Exploring the Relation Between REM Sleep Behavior Disorder Onset and Striatal Dopaminergic Dysfunction in Parkinson's Disease

Overview

Journal J Neurol

Specialty Neurology

Date 2024 Dec 16

PMID 39680181

Authors

Calogero Edoardo Cicero

Claudio Terravecchia

Silvia Tabbi

Rossella Garofalo

Antonina Luca

Giovanni Mostile

Giulia Donzuso

Donatella Contrafatto

Mario Zappia

Alessandra Nicoletti

Affiliations

Soon will be listed here.

Abstract

Background: The α-Synuclein Origin and Connectome (SOC) model recently proposed two different Parkinson's Disease (PD) phenotypes clinically based on the relationship between REM sleep behavior disorder (RBD) and motor symptoms' onset: a "body first" phenotype and a "brain first" phenotype in which RBD precedes or may follow the motor onset, respectively. A higher burden of non-motor symptoms as well as a more symmetrical clinical presentation have also been predicted in the body-first phenotype. This point has been poorly assessed through semi-quantitative striatal dopaminergic functional imaging to date.

Objectives: To explore the relation between RBD onset and striatal dysfunction in PD.

Methods: PD patients were retrospectively enrolled and clinical follow-up data were gathered. Presence and onset of probable RBD were evaluated classifying patients into PD-RBDpre (onset before motor symptoms), PD-RBDpost (onset after motor symptoms) and PD-RBD-. Semi-quantitative I-FP-CIT-DAT-SPECT imaging was performed at baseline. Mean putamen and caudate-specific binding ratios (SBR) and asymmetry index (AI) were computed.

Results: Fifty-six PD patients were enrolled (10 PD-RBDpre, 19 PD-RBDpost and 27 PD-RBD-). A more symmetrical motor impairment, higher mild cognitive impairment (MCI) prevalence, lower caudate SBR and lower putamen AI were found in PD-RBDpre. A negative trend in MCI prevalence as well as a positive trend in both caudate SBR and putamen AI were found across PD-RBDpre, PD-RBDpost and PD-RBD-.

Conclusions: Different patterns of striatal dopaminergic dysfunction and cognitive impairment based on RBD onset were unraveled, supporting the SOC model's predictions.

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