CADD (Combined Annotation Dependent Depletion)
Integrates 60+ genomic features into a single deleteriousness score. Scores ALL possible SNVs and small indels in the human genome, not just missense.
What It Does
- Scores all variant types: missense, synonymous, intronic, intergenic, UTR, splice
- PHRED-scaled score: 10 = top 10%, 20 = top 1%, 30 = top 0.1%
- Integrates: conservation, regulatory, protein impact, splice predictions
- Pre-computed for all possible SNVs in GRCh37/GRCh38
How to Use
Web
- Go to https://cadd.gs.washington.edu/
- Score tab → paste variant(s) in VCF format
- Or lookup pre-computed: https://cadd.gs.washington.edu/snv
API
# Score single variant (GRCh38)
curl "https://cadd.gs.washington.edu/api/v1.0/GRCh38/15:43600551:A:C"Pre-computed Download
# Whole genome (350GB!)
# Or per-chromosome
tabix whole_genome_SNVs.tsv.gz 15:43600551-43600551Verified Status
VERIFIED — STRC E1659A CADD PHRED score: 27.5 (raw: 4.931). Top 0.18% most deleterious variants genome-wide. Obtained via Ensembl VEP (direct CADD API returns ‘Not found’ for this position). SIFT: Deleterious (0), PolyPhen: Probably damaging (0.991).
STRC Research Usage
- STRC E1659A Conservation and Reclassification — additional computational evidence
- PHRED 27.5 = strong deleteriousness signal (>20 is commonly used pathogenicity threshold)
- Accessed via:
curl 'https://rest.ensembl.org/vep/human/region/15:43600551-43600551:1/C?CADD=1' -H 'Content-Type:application/json'
Connections
- REVEL [see-also] — missense-specific ensemble
- AlphaMissense [see-also] — DeepMind predictor
- SpliceAI [see-also] — splice-specific predictor
- STRC Variant c.4976A>C — Misha [see-also]