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Published September 2009 | Published + Supplemental Material
Journal Article Open

Dynamic Interpretation of Hedgehog Signaling in the Drosophila Wing Disc

Abstract

Morphogens are classically defined as molecules that control patterning by acting at a distance to regulate gene expression in a concentration-dependent manner. In the Drosophila wing imaginal disc, secreted Hedgehog (Hh) forms an extracellular gradient that organizes patterning along the anterior–posterior axis and specifies at least three different domains of gene expression. Although the prevailing view is that Hh functions in the Drosophila wing disc as a classical morphogen, a direct correspondence between the borders of these patterns and Hh concentration thresholds has not been demonstrated. Here, we provide evidence that the interpretation of Hh signaling depends on the history of exposure to Hh and propose that a single concentration threshold is sufficient to support multiple outputs. Using mathematical modeling, we predict that at steady state, only two domains can be defined in response to Hh, suggesting that the boundaries of two or more gene expression patterns cannot be specified by a static Hh gradient. Computer simulations suggest that a spatial "overshoot" of the Hh gradient occurs, i.e., a transient state in which the Hh profile is expanded compared to the Hh steady-state gradient. Through a temporal examination of Hh target gene expression, we observe that the patterns initially expand anteriorly and then refine, providing in vivo evidence for the overshoot. The Hh gene network architecture suggests this overshoot results from the Hh-dependent up-regulation of the receptor, Patched (Ptc). In fact, when the network structure was altered such that the ptc gene is no longer up-regulated in response to Hh-signaling activation, we found that the patterns of gene expression, which have distinct borders in wild-type discs, now overlap. Our results support a model in which Hh gradient dynamics, resulting from Ptc up-regulation, play an instructional role in the establishment of patterns of gene expression.

Additional Information

© 2009 Nahmad, Stathopoulos. Received March 4, 2009; Accepted August 13, 2009; Published September 29, 2009. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. Funding: This work was funded by grants from the National Institutes of Health to John Doyle (R01-GM078992) and the Searle Scholar Foundation to AS. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript. Competing Interests: The authors have declared that no competing interests exist. We are grateful to John Doyle for helpful discussions and to Suzzane Eaton for sharing information about the nature of the hhts2 allele. We also thank Michele Crozatier, Patrick O'Farrell, and Ed Laufer for providing antibodies, as well as Gary Stuhl, Tom Kornberg, Kristi Wharton, and Kevin Moses for providing fly stocks, and John Doyle, Arthur Lander, Kai Zinn, Hilary Ashe, and members of the Stathopoulos laboratory for comments on the manuscript.

Attached Files

Published - Nahmad2009p6210Plos_Biol.pdf

Supplemental Material - journal.pbio.1000202.s001.tif

Supplemental Material - journal.pbio.1000202.s002.tif

Supplemental Material - journal.pbio.1000202.s003.tif

Supplemental Material - journal.pbio.1000202.s004.tif

Supplemental Material - journal.pbio.1000202.s005.tif

Supplemental Material - journal.pbio.1000202.s006.tif

Supplemental Material - journal.pbio.1000202.s007.doc

Supplemental Material - journal.pbio.1000202.s008.doc

Supplemental Material - journal.pbio.1000202.s009.doc

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