Parkinson Disease, Parkinsonian Disorders, Brain Disease, Basal Ganglia Diseases, Synucleinopathies
Conditions
Keywords
Neurodegenerative Diseases, Nervous System Diseases, Movement Disorders, biomarker, neuroinflammation, brain-first, body-first, axial symptoms
Brief summary
This observational study aims to systematically characterize a cohort of patients with early-stage Parkinson's disease (PD) attending the Movement Disorders Center of AUSL-IRCCS Reggio Emilia, Italy. PD is the second most common neurodegenerative disorder, affecting about 1% of individuals over 60 years of age. The project will explore clinical and biological differences between the recently proposed Brain-First and Body-First phenotypes of PD. Patients will undergo detailed clinical evaluation, neuroimaging, and biomarker assessments (including neurodegeneration and neuroinflammation markers). Particular attention will be given to the progression of axial and cognitive symptoms, which represent major contributors to disability. Findings from this study are expected to improve early patient stratification, clarify disease mechanisms, and support the development of precision medicine strategies and future disease-modifying therapies.
Detailed description
Parkinson's disease (PD) is the second most common neurodegenerative disorder after Alzheimer's disease, affecting up to 1% of individuals over the age of 60. While treatment remains symptomatic and no disease-modifying therapies are currently available, increasing research efforts are focusing on precision medicine approaches and the identification of disease subtypes that may guide prognosis and therapy. Historically, PD patients have been classified according to motor (tremor-dominant, akinetic-rigid, axial) and non-motor features (sleep disturbances, autonomic dysfunction, mood disorders, fatigue, pain, weight loss, cognitive impairment). Genetic classifications have also been introduced, with approximately 10-15% of patients carrying mutations such as GBA or LRRK2, which are associated with earlier onset and potentially more aggressive disease. In the early 2000s, Braak and colleagues proposed a neuropathological staging system in which α-synuclein pathology progresses in a stereotypical pattern from peripheral to central structures. More recent clinical and pathological evidence, however, has challenged this model and led to the proposal of two distinct subtypes: Brain-First and Body-First. In Brain-First PD, pathology begins in the central nervous system and spreads to the autonomic system; in Body-First PD, pathology originates in peripheral structures such as the enteric nervous system, propagating rostrally to involve the brain. REM sleep behavior disorder (RBD) has emerged as a clinical marker of the Body-First subtype. This study will systematically characterize patients with early-stage PD, combining detailed clinical evaluation with instrumental assessments including neuroimaging and blood-based biomarkers. In particular, the project will investigate whether Brain-First and Body-First phenotypes differ in terms of: * Clinical progression (with focus on axial and cognitive symptoms). * Neurodegeneration biomarkers, including neurofilament light chain. * Neuroinflammation markers, such as immune responses to α-synuclein, interferon-gamma, and interleukin-5. The overarching goal is to identify biological and clinical markers that distinguish PD subtypes, improve early stratification, and support the development of targeted, disease-modifying therapies.
Interventions
OTHERClinical assessments
standardized neurological examination, motor and non-motor symptom scales, cognitive testing, and autonomic symptom questionnaires.
OTHERPhenotypic classification
patients will be stratified into Brain-First and Body-First phenotypes based on the presence of RBD and instrumental findings.
Sponsors
Azienda USL Reggio Emilia - IRCCS
Study design
Observational model
COHORT
Time perspective
PROSPECTIVE
Eligibility
Sex/Gender
ALL
Age
18 Years to No maximum
Healthy volunteers
No
Inclusion criteria
* Patients diagnosed with PD according to the MDS Clinical Diagnostic Criteria for Parkinson's Disease divided into brain-first and body-first phenotypes, based on the presence or absence of a REM sleep behavior disorder diagnosed using ambulatory polysomnography methods according to the criteria of the International Classification of Sleep Disorders (ICSD-3) criteria and on data from SPECT with DATSCAN and myocardial innervation scintigraphy \[123I-MIBG\]. * Free and informed consent expressed by the participant. * At least 18 years of age.
Exclusion criteria
* Inability to express free and informed consent. * Patient with a doubtful diagnosis. * Participant under 18 years of age.
Design outcomes
Primary
| Measure | Time frame | Description |
|---|---|---|
| Assessment of the progression of axial symptoms | baseline, 12, 24, 36,48, 60 months | Differences in quantitative parameters of gait (phase duration, root mean square of the acceleration of the trunk in x, y, z axes) assessed through the instrumented Timed Up and Go test (phases considered: overall iTUG, sit-to-stand, sitting, first turn, second turn, walking forward, return gait) between the brain-first and body-first groups at diagnosis and at subsequent annual follow-up visits (5-year follow-up) in OFF-medication and ON-Medication (both in single and dual task) conditions. |
| Risk of falling in the two subgroups, brain-first and body-first | baseline, 12, 24, 36,48, 60 months | Assessment of possible differences in scores obtained on the Walking Handicap Scale (WHS) at baseline and at subsequent annual follow-up visits (5-year follow-up). The Walking Handicap Scale (WHS) measures walking ability and community mobility across six levels, from limited physiological walking to unrestricted social ambulation. Possible scores range from 1 (most limited walking ability) to 6 (fully independent walking in social environments); higher scores indicate better walking function. |
Secondary
| Measure | Time frame | Description |
|---|---|---|
| Assessment of disease progression | baseline, 12, 24, 36,48, 60 months | Assessment of the differences in the MDS-UPDRS total scores (part I, II, III, IV) and subscores (tremor, bradykinesia, rigidity, postural instability and gait difficulty, gait, dyskinesia and fluctuations subscores) in the study population at baseline and at subsequent annual follow-up visits (5-year follow-up). |
| Assessment of the progression of neurodegeneration and inflammatory biomarkers (neurofilaments, interferon-γ, cell-mediated anti-α-synuclein responses). | baseline, 12, 24, 36,48, 60 months | Assessment of the differences in neurodegeneration and inflammatory biomarkers (neurofilaments, interferon-γ, cell-mediated anti-α-synuclein responses) in a subset of 50 patients in the study population. Analysis of differences in neurofilament levels and cell-mediated responses at baseline and at subsequent annual follow-up visits (5-year follow-up). |
| Brain MRI: analysis of differences in qualitative and quantitative parameters extrapolated at diagnosis. | 24 months | Assessment of quantitative differences in the degree of cortical and subcortical atrophy (volumetric automated segmentation of cerebral regions with the Quibim Precision software® quantified as % of intracranial volume) in the study population assessed through volumetric 1.5 Tesla brain MRI at baseline. |
| Baseline Assessment of Nigrostriatal and Myocardial Denervation. | 24 months | Semiquantitative assessment (heart to mediastinum ratio \[H/M\]) of differences in myocardial denervation in the study population through cardiac 123I-MIBG scintigraphy (early and delayed imaging) |
Countries
Italy
Contacts
Primary ContactFrancesco Cavallieri, MD
Backup ContactStefania Croci, BSc
Outcome results
None listed