Application of gene set enrichment method to ChIP-chip data analysis

Yidong Chen; Fan Yang; Paul S. Meltzer

doi:10.1109/GENSIPS.2008.4555684

Application of gene set enrichment method to ChIP-chip data analysis

Yidong Chen, Fan Yang, Paul S. Meltzer

Producción científica: Conference contribution

Resumen

To elucidate biological functions from gene expression profiles, gene set enrichment analysis (GSEA) is widely applied against sets of predefined genes that may yield crucial clues to their functional themes or regulatory information. However, gene list derived from array-based chromatin- immunoprecipitation (ChIP-chip) experiments, where all genes with one or more binding sites of a given protein, possesses different characteristics than that from gene expression profiles: genes are not rank-ordered by their differential expression, but rather associated with a genomic distance to its nearest binding site from the transcription start site (TSS). In this study, we proposed a unique binding-site enrichment analysis method that enabled enrichment analysis of gene list derived from whole-genome ChIP-chip experiment to gene expression data set, such as a panel of normal tissue gene expression profiles or some cancer-related expression profiles, in order to identify the essential regulatory role of the transcription factor under study.

Idioma original	English (US)
Título de la publicación alojada	GENSIPS'08 - 6th IEEE International Workshop on Genomic Signal Processing and Statistics
DOI	https://doi.org/10.1109/GENSIPS.2008.4555684
Estado	Published - 2008
Publicado de forma externa	Sí
Evento	6th IEEE International Workshop on Genomic Signal Processing and Statistics, GENSIPS'08 - Phoenix, AZ, United States Duración: jun 8 2008 → jun 10 2008

Serie de la publicación

Nombre	GENSIPS'08 - 6th IEEE International Workshop on Genomic Signal Processing and Statistics

Other

Other	6th IEEE International Workshop on Genomic Signal Processing and Statistics, GENSIPS'08
País/Territorio	United States
Ciudad	Phoenix, AZ
Período	6/8/08 → 6/10/08

ASJC Scopus subject areas

Genetics
Signal Processing
Electrical and Electronic Engineering
Statistics, Probability and Uncertainty

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10.1109/GENSIPS.2008.4555684

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Chen, Y, Yang, F & Meltzer, PS 2008, Application of gene set enrichment method to ChIP-chip data analysis. En GENSIPS'08 - 6th IEEE International Workshop on Genomic Signal Processing and Statistics., 4555684, GENSIPS'08 - 6th IEEE International Workshop on Genomic Signal Processing and Statistics, 6th IEEE International Workshop on Genomic Signal Processing and Statistics, GENSIPS'08, Phoenix, AZ, United States, 6/8/08. https://doi.org/10.1109/GENSIPS.2008.4555684

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abstract = "To elucidate biological functions from gene expression profiles, gene set enrichment analysis (GSEA) is widely applied against sets of predefined genes that may yield crucial clues to their functional themes or regulatory information. However, gene list derived from array-based chromatin- immunoprecipitation (ChIP-chip) experiments, where all genes with one or more binding sites of a given protein, possesses different characteristics than that from gene expression profiles: genes are not rank-ordered by their differential expression, but rather associated with a genomic distance to its nearest binding site from the transcription start site (TSS). In this study, we proposed a unique binding-site enrichment analysis method that enabled enrichment analysis of gene list derived from whole-genome ChIP-chip experiment to gene expression data set, such as a panel of normal tissue gene expression profiles or some cancer-related expression profiles, in order to identify the essential regulatory role of the transcription factor under study.",

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AB - To elucidate biological functions from gene expression profiles, gene set enrichment analysis (GSEA) is widely applied against sets of predefined genes that may yield crucial clues to their functional themes or regulatory information. However, gene list derived from array-based chromatin- immunoprecipitation (ChIP-chip) experiments, where all genes with one or more binding sites of a given protein, possesses different characteristics than that from gene expression profiles: genes are not rank-ordered by their differential expression, but rather associated with a genomic distance to its nearest binding site from the transcription start site (TSS). In this study, we proposed a unique binding-site enrichment analysis method that enabled enrichment analysis of gene list derived from whole-genome ChIP-chip experiment to gene expression data set, such as a panel of normal tissue gene expression profiles or some cancer-related expression profiles, in order to identify the essential regulatory role of the transcription factor under study.

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Application of gene set enrichment method to ChIP-chip data analysis

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