Dynamic histone variant exchange accompanies gene induction in T cells

Date

2009

Authors

Sutcliffe, Elissa
Parish, Ian
He, Yiqing
Juelich, Torsten
Tierney, Mary (Louise)
Rangasamy, Danny
Milburn, Peter J
Tremethick, David
Rao, Sudha
Parish, Christopher

Journal Title

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Volume Title

Publisher

American Society for Microbiology

Abstract

Changes in chromatin composition are often a prerequisite for gene induction. Nonallelic histone variants have recently emerged as key players in transcriptional control and chromatin modulation. While the changes in chromatin accessibility and histone posttranslational modification (PTM) distribution that accompany gene induction are well documented, the dynamics of histone variant exchange that parallel these events are still poorly defined. In this study, we have examined the changes in histone variant distribution that accompany activation of the inducible CD69 and heparanase genes in T cells. We demonstrate that the chromatin accessibility increases that accompany the induction of both of these genes are not associated with nucleosome loss but instead are paralleled by changes in histone variant distribution. Specifically, induction of these genes was paralleled by depletion of the H2A.Z histone variant and concomitant deposition of H3.3. Furthermore, H3.3 deposition was accompanied by changes in PTM patterns consistent with H3.3 enriching or depleting different PTMs upon incorporation into chromatin. Nevertheless, we present evidence that these H3.3-borne PTMs can be negated by recruited enzymatic activities. From these observations, we propose that H3.3 deposition may both facilitate chromatin accessibility increases by destabilizing nucleosomes and compete with recruited histone modifiers to alter PTM patterns upon gene induction.

Description

Keywords

Keywords: beta glucuronidase; CD69 antigen; heparanase; histone; hydroxamic acid; leukocyte antigen; messenger RNA; RNA polymerase II; T lymphocyte antigen; trichostatin A; histone H2AZ; histone H3; histone h3 3; unclassified drug; affinity chromatography; antibody

Citation

Source

Molecular and Cellular Biology

Type

Journal article

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Restricted until

2037-12-31