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tooluniverse gwas snp interpretation - Claude MCP Skill
GWAS SNP Interpretation Skill
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SKILL.md# GWAS SNP Interpretation Skill
## Overview
Interpret genetic variants (SNPs) from GWAS studies by aggregating evidence from multiple sources to provide comprehensive clinical and biological context.
**Use Cases:**
- "Interpret rs7903146" (TCF7L2 diabetes variant)
- "What diseases is rs429358 associated with?" (APOE Alzheimer's variant)
- "Clinical significance of rs1801133" (MTHFR variant)
- "Is rs12913832 in any fine-mapped loci?" (Eye color variant)
## What It Does
The skill provides a comprehensive interpretation of SNPs by:
1. **SNP Annotation**: Retrieves basic variant information including genomic coordinates, alleles, functional consequence, and mapped genes
2. **Association Discovery**: Finds all GWAS trait/disease associations with statistical significance
3. **Fine-Mapping Evidence**: Identifies credible sets the variant belongs to (fine-mapped causal loci)
4. **Gene Mapping**: Uses Locus-to-Gene (L2G) predictions to identify likely causal genes
5. **Clinical Summary**: Aggregates evidence into actionable clinical significance
## Workflow
```
User Input: rs7903146
↓
[1] SNP Lookup
→ Get location, consequence, MAF
→ gwas_get_snp_by_id
↓
[2] Association Search
→ Find all trait/disease associations
→ gwas_get_associations_for_snp
↓
[3] Fine-Mapping (Optional)
→ Get credible set membership
→ OpenTargets_get_variant_credible_sets
↓
[4] Gene Predictions
→ Extract L2G scores for causal genes
→ (embedded in credible sets)
↓
[5] Clinical Summary
→ Aggregate evidence
→ Identify key traits and genes
↓
Output: Comprehensive Interpretation Report
```
## Data Sources
### GWAS Catalog (EMBL-EBI)
- **SNP annotations**: Functional consequences, mapped genes, population frequencies
- **Associations**: P-values, effect sizes, study metadata
- **Coverage**: 350,000+ publications, 670,000+ associations
### Open Targets Genetics
- **Fine-mapping**: Statistical credible sets from SuSiE, FINEMAP methods
- **L2G predictions**: Machine learning-based gene prioritization
- **Colocalization**: QTL evidence for causal genes
- **Coverage**: UK Biobank, FinnGen, and other large cohorts
## Input Parameters
### Required
- `rs_id` (str): dbSNP rs identifier
- Format: "rs" + number (e.g., "rs7903146")
- Must be valid rsID in GWAS Catalog
### Optional
- `include_credible_sets` (bool, default=True): Query fine-mapping data
- True: Complete interpretation (slower, ~10-30s)
- False: Fast associations only (~2-5s)
- `p_threshold` (float, default=5e-8): Genome-wide significance threshold
- `max_associations` (int, default=100): Maximum associations to retrieve
## Output Format
Returns `SNPInterpretationReport` containing:
### 1. SNP Basic Info
```python
{
'rs_id': 'rs7903146',
'chromosome': '10',
'position': 112998590,
'ref_allele': 'C',
'alt_allele': 'T',
'consequence': 'intron_variant',
'mapped_genes': ['TCF7L2'],
'maf': 0.293
}
```
### 2. Trait Associations
```python
[
{
'trait': 'Type 2 diabetes',
'p_value': 1.2e-128,
'beta': '0.28 unit increase',
'study_id': 'GCST010555',
'pubmed_id': '33536258',
'effect_allele': 'T'
},
...
]
```
### 3. Credible Sets (Fine-Mapping)
```python
[
{
'study_id': 'GCST90476118',
'trait': 'Renal failure',
'finemapping_method': 'SuSiE-inf',
'p_value': 3.5e-42,
'predicted_genes': [
{'gene': 'TCF7L2', 'score': 0.863}
],
'region': '10:112950000-113050000'
},
...
]
```
### 4. Clinical Significance
```
Genome-wide significant associations with 100 traits/diseases:
- Type 2 diabetes
- Diabetic retinopathy
- HbA1c levels
...
Identified in 20 fine-mapped loci.
Predicted causal genes: TCF7L2
```
## Example Usage
See `QUICK_START.md` for platform-specific examples.
## Tools Used
### GWAS Catalog Tools
1. `gwas_get_snp_by_id`: Get SNP annotation
2. `gwas_get_associations_for_snp`: Get all trait associations
### Open Targets Tools
3. `OpenTargets_get_variant_info`: Get variant details with population frequencies
4. `OpenTargets_get_variant_credible_sets`: Get fine-mapping credible sets with L2G
## Interpretation Guide
### P-value Significance Levels
- **p < 5e-8**: Genome-wide significant (strong evidence)
- **p < 5e-6**: Suggestive (moderate evidence)
- **p < 0.05**: Nominal (weak evidence)
### L2G Score Interpretation
- **> 0.5**: High confidence causal gene
- **0.1-0.5**: Moderate confidence
- **< 0.1**: Low confidence
### Clinical Actionability
1. **High**: Multiple genome-wide significant associations + in credible sets + high L2G scores
2. **Moderate**: Genome-wide significant associations but limited fine-mapping
3. **Low**: Suggestive associations or limited replication
## Limitations
1. **Variant ID Conversion**: OpenTargets requires chr_pos_ref_alt format, which may need allele lookup
2. **Population Specificity**: Associations may vary by ancestry
3. **Effect Sizes**: Beta values are study-dependent (different phenotype scales)
4. **Causality**: Associations don't prove causation; fine-mapping improves confidence
5. **Currency**: Data reflects published GWAS; latest studies may not be included
## Best Practices
1. **Use Full Interpretation**: Enable `include_credible_sets=True` for clinical decisions
2. **Check Multiple Variants**: Look at other variants in the same locus
3. **Validate Populations**: Consider ancestry-specific effect sizes
4. **Review Publications**: Check original studies for context
5. **Integrate Evidence**: Combine with functional data, eQTLs, pQTLs
## Technical Notes
### Performance
- **Fast mode** (no credible sets): 2-5 seconds
- **Full mode** (with credible sets): 10-30 seconds
- **Bottleneck**: OpenTargets GraphQL API rate limits
### Error Handling
- Invalid rs_id: Returns error message
- No associations: Returns empty list with note
- API failures: Graceful degradation (returns partial results)
## Related Skills
- **Gene Function Analysis**: Interpret predicted causal genes
- **Disease Ontology Lookup**: Understand trait classifications
- **PubMed Literature Search**: Find original GWAS publications
- **Variant Effect Prediction**: Functional consequence analysis
## References
1. GWAS Catalog: https://www.ebi.ac.uk/gwas/
2. Open Targets Genetics: https://genetics.opentargets.org/
3. GWAS Significance Thresholds: Fadista et al. 2016
4. L2G Method: Mountjoy et al. 2021 (Nature Genetics)
## Version
- **Version**: 1.0.0
- **Last Updated**: 2026-02-13
- **ToolUniverse Version**: >= 1.0.0
- **Tools Required**: gwas_get_snp_by_id, gwas_get_associations_for_snp, OpenTargets_get_variant_credible_setsSignals
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Information
- Repository
- mims-harvard/ToolUniverse
- Author
- mims-harvard
- Last Sync
- 2/20/2026
- Repo Updated
- 2/20/2026
- Created
- 2/19/2026
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