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Date publication

mai 2017

Journal

BMC bioinformatics

Auteurs

Membres identifiés du Cancéropôle Est :
Dr GRONEMEYER Hinrich


Tous les auteurs :
Saleem MM, Mendoza-Parra MA, Cholley PE, Blum M, Gronemeyer H

Résumé

Exponentially increasing numbers of NGS-based epigenomic datasets in public repositories like GEO constitute an enormous source of information that is invaluable for integrative and comparative studies of gene regulatory mechanisms. One of today's challenges for such studies is to identify functionally informative local and global patterns of chromatin states in order to describe the regulatory impact of the epigenome in normal cell physiology and in case of pathological aberrations. Critically, the most preferred Chromatin ImmunoPrecipitation-Sequencing (ChIP-Seq) is inherently prone to significant variability between assays, which poses significant challenge on comparative studies. One challenge concerns data normalization to adjust sequencing depth variation.

Mots clés

ChIP-seq, Epigenome, Multi-sample analysis, Quantile-based data normalization

Référence

BMC Bioinformatics. 2017 May;18(1):259

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