A causal role for ERG in neoplastic transformation of prostate epithelium

  1. Olga Klezovitch*,
  2. Michael Risk*,,
  3. Ilsa Coleman*,
  4. Jared M. Lucas*,
  5. Manda Null*,
  6. Lawrence D. True,
  7. Peter S. Nelson*,,,§,,, and
  8. Valeri Vasioukhin*,,
  1. *Division of Human Biology, Fred Hutchinson Cancer Research Center, Seattle, WA 98109; and
  2. Departments of Urology,
  3. §Medicine,
  4. Genome Sciences,
  5. Pathology and Institute for Stem Cell and Regenerative Medicine, University of Washington, Seattle, WA 98195

  1. Communicated by Leland H. Hartwell, Fred Hutchinson Cancer Research Center, Seattle, WA, December 12, 2007 (received for review August 30, 2007)

Abstract

A significant proportion of human prostate cancers carry a chromosomal rearrangement resulting in the overexpression of the ETS transcription factor, ERG; however, the functional significance of this event is poorly understood. We report here that up-regulation of ERG transcript is sufficient for the initiation of prostate neoplasia. In agreement with measurements of ERG transcripts, we found that ERG protein is expressed in neoplastic human prostate epithelium. Overexpression of ERG in prostate cell lines increased cell invasion. Moreover, targeted expression of this transcript in vivo in luminal prostate epithelial cells of transgenic mice results in initiation of prostate neoplasia observed as the development of focal precancerous prostatic intraepithelial neoplasia (PIN). Similar to human cancers, luminal epithelial cells in these PIN lesions displace diminishing in numbers basal epithelial cells and establish direct contact with the stromal cell compartment. Loss of basal cells is considered to be one of the critical hallmarks of human prostate cancer; however, the mechanisms responsible for this event were unknown. We propose that up-regulation of ERG in human prostate cancer activates cell invasion programs that subsequently displace basal cells by neoplastic epithelium. Our data demonstrate that ERG plays an important causal role in the transformation of prostate epithelium and should be considered as a target for prevention or early therapeutic intervention.

Footnotes

  • To whom correspondence may be addressed. E-mail: pnelson{at}fhcrc.org or vvasiouk{at}fhcrc.org

  • Author contributions: O.K., P.S.N., and V.V. designed research; O.K., M.R., I.C., J.M.L., M.N., and L.D.T. performed research; O.K., L.D.T., P.S.N., and V.V. analyzed data; and O.K., P.S.N., and V.V. wrote the paper.

  • The authors declare no conflict of interest.

  • This article contains supporting information online at www.pnas.org/cgi/content/full/0711711105/DC1.

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  1. Published online before print February 1, 2008, doi: 10.1073/pnas.0711711105 PNAS February 12, 2008 vol. 105 no. 6 2105-2110
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