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neurodegenerative-biomarker-correlation-matrix
Overview
The Neurodegenerative Biomarker Correlation Matrix provides a comprehensive comparison of cerebrospinal fluid (CSF) and blood-based biomarkers across major neurodegenerative diseases. This matrix enables clinicians and researchers to understand biomarker patterns for differential diagnosis and disease progression monitoring.
Overview
The Neurodegenerative Biomarker Correlation Matrix provides a comprehensive comparison of cerebrospinal fluid (CSF) and blood-based biomarkers across major neurodegenerative diseases. This matrix enables clinicians and researchers to understand biomarker patterns for differential diagnosis and disease progression monitoring.
This page synthesizes evidence from the latest biomarker studies across Alzheimer's disease (AD), Parkinson's disease (PD), Dementia with Lewy Bodies (DLB), Multiple System Atrophy (MSA), Frontotemporal Dementia (FTD), and Amyotrophic Lateral Sclerosis (ALS)[@blennow2024][@hansson2024].
Biomarker Summary Table
Key: Biomarker Level
| Symbol | Meaning |
|--------|---------|
| ↑↑ | Strongly elevated |
| ↑ | Moderately elevated |
| ↔ | Normal |
| ↓ | Moderately decreased |
| ↓↓ | Strongly decreased |
CSF Biomarker Matrix
| Biomarker | AD | PD | DLB | MSA | FTD | ALS |
|-----------|-----|------|------|------|------|------|
| [p-tau181](/biomarkers/p-tau181) | ↑↑ | ↔ | ↔/↑ | ↔ | ↔ | ↔ |
| [p-tau217](/biomarkers/p-tau217) | ↑↑ | ↔ | ↔/↑ | ↔ | ↔ | ↔ |
| [NfL](/biomarkers/neurofilament-light-chain) | ↑ | ↔/↑ | ↑ | ↑↑ | ↑/↑↑ | ↑↑↑ |
| [Alpha-synuclein](/biomarkers/alpha-synuclein) | ↓ | ↓↓ | ↓↓ | ↓↓ | ↔ | ↔ |
| [TDP-43](/biomarkers/tdp-43) | ↔ | ↔ | ↔ | ↔ | ↑ | ↑↑ |
| [GFAP](/biomarkers/gfap-glial-fibrillary-acidic-protein) | ↑ | ↔ | ↔/↑ | ↔/↑ | ↔/↑ | ↑ |
Blood (Plasma/Serum) Biomarker Matrix
| Biomarker | AD | PD | DLB | MSA | FTD | ALS |
|-----------|-----|------|------|------|------|------|
| p-tau181 | ↑↑ | ↔ | ↔ | ↔ | ↔ | ↔ |
| p-tau217 | ↑↑ | ↔ | ↔ | ↔ | ↔ | ↔ |
| NfL | ↑ | ↔/↑ | ↑ | ↑↑ | ↑ | ↑↑↑ |
| Alpha-synuclein | ↔ | ↓/↔ | ↓/↔ | ↓ | ↔ | ↔ |
| TDP-43 | ↔ | ↔ | ↔ | ↔ | ↑ | ↑ |
| GFAP | ↑↑ | ↔ | ↔/↑ | ↔ | ↔/↑ | ↑ |
Diagnostic Utility by Biomarker
Phosphorylated Tau (p-tau181)
Best for: Distinguishing AD from other neurodegenerative diseases
| Metric | AD vs. Controls | AD vs. FTD | AD vs. PD |
|--------|-----------------|------------|-----------|
| Sensitivity | 85-90% | 85% | 90% |
| Specificity | 85-90% | 80% | 88% |
| AUC | 0.92-0.95 | 0.88 | 0.93 |
- AD: Strongly elevated in CSF and plasma
- PD/DLB/MSA: Typically normal or only mildly elevated
- FTD/ALS: Normal[@thijssen2024]
Phosphorylated Tau (p-tau217)
Best for: Highest accuracy for AD across the cognitive continuum
| Metric | AD vs. Controls | AD vs. FTD | AD vs. DLB |
|--------|-----------------|------------|-----------|
| Sensitivity | 88-92% | 90% | 88% |
| Specificity | 88-92% | 85% | 82% |
| AUC | 0.94-0.97 | 0.91 | 0.88 |
- AD: Strongly elevated; detects earliest preclinical changes
- PD/DLB/MSA: Typically normal
- FTD/ALS: Normal[@pichetit2024]
Neurofilament Light Chain (NfL)
Best for: General neurodegeneration marker, prognostic utility
| Metric | ALS vs. Controls | ALS vs. FTD | PD vs. MSA |
|--------|------------------|-------------|------------|
| Sensitivity | 90-95% | 85% | 75% |
| Specificity | 90-95% | 80% | 82% |
| AUC | 0.96-0.98 | 0.88 | 0.82 |
- ALS: Strongly elevated (highest levels of all diseases)
- MSA: Markedly elevated (distinguishes from PD)
- FTD: Elevated, correlates with disease severity
- AD/PD: Moderately elevated; prognostic for cognitive decline[@kaufmann2024]
Alpha-Synuclein
Best for: Detecting synucleinopathies (PD, DLB, MSA)
| Metric | PD vs. Controls | DLB vs. AD | MSA vs. PD |
|--------|-----------------|------------|------------|
| Sensitivity (RT-QuIC) | 88-95% | 75% | 80% |
| Specificity (RT-QuIC) | 90-95% | 82% | 78% |
| AUC | 0.92 | 0.80 | 0.81 |
- PD: Decreased total α-syn; RT-QuIC positive in 88-95%
- DLB: Decreased total α-syn; RT-QuIC positive in 75-85%
- MSA: Decreased total α-syn; RT-QuIC positive in 80-90%
- AD/FTD/ALS: Typically normal[@oroza2024]
TDP-43
Best for: Detecting TDP-43 proteinopathies (ALS, FTD)
| Metric | ALS vs. Controls | FTD vs. AD | ALS-FTD vs. PD |
|--------|------------------|------------|----------------|
| Sensitivity | 70-80% | 75% | 78% |
| Specificity | 80-85% | 78% | 82% |
| AUC | 0.82 | 0.80 | 0.84 |
- ALS: Elevated in CSF (detects pathological burden)
- FTD: Elevated, especially in ALS-FTD spectrum
- PD/DLB/MSA/AD: Typically normal[@leotti2024]
Glial Fibrillary Acidic Protein (GFAP)
Best for: Astrocyte activation, AD-specific elevation in blood
| Metric | AD vs. Controls | AD vs. FTD | AD vs. PD |
|--------|-----------------|------------|-----------|
| Sensitivity | 80-85% | 78% | 85% |
| Specificity | 82-88% | 75% | 88% |
| AUC | 0.88-0.92 | 0.82 | 0.90 |
- AD: Elevated in both CSF and plasma; blood shows strongest signal
- PD/DLB: Normal or mildly elevated
- ALS: Elevated (neuroinflammation marker)
- FTD/MSA: Variable[@garton2024]
Disease-Specific Biomarker Profiles
Alzheimer's Disease (AD)
Core biomarker signature: ↓ Aβ42/Aβ40 + ↑↑ p-tau181/217 + ↑ NfL + ↑ GFAP
| Biomarker | CSF | Blood | Clinical Utility |
|-----------|-----|-------|------------------|
| Aβ42/Aβ40 | ↓↓ | ↓ | Amyloid pathology detection |
| p-tau181 | ↑↑ | ↑↑ | Core diagnostic marker |
| p-tau217 | ↑↑ | ↑↑ | Highest accuracy |
| NfL | ↑ | ↑ | Disease progression |
| GFAP | ↑ | ↑↑ | Astrocyte activation |
Parkinson's Disease (PD)
Core biomarker signature: ↓ total α-syn + RT-QuIC positive + normal tau
| Biomarker | CSF | Blood | Clinical Utility |
|-----------|-----|-------|------------------|
| Total α-syn | ↓↓ | ↓/↔ | Synuclein pathology |
| p-Ser129 α-syn | ↑ | ↑ | Pathology burden |
| NfL | ↔/↑ | ↔/↑ | Cognitive decline risk |
| RT-QuIC | + (88-95%) | N/A | Disease confirmation |
Dementia with Lewy Bodies (DLB)
Core biomarker signature: ↓ α-syn + normal tau + ↑ NfL
| Biomarker | CSF | Blood | Clinical Utility |
|-----------|-----|-------|------------------|
| Total α-syn | ↓↓ | ↓/↔ | Synuclein pathology |
| p-tau181 | ↔/↑ | ↔ | AD comorbidity |
| NfL | ↑ | ↑ | Disease severity |
| RT-QuIC | + (75-85%) | N/A | DLB confirmation |
Multiple System Atrophy (MSA)
Core biomarker signature: ↓ α-syn + ↑↑ NfL + normal tau
| Biomarker | CSF | Blood | Clinical Utility |
|-----------|-----|-------|------------------|
| Total α-syn | ↓↓ | ↓ | Synuclein pathology |
| NfL | ↑↑ | ↑↑ | Distinguish from PD |
| p-tau | ↔ | ↔ | Rule out AD |
| RT-QuIC | + (80-90%) | N/A | MSA confirmation |
Frontotemporal Dementia (FTD)
Core biomarker signature: ↑ NfL + normal AD biomarkers + ↑ TDP-43
| Biomarker | CSF | Blood | Clinical Utility |
|-----------|-----|-------|------------------|
| NfL | ↑/↑↑ | ↑ | Disease severity |
| p-tau | ↔ | ↔ | Rule out AD |
| TDP-43 | ↑ | ↑ | FTD-FUS/ALS-FTD |
| Progranulin | ↓ (genetic) | ↓ (genetic) | Genetic subtype |
Amyotrophic Lateral Sclerosis (ALS)
Core biomarker signature: ↑↑ NfL + ↑ TDP-43 + normal tau
| Biomarker | CSF | Blood | Clinical Utility |
|-----------|-----|-------|------------------|
| NfL | ↑↑↑ | ↑↑↑ | Diagnostic + prognostic |
| pNfH | ↑↑ | ↑↑ | Disease progression |
| TDP-43 | ↑↑ | ↑ | Pathology burden |
| p-tau | ↔ | ↔ | Rule out AD |
Cross-Disease Differential Diagnostic Panels
AD vs. FTD vs. ALS
| Panel | AD | FTD | ALS |
|-------|-----|------|-----|
| p-tau181 | ↑↑ | ↔ | ↔ |
| p-tau217 | ↑↑ | ↔ | ↔ |
| NfL | ↑ | ↑/↑↑ | ↑↑↑ |
| TDP-43 | ↔ | ↑ | ↑↑ |
Algorithm: If p-tau elevated → AD. If NfL very high with TDP-43 → ALS. If NfL elevated with normal p-tau and TDP-43 → FTD.
PD vs. DLB vs. MSA
| Panel | PD | DLB | MSA |
|-------|-----|------|------|
| α-syn (total) | ↓↓ | ↓↓ | ↓↓ |
| NfL | ↔/↑ | ↑ | ↑↑ |
| RT-QuIC | + | + | + |
| p-tau | ↔ | ↔/↑ | ↔ |
Algorithm: If NfL very high → MSA. If NfL moderately elevated with cognitive fluctuations → DLB. If NfL normal/mildly elevated → PD.
AD vs. DLB vs. PD
| Panel | AD | DLB | PD |
|-------|-----|------|------|
| p-tau181/217 | ↑↑ | ↔/↑ | ↔ |
| α-syn | ↓ | ↓↓ | ↓↓ |
| NfL | ↑ | ↑ | ↔/↑ |
| GFAP | ↑↑ | ↔/↑ | ↔ |
Clinical Applications
Diagnostic Algorithm
- If elevated → Consider AD or AD comorbidity
- If normal → Proceed to Step 2
- If positive → Synucleinopathy (PD/DLB/MSA)
- If negative → Proceed to Step 3
- If NfL very high + TDP-43 elevated → ALS or ALS-FTD
- If NfL elevated with normal p-tau → FTD
Prognostic Biomarkers
- NfL: Strongest prognostic marker across all diseases; higher = faster progression
- p-tau: Correlates with cognitive decline rate in AD
- Neurogranin: Predicts cognitive progression in AD
Therapeutic Monitoring
- NfL: Used as outcome biomarker in ALS and AD clinical trials
- p-tau: Reduced by anti-amyloid therapies (lecanemab, donanemab)
- GFAP: May track astrocyte-related treatment effects
Limitations and Considerations
Assay Variability
- Different platforms (Simoa, Lumipulse, Elecsys) have different cutoffs
- Cross-platform standardization ongoing
Disease Overlap
- Biomarkers elevated in multiple conditions (NfL, GFAP)
- AD comorbidity common in FTD, DLB, PD
Sample Type
- Blood less invasive but sometimes less sensitive than CSF
- Pre-analytical factors (hemolysis, fasting) affect blood biomarkers
Dynamic Range
- NfL has broad range (useful for ALS, less for early PD)
- p-tau shows ceiling effects in advanced AD
Related Pages
- [CSF Biomarker Comparison](/biomarkers/csf-biomarker-comparison)
- [Blood-Based Biomarkers](/biomarkers/blood-based-biomarkers-neurodegeneration)
- [p-Tau181](/biomarkers/p-tau181)
- [p-Tau217](/biomarkers/p-tau217)
- [Neurofilament Light Chain](/biomarkers/neurofilament-light-chain)
- [Alpha-Synuclein](/biomarkers/alpha-synuclein)
- [TDP-43](/biomarkers/tdp-43)
- [GFAP](/biomarkers/gfap-glial-fibrillary-acidic-protein)
- [Alzheimer's Disease Biomarkers](/biomarkers/alzheimers-biomarkers)
- [Parkinson's Disease Biomarkers](/biomarkers/parkinsons-disease-biomarkers)
- [DLB Biomarkers](/biomarkers/dementia-lewy-bodies-biomarkers)
- [MSA Biomarkers](/biomarkers/multiple-system-atrophy-biomarkers)
References
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