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Early Dementia with Lewy Bodies and Parkinson’s Disease with RBD: two faces of the same coin?

B. Orso, P. Mattioli, F. Famà, F. Massa, M. Pardini, A. Brugnolo, N. Girtler, S. Raffa, L. Sofia, S. Morbelli, D. Arnaldi (Genoa, Italy)

Meeting: 2024 International Congress

Abstract Number: 126

Keywords: Positron emission tomography(PET), Single-photon emission computed tomography(SPECT), Synucleinopathies

Category: Parkinson's Disease and Lewy Body Dementia

Objective: To describe clinical and imaging differences in de novo PD with and without REM sleep Behaviour Disorder (dnPDRBD – de novo PD) and de novo DLB with RBD (dnDLBRBD) patients to gain insight on the neuronal α-synuclein diseases (NSDs) continuum.

Background: The new definition of NSDs suggests that a clear distinction between PD and DLB should be reconsidered.[1]

Method: 32 de novo PD (age 72.6±6; 23 males), 30 de novo DLB (age 78±5.4; 18 males) patients with evidence of RBD, and 31 de novo PD (age 71.8±6; 19 males), underwent clinical and neuropsychological evaluation, brain [18F]FDG PET and [123I]FP-CIT SPECT. Between-group demographic, clinical, cognitive and imaging features were compared by performing an analysis of variance (ANOVA). [18F]FDG-PET and [123I]FP-CIT SPECT images (48%) were flipped (More affected hemisphere-MAH= right; Less Affected Hemisphere-LAH= left).

Results: Compared with dnPDRBD and de novo PD, dnDLBRBD patients were older, with lower education and lower MMSE scores (p<0.001)[Table 1]. Differences in frequency of MCI, Parkinsonism, Visual Hallucinations and Fluctuations are summarized in Figure 1. We found a significant variance in [18F]FDG uptake in the temporal and occipital gyri, precuneus, and the right cuneus[Figure 2A]. At post-hoc, dnDLBRBD patients have a worst alteration of brain metabolism than de novo PD and dnPDRBD patients (p<0.0001)[Figure 2B]. De novo PD presents with a significantly lower [123I]FP-CIT binding in the LAH Putamen (p=0.04), MAH Putamen (p=0.04), mean Putamen uptake (p=0.03) and LAH Caudate (p=0.02) compared to dnPDRBD. [123I]FP-CIT binding profiles are shown in Figure 3. dnDLBRBD patients had a more severe global cognitive impairment than both de novo PD and dnPDRBD patients. de novo PD and dnPDRBD patients had a similar cognitive profile[Figure 4].

Conclusion: We confirmed that DLB and PD are placed on the same pathological NSDs continuum. In PD, presence of RBD helps determining in which end of the continuum patients fit better.

Table 1: Demographic and clinical features.

Table 1: Demographic and clinical features.

Figure 1: Frequency of core clinical features

Figure 1: Frequency of core clinical features

Figure 2: FDG Analysis of variance (ANOVA) results

Figure 2: FDG Analysis of variance (ANOVA) results

Figure 3: SPECT Analysis of variance (ANOVA)

Figure 3: SPECT Analysis of variance (ANOVA)

Figure 4: NPS Analysis of variance (ANOVA) results

Figure 4: NPS Analysis of variance (ANOVA) results

References: [1] Simuni, T., Chahine, L. M., Poston, K., Brumm, M., Buracchio, T., Campbell, M., … & Marek, K. (2024). A biological definition of neuronal α-synuclein disease: towards an integrated staging system for research. The Lancet Neurology, 23(2), 178-190.

To cite this abstract in AMA style:

B. Orso, P. Mattioli, F. Famà, F. Massa, M. Pardini, A. Brugnolo, N. Girtler, S. Raffa, L. Sofia, S. Morbelli, D. Arnaldi. Early Dementia with Lewy Bodies and Parkinson’s Disease with RBD: two faces of the same coin? [abstract]. Mov Disord. 2024; 39 (suppl 1). https://www.mdsabstracts.org/abstract/early-dementia-with-lewy-bodies-and-parkinsons-disease-with-rbd-two-faces-of-the-same-coin/. Accessed July 13, 2025.
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