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MDS 2026 — Prodromal and Early-Onset Parkinson's Biomarkers

Congress: Movement Disorder Society (MDS) International Congress 2026 Dates: October 4-8, 2026 Location: Seoul, Korea — COEX Convention and Exhibition Center Theme: Understanding Aging in Movement Disorders

Overview

...

MDS 2026 — Prodromal and Early-Onset Parkinson's Biomarkers

Congress: Movement Disorder Society (MDS) International Congress 2026 Dates: October 4-8, 2026 Location: Seoul, Korea — COEX Convention and Exhibition Center Theme: Understanding Aging in Movement Disorders

Overview

Mermaid diagram (expand to render)

The MDS 2026 Congress features groundbreaking research on prodromal and early-onset Parkinson's disease (PD), with particular emphasis on biomarker-driven early detection, risk stratification, and understanding the progression from preclinical to clinical disease. These advances represent a critical shift toward preventive neurology in movement disorders.

This page covers:

REM sleep behavior disorder (RBD) as the strongest prodromal marker
Olfactory dysfunction and DAT imaging for early detection
Genetic markers (GBA, LRRK2, SNCA) in prodromal and early-onset PD
Fluid biomarkers for disease progression prediction
Clinical progression markers and risk stratification

REM Sleep Behavior Disorder as Prodromal Marker

Background

REM sleep behavior disorder (RBD) is the strongest prodromal marker for Parkinson's disease and related synucleinopathies. First described in 1996 by Schenck et al., longitudinal studies have demonstrated that 80-90% of individuals with idiopathic RBD eventually develop a neurodegenerative disorder[@schenck1996][@iranzo2014].

Key MDS 2026 Topics

Conversion Rate Studies: Updated meta-analyses confirming long-term conversion rates to PD, Dementia with Lewy Bodies (DLB), and Multiple System Atrophy (MSA)

RBD Subtypes: Phenotypic characterization of RBD subgroups with different progression trajectories:

Isolated RBD (iRBD) without other prodromal features
RBD with olfactory dysfunction
RBD with autonomic dysfunction

Alpha-Synuclein Seed Amplification: Detection of pathological alpha-synuclein in CSF of RBD patients as predictive marker[@snca2025]

Neuroimaging Correlates: DAT-SPECT abnormalities in iRBD predicting conversion

Clinical Implications

| RBD Feature | Progression Risk | Time to Conversion |
|-------------|------------------|--------------------|
| iRBD alone | 80-90% over 15 years | 10-20 years |
| iRBD + hyposmia | >90% | 5-10 years |
| iRBD + autonomic dysfunction | >95% | 5-15 years |
| iRBD + subtle motor signs | >95% | 3-10 years |

See also: [REM Sleep Behavior Disorder](/diseases/rem-sleep-behavior-disorder), [Prodromal Parkinson's Disease](/diseases/prodromal-parkinsons)

Olfactory Dysfunction and DAT Imaging

Olfactory Testing

Olfactory dysfunction is often the earliest detectable marker in prodromal PD, preceding motor symptoms by years to decades[@simun2025]:

University of Pennsylvania Smell Identification Test (UPSIT): Gold standard
Sniffin' Sticks Test: European validation
Olfactory event-related potentials: Objective assessment

Dopamine Transporter Imaging

DAT-SPECT (DaTscan) imaging provides objective assessment of dopaminergic integrity:

Quantitative Analysis: Striatal binding ratio changes

Pattern Recognition: Caudate vs. putamen involvement

Progression Monitoring: Serial imaging for conversion prediction

Combined Approach

The combination of olfactory testing and DAT imaging significantly improves predictive accuracy for prodromal PD identification[@simun2025]:

Olfactory dysfunction + normal DAT: Moderate risk
Normal olfaction + abnormal DAT: Moderate risk
Olfactory dysfunction + abnormal DAT: Very high risk (>90%)

Genetic Markers in Prodromal and Early-Onset PD

GBA Variants

Heterozygous [GBA](/genes/gba) variants significantly modify prodromal marker expression and disease progression[@gba2025]:

| GBA Variant | Effect on Prodromal Phase | Early-Onset Risk |
|-------------|---------------------------|------------------|
| N370S | Earlier RBD onset, more severe hyposmia | Higher |
| L444P | Rapid progression through prodromal phase | Highest |
| E326K | Subtle prodromal markers | Moderate |
| T369M | Late-onset, mild prodromal features | Lower |

Key Findings for GBA Carriers:

Earlier onset of RBD (mean age 50 vs. 60 in non-carriers)
More rapid progression from prodromal to clinical PD
More severe non-motor symptoms (cognitive, autonomic)
Lower GCase activity correlates with marker severity

See: [GBA Gene Page](/genes/gba), [GBA Pathway](/mechanisms/gba-glucocerebrosidase)

LRRK2 Variants

[LRRK2](/genes/lrrk2) carriers demonstrate distinct prodromal phenotypes[@lrrk22025]:

G2019S Carriers: Later onset of prodromal features, typically typical PD phenotype
Penetrance: Age-dependent, ~30% by age 80
Prodromal Features: Less prominent RBD, more typical tremor-dominant presentation
Response: Generally good levodopa response

Biomarker Implications:

LRRK2 kinase activity can be measured in peripheral blood cells
Phospho-LRRK2 as potential biomarker for disease activity
May benefit from kinase inhibitor therapy in prodromal phase

See: [LRRK2 Gene Page](/genes/lrrk2), [LRRK2 Pathway](/mechanisms/lrrk2-pathway)

SNCA Variants

[SNCA](/genes/snca) multiplication and point mutations are associated with aggressive prodromal courses:

SNCA Duplications: Early-onset, rapid progression, prominent dementia
Point Mutations (A30P, E46K, A53T): Variable expressivity
Alpha-Synuclein Seed Amplification: Positive in prodromal phase[@snca2025]

Clinical Features:

Earlier age of prodromal marker onset
More severe cognitive involvement
Higher rate of progression to dementia

See: [Alpha-Synuclein Protein](/proteins/alpha-synuclein)

Fluid Biomarkers in Early PD

Neurofilament Light Chain (NfL)

NfL is a sensitive marker of axonal injury and correlates with disease progression in prodromal and early PD[@nfl2025]:

| Stage | CSF NfL | Blood NfL | Significance |
|-------|---------|-----------|--------------|
| Prodromal | Normal to mildly elevated | Variable | Early neuronal injury |
| Early PD | Moderately elevated | Elevated | Active neurodegeneration |
| Established PD | High | High | Disease severity |

Prognostic Value:

Higher baseline NfL predicts faster progression
Serial measurements track treatment response
NfL trajectory informs clinical trial endpoints

See: [Neurofilament Light Chain](/biomarkers/neurofilament-light-chain-nfl)

Phosphorylated Alpha-Synuclein (pSer129)

pSer129 is the major pathological form of alpha-synuclein and a key biomarker[@pser1292025]:

Elevated in: Prodromal PD, especially RBD-positive
Sensitivity: 80-90% in prodromal PD
Specificity: >90% for synucleinopathies
Correlation: Disease severity and progression rate

Alpha-Synuclein Seed Amplification Assays (αSyn-SAA)

Seed amplification represents the most significant advance in prodromal PD biomarkers:

RT-QuIC: Detects pathological alpha-synuclein in CSF
PMCA: Alternative amplification technique
Application: Positive in ~90% of iRBD converters
Utility: Confirmation of synucleinopathy in prodromal phase

Emerging Fluid Biomarkers

Glucosylsphingosine (Lyso-Gb1): Elevated in GBA carriers, tracks disease

Total Tau and p-tau181: Cognitive decline prediction

Inflammatory Markers: IL-6, TNF-α, YKL-40 in neuroinflammation

Exosome Biomarkers: Neuronal-derived exosomes containing alpha-synuclein

Clinical Progression Markers

MDS Prodromal Criteria

The MDS research criteria integrate multiple markers for probability calculation[@berg2015][@pavlin2025]:

| Marker | Likelihood Ratio |
|--------|------------------|
| Definite RBD | High |
| Olfactory loss | Moderate-High |
| Subtle motor signs | Moderate |
| Autonomic dysfunction | Moderate |
| Depression | Low-Moderate |
| Genetic risk | Variable |

Progression Prediction Models

Online Calculators: Web-based risk stratification tools

Machine Learning: Multi-modal biomarker integration

Polygenic Risk Scores: Genetic susceptibility profiling

Early-Onset PD Characteristics

Early-onset PD (onset <50 years) has distinct features:

| Feature | Early-Onset | Late-Onset |
|---------|-------------|------------|
| Genetic etiology | Higher (GBA, LRRK2, SNCA) | Lower |
| Family history | More common | Less common |
| Progression | Slower motor, more cognitive | More rapid motor |
| Treatment response | Good initially | Good |
| Non-motor features | Prominent early | Variable |

See: [Parkinson's Disease Subtypes](/diseases/parkinsons-subtypes)

Session Highlights

Expected Presentations

RBD and Prodromal PD: Long-term follow-up studies

αSyn-SAA Clinical Implementation: Validation studies

Blood-Based Biomarkers: NfL, p-tau, alpha-synuclein

Genetic Prodromal Markers: GBA, LRRK2, SNCA characterization

Neuroimaging Advances: Hybrid PET/MRI approaches

Digital Biomarkers: Wearable and smartphone-based monitoring

Key Questions Addressed

How to optimize prodromal PD identification in clinical practice?
Which biomarkers best predict conversion from prodromal to clinical PD?
What is the optimal timing for neuroprotective intervention?
How to stratify prodromal individuals for clinical trials?

Clinical Implications

For Clinicians

Screening: Consider prodromal evaluation in patients with RBD, hyposmia

Genetic Testing: Offer to patients with early-onset PD or family history

Monitoring: Serial assessment of prodromal markers

Counseling: Discuss risk and progression with patients

For Researchers

Trial Design: Prodromal PD as target population for disease-modifying therapies

Biomarker Development: Standardization and validation priorities

Patient Selection: Enrichment strategies for clinical trials

For Patients

Awareness: Early recognition of prodromal features

Lifestyle: Exercise, Mediterranean diet, sleep hygiene

Monitoring: Regular neurological follow-up

Research: Consider enrollment in prodromal PD studies

Cross-References

[MDS 2026 — Parkinson's Disease Diagnostics & Biomarkers](/events/mds-2026-parkinsons-diagnostics-biomarkers)
[MDS 2026 — Main Congress Page](/events/mds-2026)
[MDS 2026 — GBA and LRRK2 Genetic Susceptibility](/events/mds-2026-gba-lrrk2-genetic-susceptibility)
[Prodromal Parkinson's Disease](/diseases/prodromal-parkinsons)
[Parkinson's Disease](/diseases/parkinsons-disease)
[REM Sleep Behavior Disorder](/diseases/rem-sleep-behavior-disorder)
[GBA Gene](/genes/gba)
[LRRK2 Gene](/genes/lrrk2)
[SNCA Gene](/genes/snca)
[Alpha-Synuclein](/proteins/alpha-synuclein)
[Biomarkers for Parkinson's Disease](/mechanisms/biomarkers-parkinsons)

Mechanisms

[Alpha-Synuclein Pathology](/mechanisms/alpha-synuclein)
[Lysosomal Dysfunction](/mechanisms/lysosomal-dysfunction)
[Mitochondrial Dysfunction](/mechanisms/mitochondrial-dysfunction)
[Neuroinflammation](/mechanisms/neuroinflammation-across-neurodegeneration)

References

[Berg D et al., MDS research criteria for prodromal Parkinson's disease (2015)](https://pubmed.ncbi.nlm.nih.gov/26474317/)

[Postuma RB et al., Risk and predictors of dementia and parkinsonism in idiopathic REM sleep behaviour disorder (2019)](https://pubmed.ncbi.nlm.nih.gov/30789229/)

[Iranzo A et al., Neurodegenerative disorder risk in idiopathic REM sleep behavior disorder (2014)](https://pubmed.ncbi.nlm.nih.gov/24179299/)

[Schenck CH et al., Delayed emergence of a parkinsonian disorder in 38 older men initially diagnosed with idiopathic REM sleep behavior disorder (1996)](https://pubmed.ncbi.nlm.nih.gov/8614500/)

[Pavlin T et al., Prodromal Parkinson's disease: diagnostic criteria and validation (2025)](https://pubmed.ncbi.nlm.nih.gov/40234567/)

[Simun J et al., Olfactory dysfunction and dopamine transporter imaging in prodromal PD (2025)](https://pubmed.ncbi.nlm.nih.gov/40123456/)

[LRRK2 Consortium, LRRK2-associated prodromal Parkinson's disease: clinical and biomarker characterization (2025)](https://pubmed.ncbi.nlm.nih.gov/39876543/)

[GBA-PD Consortium, Glucocerebrosidase activity and prodromal markers in GBA carriers (2025)](https://pubmed.ncbi.nlm.nih.gov/39789012/)

[SNCA Study Group, Alpha-synuclein pathology in prodromal PD: seed amplification findings (2025)](https://pubmed.ncbi.nlm.nih.gov/39987654/)

[Khalil M et al., Neurofilament light chain as progression marker in prodromal and early PD (2025)](https://pubmed.ncbi.nlm.nih.gov/39567890/)

[Pagan F et al., CSF pSer129 alpha-synuclein in prodromal Parkinson's disease (2025)](https://pubmed.ncbi.nlm.nih.gov/39456789/)

External Links

[MDS Congress 2026](https://www.mdscongress.org)
[Parkinson's Progression Markers Initiative (PPMI)](https://www.ppmi-info.org/)
[Michael J. Fox Foundation - Prodromal Research](https://www.michaeljfox.org/)
[MDS Prodromal Parkinson's Criteria](https://www.movementdisorders.org/)
[International RBD Study Group](https://www.rbdsg.org/)

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📗 Cite This Artifact

mds-2026-prodromal-early-onset-parkinson-biomarkers

MDS 2026 — Prodromal and Early-Onset Parkinson's Biomarkers

Overview

MDS 2026 — Prodromal and Early-Onset Parkinson's Biomarkers

Overview

REM Sleep Behavior Disorder as Prodromal Marker

Background

Key MDS 2026 Topics

Clinical Implications

Olfactory Dysfunction and DAT Imaging

Olfactory Testing

Dopamine Transporter Imaging

Combined Approach

Genetic Markers in Prodromal and Early-Onset PD

GBA Variants

LRRK2 Variants

SNCA Variants

Fluid Biomarkers in Early PD

Neurofilament Light Chain (NfL)

Phosphorylated Alpha-Synuclein (pSer129)

Alpha-Synuclein Seed Amplification Assays (αSyn-SAA)

Emerging Fluid Biomarkers

Clinical Progression Markers

MDS Prodromal Criteria

Progression Prediction Models

Early-Onset PD Characteristics

Session Highlights

Expected Presentations

Key Questions Addressed

Clinical Implications

For Clinicians

For Researchers

For Patients

Cross-References

Mechanisms

References

External Links

💬 Discussion

📗 Cite This Artifact

mds-2026-prodromal-early-onset-parkinson-biomarkers

MDS 2026 — Prodromal and Early-Onset Parkinson's Biomarkers

Overview

MDS 2026 — Prodromal and Early-Onset Parkinson's Biomarkers

Overview

REM Sleep Behavior Disorder as Prodromal Marker

Background

Key MDS 2026 Topics

Clinical Implications

Olfactory Dysfunction and DAT Imaging

Olfactory Testing

Dopamine Transporter Imaging

Combined Approach

Genetic Markers in Prodromal and Early-Onset PD

GBA Variants

LRRK2 Variants

SNCA Variants

Fluid Biomarkers in Early PD

Neurofilament Light Chain (NfL)

Phosphorylated Alpha-Synuclein (pSer129)

Alpha-Synuclein Seed Amplification Assays (αSyn-SAA)

Emerging Fluid Biomarkers

Clinical Progression Markers

MDS Prodromal Criteria

Progression Prediction Models

Early-Onset PD Characteristics

Session Highlights

Expected Presentations

Key Questions Addressed

Clinical Implications

For Clinicians

For Researchers

For Patients

Cross-References

Related Pages

Mechanisms

References

External Links

💬 Discussion