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Multi-Analyte Biomarker Panel for Parkinson's Disease Diagnosis and Progression

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Comprehensive multi-analyte biomarker panels represent a significant advancement in Parkinson's disease (PD) diagnostics, enabling earlier diagnosis, improved differential diagnosis from other parkinsonisms, and better progression prediction. Unlike single-marker approaches, multi-marker panels capture the heterogeneous pathology of PD and related synucleinopathies.

Core Panel Components

Alpha-Synuclein Seed Amplification (SAA)

The cornerstone of PD biomarker panels is detection of pathological alpha-synuclein through seed amplification:

| SAA Type | Sample | Sensitivity | Specificity | Clinical Use |
|----------|--------|-------------|-------------|--------------|
| RT-QuIC | CSF | 88-95% | 90-98% | PD diagnosis |
| PMCA | CSF | 90-97% | 88-95% | PD diagnosis |
| Blood-based SAA | Blood | 75-85% | 85-92% | Screening |
| Skin biopsy SAA | Skin | 90-95% | 92-98% | Confirmatory |

Key advantages: SAA can detect prodromal PD in REM sleep behavior disorder (RBD) patients with 80-90% conversion prediction over 5 years.

Neurodegeneration Markers

| Biomarker | Sample | Utility | Key Findings |
|-----------|--------|---------|---------------|
| NfL | CSF, Plasma | Progression | Higher levels correlate with faster decline |
| NfL | Saliva | Screening | Non-invasive alternative |
| p-NFH | CSF, Plasma | Axonal injury | Complement to NfL |

Evidence: Baseline NfL predicts motor and cognitive progression. Patients with high NfL decline 2-3x faster than those with low NfL.

Metabolic Biomarkers

Metabolic dysfunction is central to PD pathogenesis:

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