Search the site

The University of Manchester Library

In April 2016 Manchester eScholar was replaced by the University of Manchester’s new Research Information Management System, Pure. In the autumn the University’s research outputs will be available to search and browse via a new Research Portal. Until then the University’s full publication record can be accessed via a temporary portal and the old eScholar content is available to search and browse via this archive.

Cell cycle phase regulates glucocorticoid receptor function.

Matthews, Laura; Johnson, James; Berry, Andrew; Trebble, Peter; Cookson, Ann; Spiller, Dave; Rivers, Caroline; Norman, Michael; White, Mike; Ray, David

PloS one. 2011;6(7):e22289.

Access to files

Full-text and supplementary files are not available from Manchester eScholar. Full-text is available externally using the following links:

Full-text held externally

Abstract

The glucocorticoid receptor (GR) is a member of the nuclear hormone receptor superfamily of ligand-activated transcription factors. In contrast to many other nuclear receptors, GR is thought to be exclusively cytoplasmic in quiescent cells, and only translocate to the nucleus on ligand binding. We now demonstrate significant nuclear GR in the absence of ligand, which requires nuclear localisation signal 1 (NLS1). Live cell imaging reveals dramatic GR import into the nucleus through interphase and rapid exclusion of the GR from the nucleus at the onset of mitosis, which persists into early G(1). This suggests that the heterogeneity in GR distribution is reflective of cell cycle phase. The impact of cell cycle-driven GR trafficking on a panel of glucocorticoid actions was profiled. In G2/M-enriched cells there was marked prolongation of glucocorticoid-induced ERK activation. This was accompanied by DNA template-specific, ligand-independent GR transactivation. Using chimeric and domain-deleted receptors we demonstrate that this transactivation effect is mediated by the AF1 transactivation domain. AF-1 harbours multiple phosphorylation sites, which are consensus sequences for kinases including CDKs, whose activity changes during the cell cycle. In G2/M there was clear ligand independent induction of GR phosphorylation on residues 203 and 211, both of which are phosphorylated after ligand activation. Ligand-independent transactivation required induction of phospho-S211GR but not S203GR, thereby directly linking cell cycle driven GR modification with altered GR function. Cell cycle phase therefore regulates GR localisation and post-translational modification which selectively impacts GR activity. This suggests that cell cycle phase is an important determinant in the cellular response to Gc, and that mitotic index contributes to tissue Gc sensitivity.

Bibliographic metadata

Type of resource:
Content type:
Journal article
Publication type:
Review article
Author(s):
Published date:
2011
Article title:
Cell cycle phase regulates glucocorticoid receptor function.
Journal title:
PloS one
Abbreviated journal title:
PLoS One
ISSN:
1932-6203
Place of publication:
United States
Volume:
6
Issue:
7
Pagination:
e22289
Digital Object Identifier:
10.1371/journal.pone.0022289
Pubmed Identifier:
21829454
Pii Identifier:
PONE-D-11-03574
Funder acknowledgement:
Access state:
Active

Institutional metadata

University researcher(s):
Academic department(s):

Record metadata

Manchester eScholar ID:
uk-ac-man-scw:133077
Created by:
Ray, David
Created:
13th October, 2011, 14:16:05
Last modified by:
Ray, David
Last modified:
19th August, 2013, 18:19:02

Can we help?

The library chat service will be available from 11am-3pm Monday to Friday (excluding Bank Holidays). You can also email your enquiry to us.