Mitogen-activated Protein Kinase Regulates Nuclear Association of Human Progesterone Receptors

Overview

Journal Mol Endocrinol

Specialties Endocrinology
Molecular Biology

Date 2003 Jan 30

PMID 12554776

Citations 60

Authors

Ming Qiu

Abby Olsen

Emily Faivre

Kathryn B Horwitz

Carol A Lange

Affiliations

Soon will be listed here.

Abstract

Breast cancers often have increased MAPK activity; this pathway may drive breast cancer cell growth by targeting steroid hormone receptors. MAPK phosphorylates human progesterone receptors (PRs) on Ser294, thus regulating several aspects of PR activity. To study the role of PR Ser294 phosphorylation on subcellular distribution, we stably expressed wild-type (wt) or S294A (Ser294 to Ala) PR-B in several cell types. PRs phosphorylated on Ser294 were nuclear. Activation of MAPK induced Ser294 phosphorylation and rapid nuclear translocation of wt, but not S294A, PR-B; both receptors concentrated in the nucleus after progestin treatment. The MAPK kinase inhibitor, U0126, blocked epidermal growth factor but not progestin-induced Ser294 phosphorylation and translocation of wt PR, indicating a novel mechanism for nuclear localization. After progestin treatment, wt PR-B underwent ligand-dependent down-regulation, while S294A PR-B persisted in nuclei. Prolonged treatment with U0126 or the nuclear export inhibitor, leptomycin B, promoted nuclear accumulation of wt PR-B and blocked ligand-dependent PR down-regulation, suggesting that PR degradation occurs in the cytoplasm and requires MAPK-dependent nuclear export. Stabilization of PRs by leptomycin B also blocked PR transcriptional activity, indicating a link between nucleocytoplasmic shuttling, receptor stability, and function. These results support a regulatory role for MAPK in nuclear steroid hormone receptor subcellular localization and coupling to multiple PR functions.

Citing Articles

Bio-Pathological Functions of Posttranslational Modifications of Histological Biomarkers in Breast Cancer.

Neagu A, Josan C, Jayaweera T, Morrissiey H, Johnson K, Darie C Molecules. 2024; 29(17).

PMID: 39275004 PMC: 11397409. DOI: 10.3390/molecules29174156.

A molecular toolbox to study progesterone receptor signaling.

Aarts M, Wagner M, van der Wal T, van Boxtel A, van Amerongen R J Mammary Gland Biol Neoplasia. 2023; 28(1):24.

PMID: 38019315 PMC: 10687192. DOI: 10.1007/s10911-023-09550-0.

Global signalling network analysis of luminal T47D breast cancer cells in response to progesterone.

Wright R, Vastolo V, Oliete J, Carbonell-Caballero J, Beato M Front Endocrinol (Lausanne). 2022; 13:888802.

PMID: 36034422 PMC: 9403329. DOI: 10.3389/fendo.2022.888802.

Stochastic model of ERK-mediated progesterone receptor translocation, clustering and transcriptional activity.

Marquez-Lago T, Steinberg S Sci Rep. 2022; 12(1):11791.

PMID: 35821038 PMC: 9276744. DOI: 10.1038/s41598-022-13821-x.

The Role of Progesterone Receptors in Breast Cancer.

Li Z, Wei H, Li S, Wu P, Mao X Drug Des Devel Ther. 2022; 16:305-314.

PMID: 35115765 PMC: 8801368. DOI: 10.2147/DDDT.S336643.