• Title of article

    let-7 Regulates Self Renewal and Tumorigenicity of Breast Cancer Cells

  • Author/Authors

    Fengyan Yu، نويسنده , , Herui Yao، نويسنده , , Pengcheng Zhu، نويسنده , , Xiaoqin Zhang، نويسنده , , Qiuhui Pan، نويسنده , , Chang Gong، نويسنده , , Yijun Huang، نويسنده , , Xiaoqu Hu، نويسنده , , Fengxi Su، نويسنده , , Judy Lieberman، نويسنده , , Erwei Song، نويسنده ,

  • Issue Information
    هفته نامه با شماره پیاپی سال 2007
  • Pages
    15
  • From page
    1109
  • To page
    1123
  • Abstract
    Cancers may arise from rare self-renewing tumor-initiating cells (T-IC). However, how T-IC self renewal, multipotent differentiation, and tumorigenicity are maintained remains obscure. Because miRNAs can regulate cell-fate decisions, we compared miRNA expression in self-renewing and differentiated cells from breast cancer lines and in breast T-IC (BT-IC) and non-BT-IC from 1° breast cancers. let-7 miRNAs were markedly reduced in BT-IC and increased with differentiation. Infecting BT-IC with let-7-lentivirus reduced proliferation, mammosphere formation, and the proportion of undifferentiated cells in vitro and tumor formation and metastasis in NOD/SCID mice, while antagonizing let-7 by antisense oligonucleotides enhanced in vitro self renewal of non-T-IC. Increased let-7 paralleled reduced H-RAS and HMGA2, known let-7 targets. Silencing H-RAS in a BT-IC-enriched cell line reduced self renewal but had no effect on differentiation, while silencing HMGA2 enhanced differentiation but did not affect self renewal. Therefore let-7 regulates multiple BT-IC stem cell-like properties by silencing more than one target.
  • Journal title
    CELL
  • Serial Year
    2007
  • Journal title
    CELL
  • Record number

    1019050