ワンクリックで
guide-risk-precheck
Precheck biological and interpretation risks before selecting perturbation targets or guide designs.
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
Precheck biological and interpretation risks before selecting perturbation targets or guide designs.
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
| name | guide_risk_precheck |
| description | Precheck biological and interpretation risks before selecting perturbation targets or guide designs. |
| category | bio/perturb_seq |
| version | 1 |
| requires_tools | ["search_knowledge_base","evidence_review","ensembl_api","ncbi_eutils","python_repl"] |
| requires_network | true |
| user_invocable | true |
| tags | ["guide","crispr","risk","precheck","perturbation"] |
| aliases | ["perturbation_risk_precheck"] |
| species | any |
| modality | perturb_seq |
| stage | validation |
| stability | stable |
| safety_level | medium |
Flag major biological and interpretation risks before the user commits to a perturbation target or downstream guide design workflow.
Use this skill when the user is considering targets for CRISPR, CRISPRi, CRISPRa, or Perturb-seq and wants an early warning on likely failure modes.
search_knowledge_base for local design notes, prior screen guidance, or target-specific warnings.ensembl_api and ncbi_eutils to check gene structure, isoform complexity, prior perturbation context, and biologically plausible failure modes.evidence_review on the target-plus-system question so supported concerns are separated from speculation.python_repl to build a compact risk table when comparing multiple targets.search_knowledge_base, ensembl_api, ncbi_eutils, and evidence_review findings support the warning.Manage the BioAPEX current-feature workflow from scoping through review and completion
Turn an analysis request into a Slurm-ready execution plan with commands, resource assumptions, and job structure.
Scale a buffer recipe to a target volume and compute component masses/volumes.
Save a fetched summary or document to the knowledge base for later retrieval (e.g. after PubMed/UniProt lookup).
Interpret scRNA clusters using marker genes and suggest cell type or state.
Critically evaluate a perturbation hypothesis — challenge assumptions, propose negative controls, and flag confounders.