Molecular Heterogeneity in Breast Carcinoma Cells with Increased Invasive Capacities

BACKGROUND: Metastatic progression of breast cancer is still a challenge in clinical oncology. Therefore, an elucidation how carcinoma cells belonging to different breast cancer subtypes realize their metastatic capacities is needed. The aim of this study was to elucidate a similarity of activated m...

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Autores principales: Negro, Giulia, Aschenbrenner, Bertram, Brezar, Simona Kranjc, Cemazar, Maja, Coer, Andrej, Gasljevic, Gorana, Savic, Dragana, Sorokin, Maxim, Buzdin, Anton, Callari, Maurizio, Kvitsaridze, Irma, Jewett, Anahid, Vasileva-Slaveva, Mariela, Ganswindt, Ute, Skvortsova, Ira, Skvortsov, Sergej
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Sciendo 2020
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7087425/
https://www.ncbi.nlm.nih.gov/pubmed/32061169
http://dx.doi.org/10.2478/raon-2020-0007
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author Negro, Giulia
Aschenbrenner, Bertram
Brezar, Simona Kranjc
Cemazar, Maja
Coer, Andrej
Gasljevic, Gorana
Savic, Dragana
Sorokin, Maxim
Buzdin, Anton
Callari, Maurizio
Kvitsaridze, Irma
Jewett, Anahid
Vasileva-Slaveva, Mariela
Ganswindt, Ute
Skvortsova, Ira
Skvortsov, Sergej
author_facet Negro, Giulia
Aschenbrenner, Bertram
Brezar, Simona Kranjc
Cemazar, Maja
Coer, Andrej
Gasljevic, Gorana
Savic, Dragana
Sorokin, Maxim
Buzdin, Anton
Callari, Maurizio
Kvitsaridze, Irma
Jewett, Anahid
Vasileva-Slaveva, Mariela
Ganswindt, Ute
Skvortsova, Ira
Skvortsov, Sergej
author_sort Negro, Giulia
collection PubMed
description BACKGROUND: Metastatic progression of breast cancer is still a challenge in clinical oncology. Therefore, an elucidation how carcinoma cells belonging to different breast cancer subtypes realize their metastatic capacities is needed. The aim of this study was to elucidate a similarity of activated molecular pathways underlying an enhancement of invasiveness of carcinoma cells belonging to different breast carcinoma subtypes. MATERIALS AND METHODS: In order to reach this aim, parental and invasive (INV) MDA-MB-231 (triple-negative), T47D (hormone receptor-positive), and Au565 (Her2-positive) breast carcinoma cells were used and their molecular phenotypes were compared using a proteomic approach. RESULTS: Independently from breast cancer subtypes, INV cells have demonstrated fibroblast-like morphology accompanied by enhancement of invasive and migratory capacities, increased expression of cancer stem cell markers, and delayed tumor growth in in vivo animal models. However, the global proteomic analysis has highlighted that INV cells were different in protein expressions from the parental cells, and Her2-positive Au565-INV cells showed the most pronounced molecular differences compared to the triple-negative MDA-MB-231-INV and hormone receptor-positive T47D-INV cells. Although Au565-INV breast carcinoma cells possessed the highest number of deregulated proteins, they had the lowest overlapping in proteins commonly expressed in MDA-MB-231-INV and T47D-INV cells. CONCLUSIONS: We can conclude that hormone receptor-positive cells with increased invasiveness acquire the molecular characteristics of triple-negative breast cancer cells, whereas Her2-positive INV cells specifically changed their own molecular phenotype with very limited partaking in the involved pathways found in the MDA-MB-231-INV and T47D-INV cells. Since hormone receptor-positive invasive cells share their molecular properties with triple-negative breast cancer cells, we assume that these types of metastatic disease can be treated rather equally with an option to add anti-hormonal agents. In contrast, Her2-positive metastasis should be carefully evaluated for more effective therapeutic approaches which are distinct from the triple-negative and hormone-positive metastatic breast cancers.
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spelling pubmed-70874252020-03-26 Molecular Heterogeneity in Breast Carcinoma Cells with Increased Invasive Capacities Negro, Giulia Aschenbrenner, Bertram Brezar, Simona Kranjc Cemazar, Maja Coer, Andrej Gasljevic, Gorana Savic, Dragana Sorokin, Maxim Buzdin, Anton Callari, Maurizio Kvitsaridze, Irma Jewett, Anahid Vasileva-Slaveva, Mariela Ganswindt, Ute Skvortsova, Ira Skvortsov, Sergej Radiol Oncol Research Article BACKGROUND: Metastatic progression of breast cancer is still a challenge in clinical oncology. Therefore, an elucidation how carcinoma cells belonging to different breast cancer subtypes realize their metastatic capacities is needed. The aim of this study was to elucidate a similarity of activated molecular pathways underlying an enhancement of invasiveness of carcinoma cells belonging to different breast carcinoma subtypes. MATERIALS AND METHODS: In order to reach this aim, parental and invasive (INV) MDA-MB-231 (triple-negative), T47D (hormone receptor-positive), and Au565 (Her2-positive) breast carcinoma cells were used and their molecular phenotypes were compared using a proteomic approach. RESULTS: Independently from breast cancer subtypes, INV cells have demonstrated fibroblast-like morphology accompanied by enhancement of invasive and migratory capacities, increased expression of cancer stem cell markers, and delayed tumor growth in in vivo animal models. However, the global proteomic analysis has highlighted that INV cells were different in protein expressions from the parental cells, and Her2-positive Au565-INV cells showed the most pronounced molecular differences compared to the triple-negative MDA-MB-231-INV and hormone receptor-positive T47D-INV cells. Although Au565-INV breast carcinoma cells possessed the highest number of deregulated proteins, they had the lowest overlapping in proteins commonly expressed in MDA-MB-231-INV and T47D-INV cells. CONCLUSIONS: We can conclude that hormone receptor-positive cells with increased invasiveness acquire the molecular characteristics of triple-negative breast cancer cells, whereas Her2-positive INV cells specifically changed their own molecular phenotype with very limited partaking in the involved pathways found in the MDA-MB-231-INV and T47D-INV cells. Since hormone receptor-positive invasive cells share their molecular properties with triple-negative breast cancer cells, we assume that these types of metastatic disease can be treated rather equally with an option to add anti-hormonal agents. In contrast, Her2-positive metastasis should be carefully evaluated for more effective therapeutic approaches which are distinct from the triple-negative and hormone-positive metastatic breast cancers. Sciendo 2020-02-14 /pmc/articles/PMC7087425/ /pubmed/32061169 http://dx.doi.org/10.2478/raon-2020-0007 Text en © 2020 Giulia Negro, Bertram Aschenbrenner, Simona Kranjc Brezar, Maja Cemazar, Andrej Coer, Gorana Gasljevic, Dragana Savic, Maxim Sorokin, Anton Buzdin, Maurizio Callari, Irma Kvitsaridze, Anahid Jewett, Mariela Vasileva-Slaveva, Ute Ganswindt, Ira Skvortsova, Sergej Skvortsov, published by Sciendo http://creativecommons.org/licenses/by-nc-nd/3.0 This work is licensed under the Creative Commons Attribution-NonCommercial-NoDerivatives 3.0 License.
spellingShingle Research Article
Negro, Giulia
Aschenbrenner, Bertram
Brezar, Simona Kranjc
Cemazar, Maja
Coer, Andrej
Gasljevic, Gorana
Savic, Dragana
Sorokin, Maxim
Buzdin, Anton
Callari, Maurizio
Kvitsaridze, Irma
Jewett, Anahid
Vasileva-Slaveva, Mariela
Ganswindt, Ute
Skvortsova, Ira
Skvortsov, Sergej
Molecular Heterogeneity in Breast Carcinoma Cells with Increased Invasive Capacities
title Molecular Heterogeneity in Breast Carcinoma Cells with Increased Invasive Capacities
title_full Molecular Heterogeneity in Breast Carcinoma Cells with Increased Invasive Capacities
title_fullStr Molecular Heterogeneity in Breast Carcinoma Cells with Increased Invasive Capacities
title_full_unstemmed Molecular Heterogeneity in Breast Carcinoma Cells with Increased Invasive Capacities
title_short Molecular Heterogeneity in Breast Carcinoma Cells with Increased Invasive Capacities
title_sort molecular heterogeneity in breast carcinoma cells with increased invasive capacities
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7087425/
https://www.ncbi.nlm.nih.gov/pubmed/32061169
http://dx.doi.org/10.2478/raon-2020-0007
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