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| Anàlisi de pics ChIP-seq assistida per aprenentatge automàtic× | Expressió Diferencial en RNA-seq× | |
|---|---|---|
| Camp | Bioinformàtica | Bioinformàtica |
| Família | Process / pipeline | Process / pipeline |
| Any d'origen≠ | 2008 (classical); ML-assisted variants 2012–present | 2008–2010 (RNA-seq DE methodology established) |
| Autor original≠ | Building on MACS (Zhang et al. 2008); ML extensions by Haiminen et al. and others (2010s–2020s) | Multiple groups; foundational methods from Anders & Huber (DESeq, 2010), Robinson, McCarthy & Smyth (edgeR, 2010) |
| Tipus≠ | Supervised/unsupervised ML-augmented peak detection pipeline | Quantitative genomics pipeline |
| Font seminal≠ | Kharchenko, P. V., Tolstorukov, M. Y., & Park, P. J. (2008). Design and analysis of ChIP-seq experiments for DNA-binding proteins. Nature Biotechnology, 26(12), 1351-1359. DOI ↗ | Love, M. I., Huber, W., & Anders, S. (2014). Moderated estimation of fold change and dispersion for RNA-seq data with DESeq2. Genome Biology, 15(12), 550. DOI ↗ |
| Àlies | ML-based ChIP-seq peak detection, deep learning ChIP-seq peak calling, ML-enhanced ChIP-seq analysis, AI-assisted ChIP-seq peak identification | RNA-seq DE analysis, transcriptomic differential expression, bulk RNA-seq DE, DEA |
| Relacionats | 6 | 6 |
| Resum≠ | Machine learning-assisted ChIP-seq peak calling extends classical statistical peak detection with supervised or unsupervised learning models that distinguish genuine protein-binding sites from background noise. By training on sequence composition, read coverage profiles, and epigenomic features, these methods improve sensitivity and specificity compared with threshold-based approaches, particularly in low-signal or heterogeneous chromatin contexts. | RNA-seq differential expression (DE) analysis identifies genes whose transcript abundance differs significantly between two or more biological conditions — for example, treated versus control, or diseased versus healthy tissue. Starting from raw sequencing reads, the pipeline moves through alignment, count-based normalization, statistical modeling of count dispersion, hypothesis testing, and multiple-testing correction to produce a ranked list of differentially expressed genes accompanied by fold-change estimates and adjusted p-values. |
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