Deletion of an AML1-ETO C-terminal NcoR/SMRT-interacting region strongly induces leukemia development

  1. Ming Yan*,,
  2. Sebastien A. Burel*,,
  3. Luke F. Peterson*,,
  4. Eiki Kanbe*,
  5. Hiromi Iwasaki,
  6. Anita Boyapati*,
  7. Robert Hines*,
  8. Koichi Akashi, and
  9. Dong-Er Zhang*,§
  1. *Department of Molecular and Experimental Medicine, The Scripps Research Institute, La Jolla, CA 92037; and Department of Cancer Immunology and AIDS, Dana–Farber Cancer Institute, Boston, MA 02115

  1. Edited by Peter K. Vogt, The Scripps Research Institute, La Jolla, CA, and approved October 18, 2004 (received for review September 12, 2004)

Abstract

Normal blood-cell differentiation is controlled by regulated gene expression and signal transduction. Transcription deregulation due to chromosomal translocation is a common theme in hematopoietic neoplasms. AML1-ETO, which is a fusion protein generated by the 8;21 translocation that is commonly associated with the development of acute myeloid leukemia, fuses the AML1 runx family DNA-binding transcription factor to the ETO corepressor that associates with histone deacetylase complexes. Analyses have demonstrated that AML1-ETO blocks AML1 function and requires additional mutagenic events to promote leukemia. Here, we report that the loss of the molecular events of AML1-ETO C-terminal NCoR/SMRT-interacting domain transforms AML1-ETO into a potent leukemogenic protein. Contrary to full-length AML1-ETO, the truncated form promotes in vitro growth and does not obstruct the cell-cycle machinery. These observations suggest a previously uncharacterized mechanism of tumorigenesis, in which secondary mutation(s) in molecular events disrupting the function of a domain of the oncogene promote the development of malignancy.

Footnotes

  • § To whom correspondence should be addressed. E-mail: dzhang{at}scripps.edu.

  • M.Y., S.A.B., and L.F.P. contributed equally to the work.

  • This paper was submitted directly (Track II) to the PNAS office.

  • Abbreviations: AML, acute myeloid leukemia; En, embryonic day n; HA, hemagglutinin.

  • See Commentary on page 16985.

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  1. Published online before print November 29, 2004, doi: 10.1073/pnas.0406702101 PNAS December 7, 2004 vol. 101 no. 49 17186-17191
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