解剖连通性研究显示,MSA和PSP中皮质脊髓束的纤维数量较少(相对于PD和对照组),PSP或晚期MSA患者中追踪到的皮质投射纤维较少(相对于早期MSA或PD患者及对照组)。最后,我们报告了关于DTI参数在监测疾病进展方面价值 的主要文献数据。一方面观察到的DTI参数与另一方面的临床评分和/或疾病持续时间之间的相关性,构成了DTI在监测疾病进展方面具有价值的有力证据。在MSA中,共济失调评分与脑桥和小脑上脚的ADC值相关,而运动评分和疾病持续时间均与壳核ADC值相关。总之,DTI和连通性研究是区分“帕金森叠加”综合征的有前景的工具。
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