Abstract
AbstractSingle-cell assays for transposase-accessible chromatin sequencing data are one of the most powerful tools for studying the epigenetic heterogeneity of cell populations. However, the chromatin accessibility landscape is not well understood and lacks a proper way to interpret it. This work proposes Gene Regulation Accessibility Integrating GeneHancer (GRAIGH), a novel approach to the interpretation of genome accessibility through the integration of the GeneHancer database information, which describes genome-wide enhancer-to-gene associations. Firstly, this paper presents the methods for integrating GeneHancer with scATAC-seq data, creating a new matrix where the features are the GeneHancer elements IDs instead of the accessibility peaks. Secondly, it investigates its capability to analyze the data and detect cellular heterogeneity. In particular, this work shows that the GeneHancer elements are selectively accessible for distinct cell types, and more importantly, their connected genes are precisely known marker genes. Moreover, it investigates the specificity of GeneHancer elements accessibility, demonstrating their high selectivity against the gene activity.
Publisher
Cold Spring Harbor Laboratory
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