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prs
Apply published polygenic scores from PGS Catalog to approved local personal DNA and return raw weighted score plus overlap QC.
Codex または Claude でインストール この Prompt をコピーして Codex、Claude、または他のアシスタントに貼り付けると、Skill ページを確認してインストールできます。
メニュー
Apply published polygenic scores from PGS Catalog to approved local personal DNA and return raw weighted score plus overlap QC.
Codex または Claude でインストール この Prompt をコピーして Codex、Claude、または他のアシスタントに貼り付けると、Skill ページを確認してインストールできます。
SOC 職業分類に基づく
Use this skill for genetics, genome source, variant, gene, phenotype, disease, screen, pharmacogenomics, and Genomi install/setup maintenance questions.
Build and inspect ClinVar exact-match evidence and candidate inventories. Use for clinical labels, VUS/conflict, carrier context, and drug-response rows.
Activate this skill for "/genomi decode", "decode my genome", "decode my DNA", "show me the dashboard", "the Genomi dashboard", "one-shot rundown", or any all-at-once request that asks Genomi to compose every capability's findings into a single artifact. This is the whole-genome dashboard kicker — it sweeps every relevant Genomi capability in one shot, not a per-target lookup. Composes evidence from every relevant Genomi capability into a single self-contained Genomi Dashboard.html and returns localhost serve metadata. Active genome required.
Answer drug-response, medication, PharmGKB-style, PGxDB, ATC, DrugBank, gene-drug, and variant-drug questions using public PGx evidence plus local sample genotype support when an Active Genome Index is selected.
Plan rare disease, hereditary disease, cancer risk, carrier-relevance, and observed-condition source investigation from public targets or selected active genome evidence.
Answer specific rsID, allele, gene, region, genotype, and absence/callability questions using explicit session context or public evidence.
| name | prs |
| description | Apply published polygenic scores from PGS Catalog to approved local personal DNA and return raw weighted score plus overlap QC. |
| tools | ["prs.search_scores","prs.fetch_score_metadata","prs.list_imported_scores","prs.check_score_overlap","prs.calculate_score","prs.build_source_context"] |
Use this skill when the user asks about polygenic risk scores, PRS, PGS Catalog scores, common disease or trait risk from many variants, or applying a published scoring file to their genome.
GRCh38 when omitted; use GRCh37 only when the
Active Genome Index is GRCh37/hg19.score_mean and score_sd
are supplied for the same score, build, cohort/reference distribution, and
scoring convention.prs.search_scores for public trait or score discovery. If the user
already supplies a PGS ID, use that ID directly.prs.fetch_score_metadata when the source publication, build, variant
count, scoring-file URLs, licensing, or cohort/evaluation context matters.prs.calculate_score with the chosen pgs_id and the user's genome
source to get the raw weighted score plus overlap QC.prs.check_score_overlap when you only need readiness and QC without a
calculated score.prs.list_imported_scores when the user asks what scores are already
available locally.prs.build_source_context when the user asks what PRS can or cannot
tell them.PGS Catalog rarely publishes a reference cohort mean/SD, so a raw weighted score has units on an arbitrary scale. Deliver a defensible directional or quantitative answer for this specific question by combining capabilities that contribute orthogonal evidence — population allele frequencies feeding a closed-form z, direct effect-allele dosages at well-replicated lead loci, additional published scores derived by different methods, treatment-response context when the outcome is treatable, mechanism context from functional or pathway evidence, or whatever else Genomi currently exposes that fits. Disclose the assumptions of any closed-form estimate (HWE, variant independence, ancestry of the allele-frequency source).
When an Active Genome Index is scored or its overlap changes the result, report the score ID/source, genome build, overlap status, matched/missing/excluded variant counts, and whether the result is raw or calibrated. Do not add a routine Active Genome Index status line for public score metadata lookups.
Use careful language:
Directional language ("leans above population average", "in the upper tertile of the analytic z distribution") is appropriate when grounded in the orthogonal evidence the synthesis combined.
Avoid:
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.
Explain PGS Catalog provenance, local scoring workflow, genome-build defaults, calibration limits, and PRS risk boundaries.
Use when: The user asks what PRS can and cannot tell them, whether PRS means common risk analysis, or how Genomi applies published scores.
Why necessary: PRS answers require explicit boundaries around calibration, cohort portability, missing variants, and clinical non-diagnosis.
Not for: Calculating a personal score; use prs.calculate_score after Active Genome Index access approval.
Example prompts: Explain how Genomi implements PRS. Does PRS give common disease risk?
Result semantics: Returns public method context only; it does not read Active Genome Index.
Apply a published polygenic score to an approved Active Genome Index and return raw weighted score plus QC.
Use when: The user asks to calculate or apply a published PRS/PGS score to their genome.
Why necessary: This keeps Active Genome Index local, applies only selected published weights, reports overlap and build defaults, and avoids unsupported risk-category claims.
Not for: Training a new PRS model. Diagnosis, monogenic disease interpretation, medication response, or absolute-risk prediction without a validated calibration model. Ancestry or identity inference.
Example prompts: Calculate PGS000001 for my Active Genome Index. Apply this local scoring file to my GRCh38 genome.
Result semantics: Output is a raw weighted score and QC unless explicit calibration parameters are supplied. Do not phrase it as diagnosis, absolute disease risk, ethnicity, or clinical actionability.
Check how many variants from a polygenic score are usable in an approved Active Genome Index.
Use when: The agent needs PRS overlap/readiness before calculating or interpreting a published polygenic score.
Why necessary: A PRS score can be misleading with low variant overlap, build mismatch, unharmonized palindromic alleles, or missing genotype records.
Not for: Public score search; use prs.search_scores. Diagnosis or absolute risk classification.
Example prompts: Does my genome have enough overlap with PGS000001?
Result semantics: Reports overlap and calculation readiness only; missing score variants are not negative evidence for disease risk.
Fetch detailed public PGS Catalog metadata for one score ID, including scoring-file URLs and source publication context.
Use when: The agent needs the exact PGS Catalog record context — trait, build, variant count, source publication, cohort, ancestry/evaluation, licensing — before explaining or applying a score.
Why necessary: The score metadata carries build, trait, source publication, cohort, ancestry/evaluation, and licensing context that determines whether applying a score is appropriate.
Not for: Calculating a personal score; use prs.calculate_score with the chosen pgs_id.
Example prompts: Fetch metadata for PGS000001.
Result semantics: Returns public PGS Catalog metadata only and may report source_unavailable if the external source cannot be reached.
Import a PGS Catalog or local scoring file into Genomi's local PRS score cache for a declared genome build.
Use when: A score has been selected and needs to be materialized locally before overlap checking or scoring.
Why necessary: Private genotype scoring must run against local score artifacts rather than uploading genotypes to external services.
Not for: Reading Active Genome Index; import is public/local score materialization only. Interpreting the score as risk; use prs.calculate_score and preserve its limitations.
Example prompts: Import PGS000001 for GRCh38. Import this local scoring file for GRCh37.
Result semantics: Creates a local cache of variant weights and manifest metadata. The default genome_build is GRCh38 when omitted and is disclosed in defaults_applied.
List polygenic scores available locally for use without reading Active Genome Index.
Use when: The user asks which polygenic scores are available locally.
Why necessary: Knowing which scores are already available locally helps the agent pick a matching genome build and avoid re-fetching.
Not for: Calculating personal PRS values; use prs.calculate_score after approval.
Example prompts: Which PRS scores are imported locally?
Result semantics: Lists local score-cache metadata only; it does not read Active Genome Index.
Search public PGS Catalog score metadata by trait, score ID, EFO term, or free-text query without reading Active Genome Index.
Use when: The user asks which published PGS/PRS scores exist for a trait or provides a PGS Catalog score ID.
Why necessary: Score selection is source-specific and must expose trait, build, variant count, publication, evaluation, and licensing context before using a score on Active Genome Index.
Not for: Reading or scoring a user's genome; pass the chosen pgs_id to prs.calculate_score after Active Genome Index access approval. Training a new PRS from GWAS summary statistics.
Example prompts: Find PGS Catalog scores for coronary artery disease. What is PGS000001?
Result semantics: Returns public score candidates and source metadata only; it does not read Active Genome Index.