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Nature 451, 535-540 (31 January 2008) | doi:10.1038/nature06496; Received 2 August 2007; Accepted 20 November 2007; Published online 2 January 2008

Predicting expression patterns from regulatory sequence in Drosophila segmentation

Eran Segal1,3, Tali Raveh-Sadka1,3, Mark Schroeder2, Ulrich Unnerstall2 & Ulrike Gaul2

  1. Department of Computer Science and Applied Mathematics, Weizmann Institute of Science, Rehovot 76100, Israel
  2. Laboratory of Developmental Neurogenetics, Rockefeller University, New York, New York 10065, USA
  3. These authors contributed equally to this work.

Correspondence to: Eran Segal1,3Ulrike Gaul2 Correspondence and requests for materials should be addressed to E.S. (Email: eran@weizmann.ac.il) or U.G. (Email: gaul@mail.rockefeller.edu).

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The establishment of complex expression patterns at precise times and locations is key to metazoan development, yet a mechanistic understanding of the underlying transcription control networks is still missing. Here we describe a novel thermodynamic model that computes expression patterns as a function of cis-regulatory sequence and of the binding-site preferences and expression of participating transcription factors. We apply this model to the segmentation gene network of Drosophila melanogaster and find that it predicts expression patterns of cis-regulatory modules with remarkable accuracy, demonstrating that positional information is encoded in the regulatory sequence and input factor distribution. Our analysis reveals that both strong and weaker binding sites contribute, leading to high occupancy of the module DNA, and conferring robustness against mutation; short-range homotypic clustering of weaker sites facilitates cooperative binding, which is necessary to sharpen the patterns. Our computational framework is generally applicable to most protein–DNA interaction systems.

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