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Hypoxia promotes a dedifferentiated phenotype in ductal breast carcinoma in situ.
202
Citations
17
References
2003
Year
Breast OncologyPathologyCell DeathCell ProliferationCancer BiologyMammary Gland DevelopmentTumor BiologyDuctal Breast CarcinomaHypoxia InducesOncologyCancer Cell BiologyStem CellsRadiation OncologyCancer ResearchHealth SciencesHypoxia (Medicine)Dedifferentiated PhenotypeCell BiologyEndocrine-related CancerCentral NecrosisBreast CancerMedicine
In cultured neuroblastoma cells, hypoxia induces a dedifferentiated phenotype. We tested whether hypoxia-induced dedifferentiation also occurs in vivo in mammary ductal carcinoma in situ with its well-defined lesions and distinct areas of necrosis. Ductal carcinoma in situ cells surrounding the central necrosis have high hypoxia inducible factor-1alpha protein levels, down-regulated estrogen receptor-alpha, and increased expression of the epithelial breast stem cell marker cytokeratin 19; lose their polarization; and acquire an increased nucleus/cytoplasm ratio, hallmarks of poor architectural and cellular differentiation. The hypoxia-induced changes were confirmed in cultured breast cancer cells. We propose that hypoxia-induced dedifferentiation is a mechanism that promotes tumor progression in breast cancer.
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