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ChIP-seq Peak Calling×변이 호출×
분야생물정보학생물정보학
계열Process / pipelineProcess / pipeline
기원 연도2007–20082009–2010 (modern high-throughput era)
창시자Johnson et al. (ChIP-seq concept, 2007); Zhang et al. (MACS algorithm, 2008)Li et al. (SAMtools/bcftools, 2009); McKenna et al. (GATK, 2010)
유형Computational genomics pipelineComputational genomics pipeline
원전Zhang, 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 ↗McKenna, A., Hanna, M., Banks, E., Sivachenko, A., Cibulskis, K., Kernytsky, A., ... & DePristo, M. A. (2010). The Genome Analysis Toolkit: A MapReduce framework for analyzing next-generation DNA sequencing data. Genome Research, 20(9), 1297–1303. DOI ↗
별칭ChIP-seq analysis, peak detection, MACS peak calling, ChIP peak identificationSNP calling, genotyping from sequencing, mutation detection, variant detection
관련66
요약ChIP-seq peak calling is a computational pipeline that identifies genomic regions where a protein of interest — a transcription factor or histone modification — is enriched, based on sequencing reads from chromatin immunoprecipitation experiments. It converts raw sequencing data into a set of high-confidence binding or modification sites across the genome, enabling downstream analysis of gene regulation, chromatin state, and epigenetic mechanisms.Variant calling is the computational process of identifying positions in a sequenced genome that differ from a reference sequence — including single nucleotide polymorphisms (SNPs), small insertions and deletions (indels), and structural variants. It transforms aligned sequencing reads into an interpretable catalogue of genetic differences, forming the foundation for population genetics, disease-gene discovery, and clinical genomics applications.
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ScholarGate방법 비교: ChIP-seq Peak Calling · Variant Calling. 2026-06-17에 다음에서 검색함: https://scholargate.app/ko/compare