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bio-pathway-gsea

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Atualizado16 de junho de 2026 às 14:22

Tests a ranked gene vector for coordinated expression shifts in GO, KEGG, Reactome, or MSigDB gene sets with clusterProfiler's gseGO, gseKEGG, gsePathway, and GSEA (fgseaMultilevel engine), and scores per-sample pathway activity with ssGSEA and GSVA. Covers why a GSEA result is a deterministic function of three implicit choices (the ranking STATISTIC, the weight exponent p, and which LABELS are permuted), why the input must be a NAMED vector sorted DECREASING by a signed variance-calibrated metric (DESeq2 stat, limma t) not a raw p-value that erases direction, why preranked gene-permutation is anti-conservative for correlated sets (CAMERA is the fix), why nPerm is gone (eps governs tiny p), and why set.seed is required. Use when every gene carries a DE statistic, when a hard cutoff is arbitrary, or when ORA finds nothing. For gene-list ORA see go-enrichment; the ranking statistic comes from differential-expression/de-results.

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