Complexities in the role of acetylation dynamics in modifying inducible gene activation parameters

Author:

Carrera Samantha1,O’Donnell Amanda1,Li Yaoyong1,Nowicki-Osuch Karol1ORCID,Yang Shen-Hsi1,Baker Syed Murtuza1,Spiller David1,Sharrocks Andrew D1ORCID

Affiliation:

1. Faculty of Biology, Medicine and Health, University of Manchester, Michael Smith Building, Oxford Road, Manchester M13 9PT, UK

Abstract

Abstract High levels of histone acetylation are associated with the regulatory elements of active genes, suggesting a link between acetylation and gene activation. We revisited this model, in the context of EGF-inducible gene expression and found that rather than a simple unifying model, there are two broad classes of genes; one in which high lysine acetylation activity is required for efficient gene activation, and a second group where the opposite occurs and high acetylation activity is inhibitory. We examined the latter class in more detail using EGR2 as a model gene and found that lysine acetylation levels are critical for several activation parameters, including the timing of expression onset, and overall amplitudes of the transcriptional response. In contrast, DUSP1 responds in the canonical manner and its transcriptional activity is promoted by acetylation. Single cell approaches demonstrate heterogenous activation kinetics of a given gene in response to EGF stimulation. Acetylation levels modify these heterogenous patterns and influence both allele activation frequencies and overall expression profile parameters. Our data therefore point to a complex interplay between acetylation equilibria and target gene induction where acetylation level thresholds are an important determinant of transcriptional induction dynamics that are sensed in a gene-specific manner.

Funder

Wellcome Trust

BBSRC

University of Manchester

Publisher

Oxford University Press (OUP)

Subject

Genetics

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