4.4 Article

Endometrial Cancer Spheres Show Cancer Stem Cells Phenotype and Preference for Oxidative Metabolism

期刊

PATHOLOGY & ONCOLOGY RESEARCH
卷 25, 期 3, 页码 1163-1174

出版社

SPRINGER
DOI: 10.1007/s12253-018-0535-0

关键词

Endometrial neoplasms; Neoplastic stem cells; Glucose metabolism

资金

  1. Foundation for Science and Technology, Portugal [SFRH/SINTD/60068/2009, UID/NEU/04539/2013]
  2. Portuguese Society of Gynecology
  3. CIMAGO
  4. FEDER-COMPETE [POCI-01-0145-FEDER-007440]
  5. Portuguese National Programme for Scientific Re-equipment [REDE/1517/RMN/2005]
  6. POCI 2010 (European Fund for Regional Development)
  7. Fundação para a Ciência e a Tecnologia [SFRH/SINTD/60068/2009] Funding Source: FCT

向作者/读者索取更多资源

This study aimed to characterize endometrial cancer regarding cancer stem cells (CSC) markers, regulatory and differentiation pathways, tumorigenicity and glucose metabolism. Endometrial cancer cell line ECC1 was submitted to sphere forming protocols. The first spheres generation (ES1) was cultured in adherent conditions (G1). This procedure was repeated and was obtained generations of spheres (ES1, ES2 and ES3) and spheres-derived cells in adherent conditions (G1, G2 and G3). Populations were characterized regarding CD133, CD24, CD44, aldehyde dehydrogenase (ALDH), hormonal receptors, HER2, P53 and beta-catenin, fluorine-18 fluorodeoxyglucose ([F-18]FDG) uptake and metabolism by NMR spectroscopy. An heterotopic model evaluated differential tumor growth. The spheres self-renewal was higher in ES3. The putative CSC markers CD133, CD44 and ALDH expression were higher in spheres. The expression of estrogen receptor (ER)alpha and P53 decreased in spheres, ER beta and progesterone receptor had no significant changes and beta-catenin showed a tendency to increase. There was a higher F-18-FDG uptake in spheres, which also showed a lower lactate production and an oxidative cytosol status. The tumorigenesis in vivo showed an earlier growth of tumours derived from ES3. Endometrial spheres presented self-renewal and differentiation capacity, expressed CSC markers and an undifferentiated phenotype, showing preference for oxidative metabolism.

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