Literature DB >> 24741710

Axes of differentiation in breast cancer: untangling stemness, lineage identity, and the epithelial to mesenchymal transition.

Roy Z Granit, Michal Slyper, Ittai Ben-Porath.   

Abstract

Differentiation-associated regulatory programs are central in determining tumor phenotype, and contribute to heterogeneity between tumors and between individual cells within them. The transcriptional programs that control luminal and basal lineage identity in the normal mammary epithelium, as well as progenitor and stem cell function, are active in breast cancers, and show distinct associations with different disease subtypes. Also active in some tumors is the epithelial to mesenchymal transition (EMT) program, which endows carcinoma cells with mesenchymal as well as stem cell traits. The differentiation state of breast cancer cells is thus dictated by the complex combination of regulatory programs, and these can dramatically affect tumor growth and metastatic capacity. Breast cancer differentiation is often viewed along an axis between a basal–mesenchymal–stem cell state and a luminal–epithelial–differentiated state. Here we consider the links, as well as the distinctions, between the three components of this axis: basal versus luminal, mesenchymal versus epithelial, and stem cell versus differentiated identity. Analysis on a multidimensional scale, in which each of these axes is assessed separately, may offer increased resolution of tumor differentiation state. Cancer cells possessing a high degree of stemness would display increased capacity to shift between positions on such a multidimensional scale, and to acquire intermediate phenotypes on its different axes. Further molecular analysis of breast cancer cells with a focus on single-cell profiling, and the development of improved tools for dissection of the circuits controlling gene activity, are essential for the elucidation of the programs dictating breast cancer differentiation state.

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Year:  2014        PMID: 24741710     DOI: 10.1002/wsbm.1252

Source DB:  PubMed          Journal:  Wiley Interdiscip Rev Syst Biol Med        ISSN: 1939-005X


  8 in total

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Journal:  Cell Mol Life Sci       Date:  2015-01-07       Impact factor: 9.261

2.  Coactivation of Estrogen Receptor and IKKβ Induces a Dormant Metastatic Phenotype in ER-Positive Breast Cancer.

Authors:  Lamiaa El-Shennawy; Oleksii Dubrovskyi; Irida Kastrati; Jeanne M Danes; Yiqun Zhang; Herbert E Whiteley; Chad J Creighton; Jonna Frasor
Journal:  Cancer Res       Date:  2017-12-11       Impact factor: 12.701

3.  The NF-κB Pathway Promotes Tamoxifen Tolerance and Disease Recurrence in Estrogen Receptor-Positive Breast Cancers.

Authors:  Irida Kastrati; Stacey E P Joosten; Svetlana E Semina; Luis H Alejo; Svitlana D Brovkovych; Joshua D Stender; Hugo M Horlings; Marleen Kok; Elaine T Alarid; Geoffrey L Greene; Sabine C Linn; Wilbert Zwart; Jonna Frasor
Journal:  Mol Cancer Res       Date:  2020-04-03       Impact factor: 5.852

4.  Stemness of the hybrid Epithelial/Mesenchymal State in Breast Cancer and Its Association with Poor Survival.

Authors:  Anne Grosse-Wilde; Aymeric Fouquier d'Hérouël; Ellie McIntosh; Gökhan Ertaylan; Alexander Skupin; Rolf E Kuestner; Antonio del Sol; Kathie-Anne Walters; Sui Huang
Journal:  PLoS One       Date:  2015-05-28       Impact factor: 3.240

5.  Cell state plasticity, stem cells, EMT, and the generation of intra-tumoral heterogeneity.

Authors:  Geoffrey M Wahl; Benjamin T Spike
Journal:  NPJ Breast Cancer       Date:  2017-04-19

Review 6.  Senescence-Associated Pro-inflammatory Cytokines and Tumor Cell Plasticity.

Authors:  Jean Paul Vernot
Journal:  Front Mol Biosci       Date:  2020-05-13

7.  Modeling differentiation-state transitions linked to therapeutic escape in triple-negative breast cancer.

Authors:  Margaret P Chapman; Tyler Risom; Anil J Aswani; Ellen M Langer; Rosalie C Sears; Claire J Tomlin
Journal:  PLoS Comput Biol       Date:  2019-03-11       Impact factor: 4.475

8.  An Effect of Culture Media on Epithelial Differentiation Markers in Breast Cancer Cell Lines MCF7, MDA-MB-436 and SkBr3.

Authors:  Valdis Pirsko; Inese Cakstina; Marta Priedite; Rasma Dortane; Linda Feldmane; Miki Nakazawa-Miklasevica; Zanda Daneberga; Janis Gardovskis; Edvins Miklasevics
Journal:  Medicina (Kaunas)       Date:  2018-03-30       Impact factor: 2.430

  8 in total

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