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Bayesiansk ChIP-seq toppkalling×Bayesiansk epigenomdekkende assosiasjonsstudie (Bayesian EWAS)×
FagfeltBioinformatikkBioinformatikk
FamilieProcess / pipelineProcess / pipeline
Opprinnelsesår2008–20092010s (framework developed ~2013–2016)
OpphavspersonSpyrou et al. (BayesPeak, 2009); broader Bayesian ChIP-seq framework developed across multiple groups ~2008–2012Multiple groups; Bayesian EWAS framework advanced by S. Richardson, P.-C. Tsai, J. T. Bell and colleagues
TypeProbabilistic signal detection pipelineStatistical association analysis
Opprinnelig kildeZhang, Y., Liu, T., Meyer, C. A., Eeckhoute, J., Johnson, D. S., Bernstein, B. E., Nusbaum, C., Myers, R. M., Brown, M., Li, W., & Liu, X. S. (2008). Model-based analysis of ChIP-Seq (MACS). Genome Biology, 9(9), R137. DOI ↗Richardson, S., Tsai, P. C., Bell, J. T., & Timpson, N. J. (2016). Bayesian approaches to studying associations between epigenetic marks and phenotypes. International Journal of Epidemiology, 45(3), 694–705. link ↗
AliasBayesian ChIP-seq analysis, probabilistic peak detection, Bayesian peak caller, ChIP-seq Bayesian enrichment callingBayesian EWAS, B-EWAS, Bayesian methylation-wide association study, Bayesian epigenetic association analysis
Relaterte64
SammendragBayesian ChIP-seq peak calling applies probabilistic models — typically Poisson, negative binomial, or hidden Markov models with Bayesian inference — to detect genomic regions enriched for a protein of interest in chromatin immunoprecipitation followed by sequencing experiments. By explicitly modelling read-count noise and incorporating prior distributions, Bayesian callers yield posterior probabilities of enrichment rather than simple p-values, providing a principled framework for uncertainty quantification across the genome.A Bayesian EWAS is a genome-scale association analysis that links epigenetic marks — most commonly CpG-site DNA methylation — to a phenotype or trait of interest, replacing or supplementing the classical frequentist p-value framework with a Bayesian probabilistic model. It yields posterior probabilities of association and credible intervals for each CpG site, allowing formal incorporation of prior biological knowledge and more principled handling of the multiple-testing burden intrinsic to testing hundreds of thousands of sites simultaneously.
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ScholarGateSammenlign metoder: Bayesian ChIP-seq peak calling · Bayesian epigenome-wide association study. Hentet 2026-06-18 fra https://scholargate.app/no/compare