4.6 Article

Structural Insights into the Autoregulation and Cooperativity of the Human Transcription Factor Ets-2

Journal

JOURNAL OF BIOLOGICAL CHEMISTRY
Volume 290, Issue 13, Pages 8539-8549

Publisher

AMER SOC BIOCHEMISTRY MOLECULAR BIOLOGY INC
DOI: 10.1074/jbc.M114.619270

Keywords

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Funding

  1. Structural Genomics Consortium, a registered charity [1097737]
  2. AbbVie
  3. Bayer Pharma AG
  4. Boehringer Ingelheim
  5. Canada Foundation for Innovation
  6. Genome Canada
  7. GlaxoSmithKline
  8. Janssen
  9. Lilly Canada
  10. Novartis Research Foundation
  11. Ontario Ministry of Economic Development and Innovation
  12. Pfizer
  13. Takeda
  14. Wellcome Trust [092809/Z/10/Z]

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Ets-2, like its closely related homologue Ets-1, is a member of the Ets family of DNA binding transcription factors. Both proteins are subject to multiple levels of regulation of their DNA binding and transactivation properties. One such regulatory mechanism is the presence of an autoinhibitory module, which in Ets-1 allosterically inhibits the DNA binding activity. This inhibition can be relieved by interaction with protein partners or cooperative binding to closely separated Ets binding sites in a palindromic arrangement. In this study we describe the 2.5 angstrom resolution crystal structure of a DNA complex of the Ets-2 Ets domain. The Ets domain crystallized with two distinct species in the asymmetric unit, which closely resemble the autoinhibited and DNA bound forms of Ets-1. This discovery prompted us to re-evaluate the current model for the autoinhibitory mechanism and the structural basis for cooperative DNA binding. In contrast to Ets-1, in which the autoinhibition is caused by a combination of allosteric and steric mechanisms, we were unable to find clear evidence for the allosteric mechanism in Ets-2. We also demonstrated two possibly distinct types of cooperative binding to substrates with Ets binding motifs separated by four and six base pairs and suggest possible molecular mechanisms for this behavior.

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