| Literature DB >> 36050483 |
Ana Rita Nobre1,2,3, Erica Dalla4, Jihong Yang5,6, Xin Huang5, Lena Wullkopf4, Emma Risson4, Pedram Razghandi7,8, Melisa Lopez Anton4, Wei Zheng7,8, Jose A Seoane9,10, Christina Curtis10, Ephraim Kenigsberg11,12,13, Jianlong Wang5, Julio A Aguirre-Ghiso14,15,16,17,18,19,20.
Abstract
Increasing evidence shows that cancer cells can disseminate from early evolved primary lesions much earlier than the classical metastasis models predicted. Here, we reveal at a single-cell resolution that mesenchymal-like (M-like) and pluripotency-like programs coordinate dissemination and a long-lived dormancy program of early disseminated cancer cells (DCCs). The transcription factor ZFP281 induces a permissive state for heterogeneous M-like transcriptional programs, which associate with a dormancy signature and phenotype in vivo. Downregulation of ZFP281 leads to a loss of an invasive, M-like dormancy phenotype and a switch to lung metastatic outgrowth. We also show that FGF2 and TWIST1 induce ZFP281 expression to induce the M-like state, which is linked to CDH1 downregulation and upregulation of CDH11. We found that ZFP281 not only controls the early dissemination of cancer cells but also locks early DCCs in a dormant state by preventing the acquisition of an epithelial-like proliferative program and consequent metastases outgrowth.Entities:
Year: 2022 PMID: 36050483 DOI: 10.1038/s43018-022-00424-8
Source DB: PubMed Journal: Nat Cancer ISSN: 2662-1347