miR-22 represses cancer progression by inducing cellular senescence-Reference-Cited by-同舟云学术

miR-22 represses cancer progression by inducing cellular senescence

Published:2011-04-18 Issue:2 Volume:193 Page:409-424
ISSN:1540-8140
Container-title:Journal of Cell Biology
language:en
Short-container-title:

Author:

Xu Dan¹,Takeshita Fumitaka²,Hino Yumiko¹,Fukunaga Saori¹,Kudo Yasusei¹,Tamaki Aya¹,Matsunaga Junko¹,Takahashi Ryou-u²,Takata Takashi¹,Shimamoto Akira¹,Ochiya Takahiro²,Tahara Hidetoshi¹

Affiliation:

1. Department of Cellular and Molecular Biology and Department of Oral Maxillofacial Pathobiology, Graduate School of Biomedical Science, Hiroshima University, Minami-ku, Hiroshima 734-8553, Japan

2. Division of Molecular and Cellular Medicine, National Cancer Center Research Institute, Chuo-ku, Tokyo 104-0045, Japan

Abstract

Cellular senescence acts as a barrier to cancer progression, and microRNAs (miRNAs) are thought to be potential senescence regulators. However, whether senescence-associated miRNAs (SA-miRNAs) contribute to tumor suppression remains unknown. Here, we report that miR-22, a novel SA-miRNA, has an impact on tumorigenesis. miR-22 is up-regulated in human senescent fibroblasts and epithelial cells but down-regulated in various cancer cell lines. miR-22 overexpression induces growth suppression and acquisition of a senescent phenotype in human normal and cancer cells. miR-22 knockdown in presenescent fibroblasts decreased cell size, and cells became more compact. miR-22–induced senescence also decreases cell motility and inhibits cell invasion in vitro. Synthetic miR-22 delivery suppresses tumor growth and metastasis in vivo by inducing cellular senescence in a mouse model of breast carcinoma. We confirmed that CDK6, SIRT1, and Sp1, genes involved in the senescence program, are direct targets of miR-22. Our study provides the first evidence that miR-22 restores the cellular senescence program in cancer cells and acts as a tumor suppressor.

Publisher

Rockefeller University Press

Subject

Cell Biology

Link

http://rupress.org/jcb/article-pdf/193/2/409/1351108/jcb_201010100.pdf

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