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Establishment and characterization of a new spontaneously immortalized ER -/PR -/HER2 + human breast cancer cell line, DHSF-BR16

Academic Article
Publication Date:
2021
abstract:
Invasive ductal carcinoma (IDC) constitutes the most frequent malignant cancer endangering women's health. In this study, a new spontaneously immortalized breast cancer cell line, DHSF-BR16 cells, was isolated from the primary IDC of a 74-years old female patient, treated with neoadjuvant chemotherapy and disease-free 5-years after adjuvant chemotherapy. Primary breast cancer tissue surgically removed was classified as ER-/PR-/HER2+, and the same phenotype was maintained by DHSF-BR16 cells. We examined DHSF-BR16 cell morphology and relevant biological and molecular markers, as well as their response to anticancer drugs commonly used for breast cancer treatment. MCF-7 cells were used for comparison purposes. The DHSF-BR16 cells showed the ability to form spheroids and migrate. Furthermore, DHSF-BR16 cells showed a mixed stemness phenotype (i.e. CD44+/CD24-/low), high levels of cytokeratin 7, moderate levels of cytokeratin 8 and 18, EpCAM and E-Cadh. Transcriptome analysis showed 2071 differentially expressed genes between DHSF-BR16 and MCF-7 cells (logFC > 2, p-adj < 0.01). Several genes were highly upregulated or downregulated in the new cell line (log2 scale fold change magnitude within - 9.6 to + 12.13). A spontaneous immortalization signature, mainly represented by extracellular exosomes-, plasma membrane- and endoplasmic reticulum membrane pathways (GO database) as well as by metabolic pathways (KEGG database) was observed in DHSF-BR16 cells. Also, these cells were more resistant to anthracyclines compared with MCF-7 cells. Overall, DHSF-BR16 cell line represents a relevant model useful to investigate cancer biology, to identify both novel prognostic and drug response predictive biomarkers as well as to assess new therapeutic strategies.
Iris type:
1.1 Articolo in rivista
Keywords:
expression; biology; identification; chemoteraphy; promote
List of contributors:
Nobili, S.; Mannini, A.; Parenti, A.; Raggi, C.; Lapucci, A.; Chiorino, G.; Paccosi, S.; Di Gennaro, P.; Vezzosi, V.; Romagnoli, P.; Susini, T.; Coronnello, M.
Handle:
https://ricerca.unich.it/handle/11564/752828
Full Text:
https://ricerca.unich.it//retrieve/handle/11564/752828/261157/Nobili%20et%20al%20Sci%20Rep%202021.pdf
Published in:
SCIENTIFIC REPORTS
Journal
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URL

https://www.nature.com/articles/s41598-021-87362-0
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