| name | clinvar |
| description | Build and inspect ClinVar exact-match evidence and candidate inventories.
Use for clinical labels, VUS/conflict, carrier context, and drug-response rows.
|
| tools | ["genomi.check_libraries","clinvar.match_variants","clinvar.scan_candidates","variant.gather_allele_context","variant.gather_gene_context"] |
| mutating | true |
ClinVar Evidence
Use this skill when the user asks about clinical labels, carrier findings,
pathogenic/likely pathogenic entries, VUS, conflicting classifications, drug
response, risk-factor labels, or ClinVar-derived discovery.
Goal
Build a candidate landscape from exact ClinVar matches. Use
candidate_inventory as variant-level provenance evidence and
candidate_review_groups as the carrier/condition review inventory.
Convention: See skills/conventions/evidence-quality.md.
Contract
- ClinVar matches provide exact/static evidence for source-backed
interpretation.
- Exact matching requires the optional build-specific library
clinvar-grch38 or clinvar-grch37.
- Candidate inventories are variant-level evidence, not interpretation.
- Candidate review groups are review targets. A heterozygous P/LP group can be
carrier-relevance evidence; it is not a carrier-status conclusion.
clinvar.scan_candidates returns an evidence view, grouped support,
warnings, and coverage; use those fields rather than inferring priority from
prose.
- By default,
clinvar.scan_candidates includes P/LP, conflicting, VUS,
risk/association/protective, drug-response, and benign ClinVar groups.
- If ClinVar matches are missing,
clinvar.scan_candidates materializes them
from the Active Genome Index before building the candidate inventory.
- VUS, conflicts, and low-review assertions are downgraded unless reviewed
source evidence supports a stronger claim.
- Drug-response rows use pharmacogenomic source context before actionability is
implied.
Cross-Capability Synthesis
A scope-limited result from this capability is not a final user-facing answer
when other Genomi capabilities can contribute orthogonal evidence to the same
question. Returning "cannot answer" while applicable capabilities remain
unexamined is a host-agent failure mode.
Tools
clinvar.match_variants
Materialize exact ClinVar matches for comparable Active Genome Index variants using the installed build-specific ClinVar library.
Use when: After an Active Genome Index and the matching build-specific ClinVar library are available to materialize exact ClinVar/sample matches.
Why necessary: ClinVar matching is library-scoped materialization; it turns installed public ClinVar rows into exact matches for an Active Genome Index without forcing every genome-artifact task to run ClinVar.
clinvar.scan_candidates
Build a deterministic candidate inventory and candidate review groups from exact ClinVar matches, materializing those matches from the Active Genome Index when needed.
Use when: Broad Active Genome Index disease or risk triage when exact ClinVar candidate inventory is needed.
Why necessary: Broad disease triage needs bounded ClinVar variant provenance plus review groups instead of ad hoc spot checks over a large genome file. It performs missing match materialization internally before candidate scanning.
Interpretation Rules
- Pathogenic/likely pathogenic labels need zygosity, inheritance, population
frequency, gene-disease context, and source quality.
- Carrier language belongs in
phenotype.plan_risk_investigation with
investigation_type:"carrier_review" after reviewing the group gates.
- VUS and conflicting labels use uncertainty/conflict wording.
- Drug-response labels require pharmacogenomic guideline context before clinical
actionability is implied.
- Common association/risk/protective labels usually provide limited context for
personal common-disease risk.
Routing Checks
- Prioritize ClinVar matches by actionability, review status, uncertainty,
population context, inheritance, and zygosity.
- If a ClinVar operation returns
status="requires_library_install", explain how
the named library helps this request and ask before installing it.
- Treat ClinVar condition strings as database labels that need interpretation.
- Keep the whole candidate inventory local; send selected public targets to
Journal source-review memory.