| Literature DB >> 27926867 |
Valentine Comaills1, Lilian Kabeche2, Robert Morris2, Rémi Buisson2, Min Yu2, Marissa Wells Madden2, Joseph A LiCausi2, Myriam Boukhali2, Ken Tajima1, Shiwei Pan2, Nicola Aceto2, Srinjoy Sil2, Yu Zheng3, Tilak Sundaresan4, Toshifumi Yae1, Nicole Vincent Jordan3, David T Miyamoto4, David T Ting4, Sridhar Ramaswamy4, Wilhelm Haas2, Lee Zou5, Daniel A Haber6, Shyamala Maheswaran7.
Abstract
TGF-β secreted by tumor stroma induces epithelial-to-mesenchymal transition (EMT) in cancer cells, a reversible phenotype linked to cancer progression and drug resistance. However, exposure to stromal signals may also lead to heritable changes in cancer cells, which are poorly understood. We show that epithelial cells failing to undergo proliferation arrest during TGF-β-induced EMT sustain mitotic abnormalities due to failed cytokinesis, resulting in aneuploidy. This genomic instability is associated with the suppression of multiple nuclear envelope proteins implicated in mitotic regulation and is phenocopied by modulating the expression of LaminB1. While TGF-β-induced mitotic defects in proliferating cells are reversible upon its withdrawal, the acquired genomic abnormalities persist, leading to increased tumorigenic phenotypes. In metastatic breast cancer patients, increased mesenchymal marker expression within single circulating tumor cells is correlated with genomic instability. These observations identify a mechanism whereby microenvironment-derived signals trigger heritable genetic changes within cancer cells, contributing to tumor evolution.Entities:
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Year: 2016 PMID: 27926867 PMCID: PMC5320932 DOI: 10.1016/j.celrep.2016.11.022
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423