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脑容量和代谢模式可预测进行性核上性麻痹谱系障碍的临床特征。

Patterns of brain volume and metabolism predict clinical features in the progressive supranuclear palsy spectrum.

作者信息

Ali Farwa, Clark Heather, Machulda Mary, Senjem Matthew L, Lowe Val J, Jack Clifford R, Josephs Keith A, Whitwell Jennifer, Botha Hugo

机构信息

Department of Neurology, Mayo Clinic, Rochester, MN 55905, USA.

Department of Psychiatry and Psychology, Mayo Clinic, Rochester, MN 55905, USA.

出版信息

Brain Commun. 2024 Jul 16;6(4):fcae233. doi: 10.1093/braincomms/fcae233. eCollection 2024.

Abstract

Progressive supranuclear palsy (PSP) is a neurodegenerative tauopathy that presents with highly heterogenous clinical syndromes. We perform cross-sectional data-driven discovery of independent patterns of brain atrophy and hypometabolism across the entire PSP spectrum. We then use these patterns to predict specific clinical features and to assess their relationship to phenotypic heterogeneity. We included 111 patients with PSP (60 with Richardson syndrome and 51 with cortical and subcortical variant subtypes). Ninety-one were used as the training set and 20 as a test set. The presence and severity of granular clinical variables such as postural instability, parkinsonism, apraxia and supranuclear gaze palsy were noted. Domains of akinesia, ocular motor impairment, postural instability and cognitive dysfunction as defined by the Movement Disorders Society criteria for PSP were also recorded. Non-negative matrix factorization was used on cross-sectional MRI and fluorodeoxyglucose-positron emission tomography (FDG-PET) scans. Independent models for each as well as a combined model for MRI and FDG-PET were developed and used to predict the granular clinical variables. Both MRI and FDG-PET were better at predicting presence of a symptom than severity, suggesting identification of disease state may be more robust than disease stage. FDG-PET predicted predominantly cortical abnormalities better than MRI such as ideomotor apraxia, apraxia of speech and frontal dysexecutive syndrome. MRI demonstrated prediction of cortical and more so sub-cortical abnormalities, such as parkinsonism. Distinct neuroanatomical foci were predictive in MRI- and FDG-PET-based models. For example, vertical gaze palsy was predicted by midbrain atrophy on MRI, but frontal eye field hypometabolism on FDG-PET. Findings also differed by scale or instrument used. For example, prediction of ocular motor abnormalities using the PSP Saccadic Impairment Scale was stronger than with the Movement Disorders Society Diagnostic criteria for PSP oculomotor impairment designation. Combination of MRI and FDG-PET demonstrated enhanced detection of parkinsonism and frontal syndrome presence and apraxia, cognitive impairment and bradykinesia severity. Both MRI and FDG-PET patterns were able to predict some measures in the test set; however, prediction of global cognition measured by Montreal Cognitive Assessment was the strongest. MRI predictions generalized more robustly to the test set. PSP leads to neurodegeneration in motor, cognitive and ocular motor networks at cortical and subcortical foci, leading to diverse yet overlapping clinical syndromes. To advance understanding of phenotypic heterogeneity in PSP, it is essential to consider data-driven approaches to clinical neuroimaging analyses.

摘要

进行性核上性麻痹(PSP)是一种神经退行性tau蛋白病,表现出高度异质性的临床综合征。我们对整个PSP谱系中的脑萎缩和代谢减低的独立模式进行了横断面数据驱动的发现。然后,我们使用这些模式来预测特定的临床特征,并评估它们与表型异质性的关系。我们纳入了111例PSP患者(60例患有理查森综合征,51例患有皮质和皮质下变异亚型)。91例用作训练集,20例用作测试集。记录了诸如姿势不稳、帕金森症、失用症和核上性凝视麻痹等详细临床变量的存在情况和严重程度。还记录了运动障碍协会PSP标准所定义的运动不能、眼球运动障碍、姿势不稳和认知功能障碍等领域。对横断面MRI和氟脱氧葡萄糖正电子发射断层扫描(FDG-PET)进行非负矩阵分解。分别为MRI和FDG-PET建立独立模型以及为MRI和FDG-PET建立联合模型,并用于预测详细临床变量。MRI和FDG-PET在预测症状的存在方面比预测严重程度更好,这表明识别疾病状态可能比疾病阶段更可靠。FDG-PET在预测主要皮质异常方面比MRI更好,如观念运动性失用症、言语失用症和额叶执行功能障碍综合征。MRI显示出对皮质尤其是皮质下异常的预测能力,如帕金森症。在基于MRI和FDG-PET的模型中,不同的神经解剖学病灶具有预测性。例如,MRI上的中脑萎缩可预测垂直凝视麻痹,而FDG-PET上的额叶眼区代谢减低可预测垂直凝视麻痹。研究结果也因所使用的量表或工具而异。例如,使用PSP扫视损伤量表对眼球运动异常的预测比使用运动障碍协会PSP眼球运动障碍诊断标准更强。MRI和FDG-PET的联合显示出对帕金森症和额叶综合征存在以及失用症、认知障碍和运动迟缓严重程度的检测能力增强。MRI和FDG-PET模式都能够在测试集中预测一些指标;然而,通过蒙特利尔认知评估测量的整体认知预测最强。MRI预测在测试集中的泛化性更强。PSP导致皮质和皮质下病灶处的运动、认知和眼球运动网络发生神经退行性变,从而导致多样但重叠的临床综合征。为了增进对PSP表型异质性的理解,考虑数据驱动的临床神经影像学分析方法至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9c5e/11272075/24d21727f2f3/fcae233_ga.jpg

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