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FDG-PET degeneration patterns predict amyloid deposition in Corticobasal Syndrome

J. Parmera, A. Coutinho, A. Neto, C. Ono, M. Aranha, C. Buchpiguel, R. Nitrini, E. Barbosa, S. Brucki (Sao Paulo, Brazil)

Meeting: MDS Virtual Congress 2020

Abstract Number: 1117

Keywords: Corticobasal degeneration (CBD), Parkinsonism, Positron emission tomography(PET)

Category: Parkinsonism, Atypical: PSP, CBD

Objective: To investigate if an individual clinically-focused analysis of brain FDG-PET metabolic patterns and a comprehensive neurological evaluation could distinguish Corticobasal Syndrome (CBS) pathological variants based on Pittsburgh Compound B(PIB) PET status.

Background: CBS is related to multiple pathologies, including 4-repeat tauopathies (CBD and PSP) and also Alzheimer’s disease (AD). Previous works with post-mortem analysis established FDG-PET patterns closely related to CBD, PSP or AD pathology[1].

Method: Forty patients with probable CBS[2] were evaluated concerning their movement disorders and cognition. They were submitted to FDG-PET and, according to their metabolic patterns, distributed into two groups: likely related to AD (CBS FDG-PET AD) and unrelated to AD (CBS FDG-PET nonAD). Twenty-five patients underwent PIB-PET on a hybrid PET/MRI to assess amyloid status. Both FDG-PET and PIB-PET images were analyzed based on visual and 3D-SSP semi-quantitative parameters. Each examination was blind to other modalities.

Results: Based on the patterns at FDG-PET [figure1,2], we classified 12 patients (30%) as CBS FGD-PET AD and 28(70%) as CBS FDG-PET nonAD. All patients (100%) previously classified as CBS FDG-PET AD tested positive for amyloid deposition at PIB-PET and 88,9% classified as CBS FDG-PET nonAD tested negative (p=0,001 for PIB + status; sensitivity 77,8%; specificity 100%; accuracy 94,44%). There were no significant differences in age, gender, symptoms duration and schooling at FDG-PET groups or PIB status. Functional and cognitive impairment was more severe in the CBS FDG-PET AD group, which had worst scores in memory, attention and visuospatial domains [table 2]. CBS FDG-PET AD group also presented more frequently myoclonus (100% vs. 53,6%, p=0,004), displayed less frequently dystonia (16,7% vs. 57,1%, p=0,035) and had more neglect syndrome (p =0,041) and hallucinations (p=0,039) [figure 3]. Patients with PIB positive status also presented worst cognitive scores on memory and visuospatial domains.

Conclusion: FDG-PET was useful to depict CBS degeneration patterns, being able to detect a CBS-AD group with brain amyloid deposition, worst functional and cognitive decline, also showing high accuracy to exclude AD pathology in the CBS-nonAD group. Motor and cortical symptoms such as dystonia, myoclonus and neglect syndrome might aid biomarkers in distinguishing underlying pathology.

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References: 1. Matteo Pardini, Edward D. Huey, Salvatore Spina, et al. FDG-PET patterns associated with underlying pathology in corticobasal syndrome. Neurology 2019;92:1-15. 2. Armstrong MJ, Litvan I, Lang AE, Bak TH, Bhatia KP, Borroni B, et al. Criteria for the diagnosis of corticobasal degeneration.Neurology 2013;80:496–503

To cite this abstract in AMA style:

J. Parmera, A. Coutinho, A. Neto, C. Ono, M. Aranha, C. Buchpiguel, R. Nitrini, E. Barbosa, S. Brucki. FDG-PET degeneration patterns predict amyloid deposition in Corticobasal Syndrome [abstract]. Mov Disord. 2020; 35 (suppl 1). https://www.mdsabstracts.org/abstract/fdg-pet-degeneration-patterns-predict-amyloid-deposition-in-corticobasal-syndrome/. Accessed June 15, 2025.
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