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Metastasis: tumor cells becoming MENAcing

Journal

TRENDS IN CELL BIOLOGY
Volume 21, Issue 2, Pages 81-90

Publisher

ELSEVIER SCIENCE LONDON
DOI: 10.1016/j.tcb.2010.10.001

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Funding

  1. National Cancer Institute [CA100324, CA150344, CA113395, CA126511]
  2. National Institutes of Health [GM58801]
  3. Integrated Cancer Biology Program [1-U54-CA11296]
  4. Ludwig Center for Metastasis Research at MIT

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During breast cancer metastasis cells emigrate from the primary tumor to the bloodstream, and this carries them to distant sites where they infiltrate and sometimes form metastases within target organs. These cells must penetrate the dense extracellular matrix comprising the basement membrane of the mammary duct/acinus and migrate toward blood and lymphatic vessels, processes that mammary tumor cells execute primarily using epidermal growth factor (EGF)-dependent protrusive and migratory activity. Here, we focus on how the actin regulatory protein Mena affects EGF-elicited movement, invasion and metastasis. Recent findings indicate that, in invasive migratory tumor cells, Mena isoforms that endow heightened sensitivity to EGF and increased protrusive and migratory abilities are upregulated, whereas other isoforms are selectively downregulated. This change in Mena isoform expression enables tumor cells to invade in response to otherwise benign EGF stimulus levels and could offer an opportunity to identify metastatic risk in patients.

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