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Human medulloblastoma cell lines: Investigating on cancer stem cell-like phenotype

TitleHuman medulloblastoma cell lines: Investigating on cancer stem cell-like phenotype
Publication TypeArticolo su Rivista peer-reviewed
Year of Publication2020
AuthorsCasciati, A., Tanori Mirella, Manczak R., Saada S., Tanno Barbara, Giardullo Paola, Porcù E., Rampazzo E., Persano L., Viola G., Dalmay C., Lalloue F., Pothier A., Merla Caterina, and Mancuso Mariateresa
JournalCancers
Volume12
ISSN20726694
Abstract

Medulloblastoma (MB) is the most common malignant pediatric brain tumor. Despite the progress of new treatments, the risk of recurrence, morbidity, and death remains significant and the long-term adverse effects in survivors are substantial. The fraction of cancer stem-like cells (CSCs) because of their self-renewal ability and multi-lineage differentiation potential is critical for tumor initiation, growth, and resistance to therapies. For the development of new CSC-targeted therapies, further in-depth studies are needed using enriched and stable MB-CSCs populations. This work, aimed at identifying the amount of CSCs in three available human cell lines (DAOY, D341, and D283), describes different approaches based on the expression of stemness markers. First, we explored potential differences in gene and protein expression patterns of specific stem cell markers. Then, in order to identify and discriminate undifferentiated from differentiated cells, MB cells were characterized using a physical characterization method based on a high-frequency dielectrophoresis approach. Finally, we compared their tumorigenic potential in vivo, through engrafting in nude mice. Concordantly, our findings identified the D283 human cell line as an ideal model of CSCs, providing important evidence on the use of a commercial human MB cell line for the development of new strategic CSC-targeting therapies. © 2020 by the authors. Licensee MDPI, Basel, Switzerland.

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URLhttps://www.scopus.com/inward/record.uri?eid=2-s2.0-85079176719&doi=10.3390%2fcancers12010226&partnerID=40&md5=1fabcae56e16fd6050b9a4814fd7a747
DOI10.3390/cancers12010226
Citation KeyCasciati2020