EGFR Transgene Stimulates Spontaneous Formation of MCF7 Breast Cancer Cells Spheroids with Partly Loss of HER3 Receptor

Multicellular spheroids with 3D cell–cell interactions are a useful model to simulate the growth conditions of cancer. There is evidence that in tumor spheroids, the expression of various essential molecules is changed compared to the adherent form of cell cultures. These changes include growth fact...

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Autores principales: Troitskaya, Olga, Novak, Diana, Nushtaeva, Anna, Savinkova, Maria, Varlamov, Mikhail, Ermakov, Mikhail, Richter, Vladimir, Koval, Olga
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8657849/
https://www.ncbi.nlm.nih.gov/pubmed/34884742
http://dx.doi.org/10.3390/ijms222312937
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author Troitskaya, Olga
Novak, Diana
Nushtaeva, Anna
Savinkova, Maria
Varlamov, Mikhail
Ermakov, Mikhail
Richter, Vladimir
Koval, Olga
author_facet Troitskaya, Olga
Novak, Diana
Nushtaeva, Anna
Savinkova, Maria
Varlamov, Mikhail
Ermakov, Mikhail
Richter, Vladimir
Koval, Olga
author_sort Troitskaya, Olga
collection PubMed
description Multicellular spheroids with 3D cell–cell interactions are a useful model to simulate the growth conditions of cancer. There is evidence that in tumor spheroids, the expression of various essential molecules is changed compared to the adherent form of cell cultures. These changes include growth factor receptors and ABC transporters and result in the enhanced invasiveness of the cells and drug resistance. It is known that breast adenocarcinoma MCF7 cells can spontaneously form 3D spheroids and such spheroids are characterized by high expression of EGFR/HER2, while the natural phenotype of MCF7 cells is EGFR(low)/HER2(low). Therefore, it was interesting to reveal if high epidermal growth factor receptor (EGFR) expression is sufficient for the conversion of adherent MCF7 to spheroids. In this study, an MCF7 cell line with high expression of EGFR was engineered using the retroviral transduction method. These MCF7-EGFR cells assembled in spheroids very quickly and grew predominantly as a 3D suspension culture with no special plates, scaffolds, growth supplements, or exogenous matrixes. These spheroids were characterized by a rounded shape with a well-defined external border and 100 µM median diameter. The sphere-forming ability of MCF7-EGFR cells was up to 5 times stronger than in MCF7(wt) cells. Thus, high EGFR expression was the initiation factor of conversion of adherent MCF7(wt) cells to spheroids. MCF7-EGFR spheroids were enriched by the cells with a cancer stem cell (CSC) phenotype CD24(−/low)/CD44(−) in comparison with parental MCF7(wt) cells and MCF7-EGFR adhesive cells. We suppose that these properties of MCF7-EGFR spheroids originate from the typical features of parental MCF7 cells. We showed the decreasing of HER3 receptors in MCF7-EGFR spheroids compared to that in MCF(wt) and in adherent MCF7-EGFR cells, and the same decrease was observed in the MCF7(wt) spheroids growing under the growth factors stimulation. To summarize, the expression of EGFR transgene in MCF7 cells stimulates rapid spheroids formation; these spheroids are enriched by CSC-like CD24(−)/CD44(−) cells, they partly lose HER3 receptors, and are characterized by a lower potency in drug resistance pomp activation compared to MCF7(wt). These MCF7-EGFR spheroids are a useful cancer model for the development of anticancer drugs, including EGFR-targeted therapeutics.
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spelling pubmed-86578492021-12-10 EGFR Transgene Stimulates Spontaneous Formation of MCF7 Breast Cancer Cells Spheroids with Partly Loss of HER3 Receptor Troitskaya, Olga Novak, Diana Nushtaeva, Anna Savinkova, Maria Varlamov, Mikhail Ermakov, Mikhail Richter, Vladimir Koval, Olga Int J Mol Sci Article Multicellular spheroids with 3D cell–cell interactions are a useful model to simulate the growth conditions of cancer. There is evidence that in tumor spheroids, the expression of various essential molecules is changed compared to the adherent form of cell cultures. These changes include growth factor receptors and ABC transporters and result in the enhanced invasiveness of the cells and drug resistance. It is known that breast adenocarcinoma MCF7 cells can spontaneously form 3D spheroids and such spheroids are characterized by high expression of EGFR/HER2, while the natural phenotype of MCF7 cells is EGFR(low)/HER2(low). Therefore, it was interesting to reveal if high epidermal growth factor receptor (EGFR) expression is sufficient for the conversion of adherent MCF7 to spheroids. In this study, an MCF7 cell line with high expression of EGFR was engineered using the retroviral transduction method. These MCF7-EGFR cells assembled in spheroids very quickly and grew predominantly as a 3D suspension culture with no special plates, scaffolds, growth supplements, or exogenous matrixes. These spheroids were characterized by a rounded shape with a well-defined external border and 100 µM median diameter. The sphere-forming ability of MCF7-EGFR cells was up to 5 times stronger than in MCF7(wt) cells. Thus, high EGFR expression was the initiation factor of conversion of adherent MCF7(wt) cells to spheroids. MCF7-EGFR spheroids were enriched by the cells with a cancer stem cell (CSC) phenotype CD24(−/low)/CD44(−) in comparison with parental MCF7(wt) cells and MCF7-EGFR adhesive cells. We suppose that these properties of MCF7-EGFR spheroids originate from the typical features of parental MCF7 cells. We showed the decreasing of HER3 receptors in MCF7-EGFR spheroids compared to that in MCF(wt) and in adherent MCF7-EGFR cells, and the same decrease was observed in the MCF7(wt) spheroids growing under the growth factors stimulation. To summarize, the expression of EGFR transgene in MCF7 cells stimulates rapid spheroids formation; these spheroids are enriched by CSC-like CD24(−)/CD44(−) cells, they partly lose HER3 receptors, and are characterized by a lower potency in drug resistance pomp activation compared to MCF7(wt). These MCF7-EGFR spheroids are a useful cancer model for the development of anticancer drugs, including EGFR-targeted therapeutics. MDPI 2021-11-29 /pmc/articles/PMC8657849/ /pubmed/34884742 http://dx.doi.org/10.3390/ijms222312937 Text en © 2021 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Troitskaya, Olga
Novak, Diana
Nushtaeva, Anna
Savinkova, Maria
Varlamov, Mikhail
Ermakov, Mikhail
Richter, Vladimir
Koval, Olga
EGFR Transgene Stimulates Spontaneous Formation of MCF7 Breast Cancer Cells Spheroids with Partly Loss of HER3 Receptor
title EGFR Transgene Stimulates Spontaneous Formation of MCF7 Breast Cancer Cells Spheroids with Partly Loss of HER3 Receptor
title_full EGFR Transgene Stimulates Spontaneous Formation of MCF7 Breast Cancer Cells Spheroids with Partly Loss of HER3 Receptor
title_fullStr EGFR Transgene Stimulates Spontaneous Formation of MCF7 Breast Cancer Cells Spheroids with Partly Loss of HER3 Receptor
title_full_unstemmed EGFR Transgene Stimulates Spontaneous Formation of MCF7 Breast Cancer Cells Spheroids with Partly Loss of HER3 Receptor
title_short EGFR Transgene Stimulates Spontaneous Formation of MCF7 Breast Cancer Cells Spheroids with Partly Loss of HER3 Receptor
title_sort egfr transgene stimulates spontaneous formation of mcf7 breast cancer cells spheroids with partly loss of her3 receptor
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8657849/
https://www.ncbi.nlm.nih.gov/pubmed/34884742
http://dx.doi.org/10.3390/ijms222312937
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