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Nature 451, 147-152 (10 January 2008) | doi:10.1038/nature06487; Received 1 September 2007; Accepted 21 November 2007

Endogenous human microRNAs that suppress breast cancer metastasis

Sohail F. Tavazoie1,2, Claudio Alarcón1, Thordur Oskarsson1, David Padua1, Qiongqing Wang1, Paula D. Bos1, William L. Gerald3 & Joan Massagué1

  1. Cancer Biology and Genetics Program,
  2. Department of Medicine,
  3. Department of Pathology, Memorial Sloan-Kettering Cancer Center, New York, New York 10021, USA

Correspondence to: Joan Massagué1 Correspondence and requests for materials should be addressed to J.M. (Email: massaguj@mskcc.org).

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A search for general regulators of cancer metastasis has yielded a set of microRNAs for which expression is specifically lost as human breast cancer cells develop metastatic potential. Here we show that restoring the expression of these microRNAs in malignant cells suppresses lung and bone metastasis by human cancer cells in vivo. Of these microRNAs, miR-126 restoration reduces overall tumour growth and proliferation, whereas miR-335 inhibits metastatic cell invasion. miR-335 regulates a set of genes whose collective expression in a large cohort of human tumours is associated with risk of distal metastasis. miR-335 suppresses metastasis and migration through targeting of the progenitor cell transcription factor SOX4 and extracellular matrix component tenascin C. Expression of miR-126 and miR-335 is lost in the majority of primary breast tumours from patients who relapse, and the loss of expression of either microRNA is associated with poor distal metastasis-free survival. miR-335 and miR-126 are thus identified as metastasis suppressor microRNAs in human breast cancer.

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