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Regulation of cellular plasticity and extracellular vesicle secretion in breast cancer
Uppsala University, Disciplinary Domain of Medicine and Pharmacy, Faculty of Medicine, Department of Medical Biochemistry and Microbiology. (Aristidis Moustakas, TGF-b signalling)ORCID iD: 0000-0001-6554-738X
2023 (English)Doctoral thesis, comprehensive summary (Other academic)
Description
Abstract [en]

Epithelial-to-mesenchymal transition (EMT) is a dynamic process controlling the transition of cells between epithelial and mesenchymal states in various physiological or pathological conditions. In cancer, EMT promotes cell dissemination and metastatic colonization, enriches tumors with stem cell populations and confers resistance to anticancer therapy. Instigators of EMT activate a cohort of transcription factors (EMT-TF) which regulate the expression of each other and confer dynamic chromatin modifications to transcriptionally repress epithelial and induce mesenchymal genes. In this respect, transforming growth factor-β (TGF-β) is a potent inducer of EMT in different types of cancer.

In this study we first identified a link between the EMT-TF SNAI1 that is highly expressed in aggressive triple-negative breast cancers (TNBC), with the establishment of an intermediate epithelial-mesenchymal phenotype and the dual transcriptional induction of FOXA1 and androgen receptor which define mammary epithelial cell differentiation towards the luminal subtype. Studying additional phenotypes of SNAI1 mutant TNBCs, we showed that SNAI1 through TGF-β/SMAD signaling and repression of FOXA1, induces the guanine exchange factor PSD4/EFA6B, driving a vesicular trafficking program that promotes cell-matrix interactions and invasiveness.

Tumor-derived extracellular vesicles (EV) are important mediators of intercellular communication and of microenvironment formation where tumors develop. In this study we showed that MEK/ERK signaling, drives TGF-β promoting EV secretion by regulating cholesterol homeostasis in TNBC cells. Additionally, TGF-β ligands and matrix metalloproteases identified as EV protein contents, conferred pro-invasive attributes and resistance to chemotherapeutic drugs in recipient cells.

Metabolism has a well-documented role in tumor progression and EMT maintenance and here we propose that a hybrid epithelial-mesenchymal state upon knockout of the EMT-TF SNAI2 in TNBC cells, associated with altered expression of genes involved in metabolic pathways. This perturbed cell cycle progression in the mutant cells presumably via the transcription and stem cell factor SOX4.

In conclusion, this study provides insights into the contribution of the SNAIL family EMT-TFs, in the dynamic EMT process and the mechanisms by which this manifests the development of aggressive breast carcinomas. Furthermore, it provides means on the way TGF-β impacts on the biogenesis, secretion, and functional transfer of EV cargo molecules in the context of cancer.
Place, publisher, year, edition, pages
Uppsala: Acta Universitatis Upsaliensis, 2023. , p. 82
Series
Digital Comprehensive Summaries of Uppsala Dissertations from the Faculty of Medicine, ISSN 1651-6206 ; 1928
Keywords [en]
Cellular plasticity, extracellular vesicles, breast cancer, EMT
National Category
Cell and Molecular Biology Medical Biotechnology (with a focus on Cell Biology (including Stem Cell Biology), Molecular Biology, Microbiology, Biochemistry or Biopharmacy)
Research subject
Molecular Medicine; Molecular Cellbiology
Identifiers
URN: urn:nbn:se:uu:diva-499069ISBN: 978-91-513-1767-0 (print)OAI: oai:DiVA.org:uu-499069DiVA, id: diva2:1745386
Public defence
2023-05-16, Room A1:107, BMC, Husargatan 3, Uppsala, 22:24 (English)
Opponent
Supervisors
Available from: 2023-04-21 Created: 2023-03-22 Last updated: 2023-04-21
List of papers
1. SNAI1 and SMAD/TGF-β signals antagonize FOXA1 to control PSD4/EFA6B expression and couple integrin-mediated adhesion to endocytic fate in triple-negative breast cancer cells
Open this publication in new window or tab >>SNAI1 and SMAD/TGF-β signals antagonize FOXA1 to control PSD4/EFA6B expression and couple integrin-mediated adhesion to endocytic fate in triple-negative breast cancer cells
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(English)Manuscript (preprint) (Other academic)
National Category
Cell and Molecular Biology Cancer and Oncology
Identifiers
urn:nbn:se:uu:diva-499058 (URN)
Funder
Ludwig Institute for Cancer ResearchSwedish Cancer Society, CAN2018/469Swedish Cancer Society, CAN2021/1506Pj01HSwedish Research Council, 2017-01588Swedish Research Council, 2018- 02757Swedish Research Council, 2020-01291EU, European Research Council, 787472Uppsala University
Available from: 2023-03-22 Created: 2023-03-22 Last updated: 2023-03-24Bibliographically approved
2. Loss of SNAI1 induces cellular plasticity in invasive triple-negative breast cancer cells
Open this publication in new window or tab >>Loss of SNAI1 induces cellular plasticity in invasive triple-negative breast cancer cells
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2022 (English)In: Cell Death and Disease, E-ISSN 2041-4889, Vol. 13, no 9, article id 832Article in journal (Refereed) Published
Abstract [en]

The transcription factor SNAI1 mediates epithelial-mesenchymal transition, fibroblast activation and controls inter-tissue migration. High SNAI1 expression characterizes metastatic triple-negative breast carcinomas, and its knockout by CRISPR/Cas9 uncovered an epithelio-mesenchymal phenotype accompanied by reduced signaling by the cytokine TGFβ. The SNAI1 knockout cells exhibited plasticity in differentiation, drifting towards the luminal phenotype, gained stemness potential and could differentiate into acinar mammospheres in 3D culture. Loss of SNAI1 de-repressed the transcription factor FOXA1, a pioneering factor of mammary luminal progenitors. FOXA1 induced a specific gene program, including the androgen receptor (AR). Inhibiting AR via a specific antagonist regenerated the basal phenotype and blocked acinar differentiation. Thus, loss of SNAI1 in the context of triple-negative breast carcinoma cells promotes an intermediary luminal progenitor phenotype that gains differentiation plasticity based on the dual transcriptional action of FOXA1 and AR. This function of SNAI1 provides means to separate cell invasiveness from progenitor cell de-differentiation as independent cellular programs.
Place, publisher, year, edition, pages
Springer Nature, 2022
National Category
Cell and Molecular Biology
Identifiers
urn:nbn:se:uu:diva-486983 (URN)10.1038/s41419-022-05280-z (DOI)000862661500003 ()36171192 (PubMedID)
Funder
Swedish Research Council, 2020-01291Knut and Alice Wallenberg FoundationSwedish Cancer Society, CAN2018/469Swedish Cancer Society, CAN2021/1506Pj01HSwedish Research Council, 2018-02757EU, European Research Council, 787472Uppsala UniversitySwedish National Infrastructure for Computing (SNIC)
Available from: 2022-10-24 Created: 2022-10-24 Last updated: 2024-07-04Bibliographically approved
3. SNAI2 knockout induces metabolic and cell cycle changes in breast cancer cells
Open this publication in new window or tab >>SNAI2 knockout induces metabolic and cell cycle changes in breast cancer cells
(English)Manuscript (preprint) (Other academic)
National Category
Cell and Molecular Biology Cancer and Oncology
Identifiers
urn:nbn:se:uu:diva-499066 (URN)
Funder
Science for Life Laboratory, SciLifeLabSwedish National Infrastructure for Computing (SNIC), 2017-7-265Ludwig Institute for Cancer ResearchSwedish Cancer Society, CAN2018/46Swedish Cancer Society, CAN2021/1506Pj01Swedish Research Council, 2017-01588Swedish Research Council, 2018-02757Swedish Research Council, 2020-01291EU, European Research Council, 787472Uppsala University
Available from: 2023-03-22 Created: 2023-03-22 Last updated: 2023-03-24Bibliographically approved
4. TGF-β induces cholesterol accumulation to regulate the fate of tumor-derived extracellular vesicles
Open this publication in new window or tab >>TGF-β induces cholesterol accumulation to regulate the fate of tumor-derived extracellular vesicles
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(English)Manuscript (preprint) (Other academic)
National Category
Cell and Molecular Biology Cancer and Oncology
Identifiers
urn:nbn:se:uu:diva-499060 (URN)
Funder
Swedish Cancer Society, CAN2018/469Swedish Cancer Society, CAN2021/1506Pj01HSwedish Research Council, 2018-02757
Available from: 2023-03-22 Created: 2023-03-22 Last updated: 2023-03-24Bibliographically approved

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Tsirigoti, Chrysoula

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