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Bayesian ChIP-seq peak calling×Bayesian RNA-seq Differential Expression×
FachgebietBioinformatikBioinformatik
FamilieProcess / pipelineProcess / pipeline
Entstehungsjahr2008–20092010–2013
UrheberSpyrou et al. (BayesPeak, 2009); broader Bayesian ChIP-seq framework developed across multiple groups ~2008–2012Kendziorski et al. (EBSeq); Hardcastle & Kelly (baySeq)
TypProbabilistic signal detection pipelineBayesian statistical inference pipeline
Wegweisende QuelleZhang, 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 ↗Leng, N., Dawson, J. A., Thomson, J. A., Ruotti, V., Rissman, A. I., Smits, B. M., Haag, J. D., Gould, M. N., Stewart, R. M., & Kendziorski, C. (2013). EBSeq: An empirical Bayes hierarchical model for inference in RNA-seq experiments. Bioinformatics, 29(8), 1035–1043. link ↗
AliasnamenBayesian ChIP-seq analysis, probabilistic peak detection, Bayesian peak caller, ChIP-seq Bayesian enrichment callingBayesian DE analysis, Bayesian RNA-seq DE, baySeq, EBSeq
Verwandt66
ZusammenfassungBayesian 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.Bayesian RNA-seq differential expression analysis applies hierarchical Bayesian models to RNA sequencing read-count data to identify genes whose expression levels differ significantly between biological conditions. Rather than relying solely on p-values, these methods quantify the posterior probability that a gene is differentially expressed, borrowing statistical strength across genes and naturally accommodating low sample sizes common in genomics experiments.
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ScholarGateMethoden vergleichen: Bayesian ChIP-seq peak calling · Bayesian RNA-seq differential expression. Abgerufen am 2026-06-15 von https://scholargate.app/de/compare