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	Analiza wzbogacenia szlaków bayesowskich ×	Analiza wieloomikowa wzbogacenia szlaków ×
Dziedzina	Bioinformatyka	Bioinformatyka
Rodzina	Process / pipeline	Process / pipeline
Rok powstania≠	2001–2007	2014–2016 (multi-omics extension of enrichment methods established ~2005)
Twórca≠	Pierre Baldi, Anthony Long; Michael Newton et al. (foundational Bayesian gene-set frameworks)	Building on Subramanian et al. (2005); multi-omics integration formalised by Meng et al. and others (~2014–2016)
Typ≠	Probabilistic gene-set testing	Integrative pathway analysis pipeline
Źródło pierwotne≠	Baldi, P., & Long, A. D. (2001). A Bayesian framework for the analysis of microarray expression data: regularized t-test and statistical inferences of gene changes. Bioinformatics, 17(6), 509–519. DOI ↗	Meng, C., Kuster, B., Culhane, A. C., & Gholami, A. M. (2014). A multivariate approach to the integration of multi-omics datasets. BMC Bioinformatics, 15, 162. link ↗
Inne nazwy	Bayesian gene-set testing, Bayesian GSEA, Bayesian functional enrichment, BGSEA	multi-omics pathway analysis, integrated pathway enrichment, multi-layer pathway enrichment, MOPEA
Pokrewne≠	6	1
Podsumowanie≠	Bayesian pathway enrichment analysis tests whether a predefined set of genes — a biological pathway — is systematically overrepresented among genes that show evidence of differential activity in an experiment. Unlike classical over-representation tests, it encodes prior biological knowledge as a prior distribution and updates it with the observed expression data, yielding posterior probabilities of enrichment rather than p-values. This probabilistic framing naturally handles small samples, multiple pathways, and uncertainty propagation in a coherent statistical framework.	Multi-omics pathway enrichment analysis is a bioinformatics pipeline that integrates molecular data from two or more omics layers — such as transcriptomics, proteomics, metabolomics, and epigenomics — and tests whether the combined signal from those layers converges on specific biological pathways more than expected by chance. By considering multiple molecular levels simultaneously, it identifies pathway-level dysregulation that single-omics analyses would miss.
ScholarGateZbiór danych ↗	v1 2 Źródła PUBLISHED	v1 2 Źródła PUBLISHED

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