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فراخوانی قله‌های ChIP-seq سری زمانی×تحلیل بیان افتراقی RNA-seq×
حوزهزیست‌اطلاعاتیزیست‌اطلاعاتی
خانوادهProcess / pipelineProcess / pipeline
سال پیدایش2008–2012 (ChIP-seq); time-series extensions ~2015–20202008–2010 (RNA-seq DE methodology established)
پدیدآورENCODE Consortium; extended by Haiminen et al. and broader epigenomics communityMultiple groups; foundational methods from Anders & Huber (DESeq, 2010), Robinson, McCarthy & Smyth (edgeR, 2010)
نوعComputational epigenomics pipelineQuantitative genomics pipeline
منبع بنیادینLandt, S. G., Marinov, G. K., Kundaje, A., Kheradpour, P., Pauli, F., Batzoglou, S., ... & Snyder, M. (2012). ChIP-seq guidelines and practices of the ENCODE and modENCODE consortia. Genome Research, 22(9), 1813–1831. 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 ↗
نام‌های دیگرlongitudinal ChIP-seq analysis, dynamic ChIP-seq peak calling, time-course ChIP-seq, temporal chromatin profilingRNA-seq DE analysis, transcriptomic differential expression, bulk RNA-seq DE, DEA
مرتبط56
خلاصهTime-series ChIP-seq peak calling extends standard chromatin immunoprecipitation sequencing analysis to samples collected at multiple time points. By identifying and comparing protein-DNA binding peaks across a temporal dimension, the method reveals how transcription factor occupancy, histone modifications, or chromatin remodeler binding evolve during biological processes such as differentiation, circadian cycles, or stimulus response.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.
ScholarGateمجموعه‌داده
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  3. PUBLISHED
  1. v1
  2. 2 منابع
  3. PUBLISHED

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ScholarGateمقایسهٔ روش‌ها: Time-series ChIP-seq peak calling · RNA-seq Differential Expression. بازیابی‌شده در 2026-06-18 از https://scholargate.app/fa/compare