Increased chromatin accessibility facilitates intron retention in specific cell differentiation states

Journal Publication ResearchOnline@JCU
Petrova, Veronika;Song, Renhua;DEEP Consortium;Nordström, Karl J.V.;Walter, Jörn;Wong, Justin J.-L.;Armstrong, Nicola J.;Rasko, John E.J.;Schmitz, Ulf
Abstract

Dynamic intron retention (IR) in vertebrate cells is of widespread biological importance. Aberrant IR is associated with numerous human diseases including several cancers. Despite consistent reports demonstrating that intrinsic sequence features can help introns evade splicing, conflicting findings about cell type or condition-specific IR regulation by trans-regulatory and epigenetic mechanisms demand an unbiased and systematic analysis of IR in a controlled experimental setting. We integrated matched mRNA sequencing (RNA-seq), whole-genome bisulfite sequencing (WGBS), nucleosome occupancy methylome sequencing (NOMe-Seq), and chromatin immunoprecipitation sequencing (ChIP-seq) data from primary human myeloid and lymphoid cells. Using these multi-omics data and machine learning we trained two complementary models to determine the role of epigenetic factors in the regulation of IR in cells of the innate immune system. We show that increased chromatin accessibility, as revealed by nucleosome-free regions, contributes substantially to the retention of introns in a cell-specific manner. We also confirm that intrinsic characteristics of introns are key for them to evade splicing. This study suggests an important role of chromatin architecture in IR regulation. With an increasing appreciation that pathogenic alterations are linked to RNA processing, our findings may provide useful insights for the development of novel therapeutic approaches that target aberrant splicing.

Journal

Nucleic Acids Research

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Volume

50

ISBN/ISSN

1362-4962

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Issue

20

Pages Count

17

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Publisher

Oxford University Press

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EISSN

N/A

DOI

10.1093/nar/gkac994