Alternative splicing of HDAC7 regulates its interaction with 14-3-3 proteins to alter histone marks and target gene expression

Laura M. Agosto, Michael J. Mallory, Max B. Ferretti, Davia Blake, Keegan S. Krick, Matthew R. Gazzara, Benjamin A. Garcia, Kristen W. Lynch

Research output: Contribution to journalArticlepeer-review

4 Scopus citations

Abstract

Chromatin regulation and alternative splicing are both critical mechanisms guiding gene expression. Studies have demonstrated that histone modifications can influence alternative splicing decisions, but less is known about how alternative splicing may impact chromatin. Here, we demonstrate that several genes encoding histone-modifying enzymes are alternatively spliced downstream of T cell signaling pathways, including HDAC7, a gene previously implicated in controlling gene expression and differentiation in T cells. Using CRISPR-Cas9 gene editing and cDNA expression, we show that differential inclusion of HDAC7 exon 9 controls the interaction of HDAC7 with protein chaperones, resulting in changes to histone modifications and gene expression. Notably, the long isoform, which is induced by the RNA-binding protein CELF2, promotes expression of several critical T cell surface proteins including CD3, CD28, and CD69. Thus, we demonstrate that alternative splicing of HDAC7 has a global impact on histone modification and gene expression that contributes to T cell development.

Original languageEnglish
Article number112273
JournalCell Reports
Volume42
Issue number3
DOIs
StatePublished - Mar 28 2023

Keywords

  • CP: Molecular biology
  • HDAC7
  • T cell receptors
  • alternative splicing
  • histone PTM
  • thymic development

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