AUTHOR=Martel Alexandre , Brar Hardev , Mayer Boris F. , Charron Jean-Benoit 

TITLE=Diversification of the Histone Acetyltransferase GCN5 through Alternative Splicing in Brachypodium distachyon

JOURNAL=Frontiers in Plant Science

VOLUME=8

YEAR=2017

URL=https://www.frontiersin.org/journals/plant-science/articles/10.3389/fpls.2017.02176

DOI=10.3389/fpls.2017.02176

ISSN=1664-462X

ABSTRACT=<p>The epigenetic modulatory SAGA complex is involved in various developmental and stress responsive pathways in plants. Alternative transcripts of the SAGA complex's enzymatic subunit GCN5 have been identified in <italic>Brachypodium distachyon</italic>. These splice variants differ based on the presence and integrity of their conserved domain sequences: the histone acetyltransferase domain, responsible for catalytic activity, and the bromodomain, involved in acetyl-lysine binding and genomic loci targeting. <italic>GCN5</italic> is the wild-type transcript, while alternative splice sites result in the following transcriptional variants: <italic>L-GCN5</italic>, which is missing the bromodomain and <italic>S-GCN5</italic>, which lacks the bromodomain as well as certain motifs of the histone acetyltransferase domain. Absolute mRNA quantification revealed that, across eight <italic>B. distachyon</italic> accessions, <italic>GCN5</italic> was the dominant transcript isoform, accounting for up to 90% of the entire transcript pool, followed by <italic>L-GCN5</italic> and <italic>S-GCN5</italic>. A cycloheximide treatment further revealed that the <italic>S-GCN5</italic> splice variant was degraded through the nonsense-mediated decay pathway. All alternative <italic>BdGCN5</italic> transcripts displayed similar transcript profiles, being induced during early exposure to heat and displaying higher levels of accumulation in the crown, compared to aerial tissues. All predicted protein isoforms localize to the nucleus, which lends weight to their purported epigenetic functions. S-GCN5 was incapable of forming an <italic>in vivo</italic> protein interaction with ADA2, the transcriptional adaptor that links the histone acetyltransferase subunit to the SAGA complex, while both GCN5 and L-GCN5 interacted with ADA2, which suggests that a complete histone acetyltransferase domain is required for BdGCN5-BdADA2 interaction <italic>in vivo</italic>. Thus, there has been a diversification in <italic>BdGCN5</italic> through alternative splicing that has resulted in differences in conserved domain composition, transcript fate and <italic>in vivo</italic> protein interaction partners. Furthermore, our results suggest that <italic>B. distachyon</italic> may harbor compositionally distinct SAGA-like complexes that differ based on their histone acetyltransferase subunit.</p>