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Progranulin (PGRN) - Biomarker
Progranulin (PGRN) - Biomarker
Pathway Diagram
Progranulin (PGRN) - Biomarker
Pathway Diagram
| Property | Value | [@ghidoni2022]
|----------|-------| [@baker2021]
| Category | Protein Biomarker / Therapeutic Target | [@van2021]
| Target | Progranulin protein (granulin peptides) | [@ward2020]
| Sample Type | CSF, plasma, serum | [@ahmed2020]
| Diseases | Frontotemporal Dementia, ALS, Alzheimer's Disease, Parkinson's Disease | [@sellnow2019]
| Clinical Use | Diagnosis, disease progression, treatment monitoring | [@petkau2018]
Overview
Progranulin (PGRN) is a secreted growth factor-like protein that plays important roles in neuronal survival, synaptic function, and inflammation. It is encoded by the GRN gene and is particularly important in frontotemporal dementia (FTD) where GRN mutations cause haploinsufficiency. Both the protein itself and its cleaved fragments (granulins) serve as biomarkers and therapeutic targets.
Molecular Characteristics
Gene and Protein
- Gene: GRN (Progranulin) located on chromosome 17q21.31
- Protein: Progranulin, 593 amino acids (~63 kDa)
- Structure: Contains 7.5 tandem granulin repeats
- Cleavage: Secreted as full-length protein, cleaved by proteases (elastase, MMP-9)
Normal Function
- Neuronal survival: Neurotrophic factor for neurons
- Synaptic plasticity: Regulates glutamatergic transmission
- Inflammation: Modulates microglial activation
- Wound healing: Growth factor activity
- Lysosomal function: Critical for autophagosome-lysosome fusion
Biomarker Detection Methods
ELISA
- Commercial kits available (R&D Systems, Adipogen)
- Measures total progranulin (full-length + fragments)
- Plasma: 20-50 ng/mL in healthy controls
- CSF: 1-5 ng/mL (lower than plasma)
Simoa
- Ultra-sensitive for low CSF concentrations
- Can detect early changes in pre-symptomatic carriers
Genetic Testing
- GRN mutations: Haploinsufficiency causes FTD
- C9orf72: Can be comorbid with GRN mutations
- Predictive testing: Identifies at-risk individuals
Clinical Applications
Frontotemporal Dementia (FTD)
- GRN mutation carriers: 50% reduction in plasma progranulin
- Diagnostic utility: Helps distinguish from Alzheimer's disease
- Disease progression: Levels correlate with clinical decline
- Pre-symptomatic: Changes detectable years before onset
ALS (Amyotrophic Lateral Sclerosis)
- Reduced progranulin in some ALS patients
- May correlate with disease severity
- Therapeutic target for enhancement
Alzheimer's Disease
- Variable results in AD patients
- May be elevated in some subtypes
- Ongoing research for biomarker utility
Parkinson's Disease
- Some studies show altered levels
- May reflect neuroinflammation
Diagnostic Performance
Frontotemporal Dementia
| Metric | GRN(+) FTD vs Controls | GRN(+) vs GRN(-) FTD |
|--------|---------------------|---------------------|
| Sensitivity | 75-85% | 80-90% |
| Specificity | 85-95% | 70-80% |
| AUC | 0.82-0.90 | 0.78-0.86 |
Disease Severity Correlation
- Progranulin levels inversely correlate with disease severity in FTD
- Faster progression in carriers with lowest levels
- Levels predict age of onset within mutation carriers
Comparison with Other Biomarkers
| Biomarker | FTD Utility | Specimen | AUC |
|----------|-------------|----------|-----|
| Progranulin | Primary | Plasma/CSF | 0.82-0.90 |
| NfL | Secondary | CSF/Plasma | 0.85-0.92 |
| p-Tau181 | Differential | CSF | 0.75-0.85 |
| TDP-43 | Pathology | CSF | 0.78-0.88 |
Asian Population Studies
Japanese Cohorts
- J-ADNI and Japanese FTD registries show similar progranulin reductions in GRN carriers
- Plasma progranulin cutoffs: <20 ng/mL for Japanese populations
- Specific reference ranges established for Asian populations
Korean Studies
- Korean FTD patients show comparable patterns
- GRN mutation frequency similar to Western populations
- Ongoing studies in Korean clinical centers
Chinese Studies
- Chinese Alzheimer's Association and CANDI cohort data available
- Population-specific reference ranges under development
- Cross-ethnic validity studies ongoing
Biomarker Panels with Progranulin
Recommended Panel for FTD Differential Diagnosis
| Biomarker | Specimen | Utility |
|----------|---------|----------|----------|
| Progranulin | Plasma | Primary - identifies GRN carriers |
| NfL | Plasma/CSF | Disease burden |
| p-Tau181 | CSF | AD differential |
| TDP-43 | CSF |pathology marker |
Multi-Analyte Performance
- Combined panel (progranulin + NfL): AUC 0.88-0.93
- Adds predictive value for disease progression
- Helps distinguish FTD subtypes
Regulatory Status
United States
- FDA: No FDA-cleared progranulin assay currently
- Laboratory-developed tests (LDTs) available in specialized labs
- CMS coverage: Limited to research use
Europe
- CE-IVD标记: No CE-cleared progranulin assay
- Available in specialized European reference labs
- IVDR compliance in progress for new assays
Asia
- PMDA (Japan): No approved assay
- NMPA (China): Under development
- KFDA (Korea): Research use only
Cost Analysis
| Test Type | Cost Range | Turnaround |
|----------|----------|------------|
| Plasma ELISA | $50-100 | 1-3 days |
| Simoa (ultrasensitive) | $150-250 | 3-5 days |
| CSF ELISA | $75-125 | 1-3 days |
| Genetic testing | $300-500 | 2-4 weeks |
| Full biomarker panel | $400-800 | 5-7 days |
Cost-Effectiveness
- Progranulin testing cost-effective for FTD families
- Enables predictive testing in at-risk individuals
- Guides therapeutic decisions
Pre-Analytical Considerations
Sample Collection
- Plasma: EDTA tube, centrifuge within 1 hour
- CSF: LP procedure, store at -80°C
- Fasting state may affect levels
Factors Affecting Levels
- Age: Slight decrease with age
- Sex: No significant differences
- Kidney function: May affect clearance
- Inflammation: Acute changes
Stability
- Plasma: 24 hours at room temperature
- CSF: 1 week at 4°C,长期存储 at -80°C
- Freeze-thaw: Up to 3 cycles acceptable
Disease-Specific Mechanisms
Frontotemporal Dementia with GRN Mutations
ALS
- Progranulin may be neuroprotective
- Some mutations associated with ALS-FTD spectrum
- Levels may reflect disease activity
Therapeutic Implications
Recombinant Progranulin
- AAV-mediated delivery in development
- Recombinant protein therapy
- Small molecule enhancers
Gene Therapy
- AAV vectors for GRN delivery
- CRISPR-based approaches
- Antisense oligonucleotides
Small Molecule Enhancers
- Arimoclomol: Heat shock protein co-inducer (in trials)
- Autophagy enhancers: Increase endogenous PGRN
- Proteostasis modulators: Improve folding/secretion
Background
The study of Progranulin (Pgrn) Biomarker has evolved significantly over the past decades. Research in this area has revealed important insights into the underlying mechanisms of neurodegeneration and continues to drive therapeutic development.
Historical context and key discoveries in this field have shaped our current understanding and will continue to guide future research directions.
Cross-References
- GRN Gene
- [Frontotemporal Dementia](/diseases/frontotemporal-dementia)
- TDP-43 Biomarkers
- ALS Biomarkers
- TREM2 Signaling
Limitations
Allen Brain Atlas Resources
- [Allen Brain Atlas - Gene Expression](https://human.brain-map.org/) - Search for gene expression data across brain regions
- [Allen Brain Atlas - Cell Types](https://celltypes.brain-map.org/) - Explore neuronal cell type taxonomy
External Links
- [Michael J. Fox Foundation - Alpha-Synuclein Research](https://www.michaeljfox.org/)
- [Parkinson's Foundation Biomarker Initiative](https://www.parkinson.org/)
- [NIH - Alpha-Synuclein Biomarkers](https://www.ninds.nih.gov/)
References
Pathway Diagram
The following diagram shows the key molecular relationships involving Progranulin (PGRN) - Biomarker discovered through SciDEX knowledge graph analysis:
▸Metadataorigin_type: v1_polymorphic_backfill
| slug | biomarkers-progranulin |
| kg_node_id | PROGRANULIN |
| entity_type | biomarker |
| origin_type | v1_polymorphic_backfill |
| source_table | wiki_pages |
| wiki_page_id | wp-34d3b3b21f29 |
| __merged_from | {'merged_at': '2026-05-13', 'unprefixed_id': 'biomarkers-progranulin'} |
| _schema_version | 1 |
No provenance edges found
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