| Literature DB >> 30232005 |
Roy Z Granit1, Hadas Masury1, Reba Condiotti1, Yaakov Fixler1, Yael Gabai1, Tzofia Glikman1, Simona Dalin1, Eitan Winter2, Yuval Nevo2, Einat Carmon3, Tamar Sella4, Amir Sonnenblick5, Tamar Peretz5, Ulrich Lehmann6, Keren Paz7, Federica Piccioni8, Aviv Regev9, David E Root8, Ittai Ben-Porath10.
Abstract
Differentiation events contribute to phenotypic cellular heterogeneity within tumors and influence disease progression and response to therapy. Here, we dissect mechanisms controlling intratumoral heterogeneity within triple-negative basal-like breast cancers. Tumor cells expressing the cytokeratin K14 possess a differentiation state that is associated with that of normal luminal progenitors, and K14-negative cells are in a state closer to that of mature luminal cells. We show that cells can transition between these states through asymmetric divisions, which produce one K14+ and one K14- daughter cell, and that these asymmetric divisions contribute to the generation of cellular heterogeneity. We identified several regulators that control the proportion of K14+ cells in the population. EZH2 and Notch increase the numbers of K14+ cells and their rates of symmetric divisions, and FOXA1 has an opposing effect. Our findings demonstrate that asymmetric divisions generate differentiation transitions and heterogeneity, and identify pathways that control breast cancer cellular composition.Entities:
Keywords: EZH2; FOXA1; KLF5; NFIB; Notch; asymmetric divisions; basal-like breast cancer; mammary progenitor cells; triple-negative breast cancer; tumor heterogeneity
Year: 2018 PMID: 30232005 DOI: 10.1016/j.celrep.2018.08.053
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423