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

Roni H G Wright; Viviana Vastolo; Javier Quilez Oliete; José Carbonell-Caballero; Miguel Beato

doi:10.3389/fendo.2022.888802

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

Front Endocrinol (Lausanne). 2022 Aug 11:13:888802. doi: 10.3389/fendo.2022.888802. eCollection 2022.

Authors

Roni H G Wright^{1

2}, Viviana Vastolo¹, Javier Quilez Oliete¹, José Carbonell-Caballero¹, Miguel Beato^{1

3}

Affiliations

¹ Center for Genomic Regulation (CRG), Barcelona Institute of Science and Technology (BIST), Barcelona, Spain.
² Basic Sciences Department, Faculty of Medicine and Health Sciences, Universitat Internacional de Catalunya, Barcelona, Spain.
³ Universitat Pompeu Fabra (UPF), Barcelona, Spain.

Abstract

Background: Breast cancer cells enter into the cell cycle following progestin exposure by the activation of signalling cascades involving a plethora of enzymes, transcription factors and co-factors that transmit the external signal from the cell membrane to chromatin, ultimately leading to a change of the gene expression program. Although many of the events within the signalling network have been described in isolation, how they globally team up to generate the final cell response is unclear.

Methods: In this study we used antibody microarrays and phosphoproteomics to reveal a dynamic global signalling map that reveals new key regulated proteins and phosphor-sites and links between previously known and novel pathways. T47D breast cancer cells were used, and phospho-sites and pathways highlighted were validated using specific antibodies and phenotypic assays. Bioinformatic analysis revealed an enrichment in novel signalling pathways, a coordinated response between cellular compartments and protein complexes.

Results: Detailed analysis of the data revealed intriguing changes in protein complexes involved in nuclear structure, epithelial to mesenchyme transition (EMT), cell adhesion, as well as transcription factors previously not associated with breast cancer cell proliferation. Pathway analysis confirmed the key role of the MAPK signalling cascade following progesterone and additional hormone regulated phospho-sites were identified. Full network analysis shows the activation of new signalling pathways previously not associated with progesterone signalling in T47D breast cancer cells such as ERBB and TRK. As different post-translational modifications can mediate complex crosstalk mechanisms and massive PARylation is also rapidly induced by progestins, we provide details of important chromatin regulatory complexes containing both phosphorylated and PARylated proteins.

Conclusions: This study contributes an important resource for the scientific community, as it identifies novel players and connections meaningful for breast cancer cell biology and potentially relevant for cancer management.

Keywords: MAPK/ERK signalling; PARylation; breast cancer; cell proliferation; chromatin; phosphoproteome; progesterone; signalling.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Breast Neoplasms*
Chromatin
Female
Humans
Phosphorylation
Progesterone*
Progestins
Receptors, Progesterone
Transcription Factors

Substances

Chromatin
Progestins
Receptors, Progesterone
Transcription Factors
Progesterone