Genetics, Vol. 156, 677-686, October 2000, Copyright © 2000

Regulation by Homeoproteins: A Comparison of Deformed-Responsive Elements

Jeffrey A. Pedersona, James W. LaFollettea, Cornelius Grossb, Alexey Veraksab, William McGinnisb, and James W. Mahaffeya
a Department of Genetics, North Carolina State University, Raleigh, North Carolina 27695-7614
b Department of Biology, University of California, San Diego, California 92093

Corresponding author: James W. Mahaffey, Department of Genetics, North Carolina State University, Raleigh, NC 27695-7614., jim_mahaffey{at}ncsu.edu (E-mail)

Communicating editor: T. C. KAUFMAN

Homeotic genes of Drosophila melanogaster encode transcription factors that specify segment identity by activating the appropriate set of target genes required to produce segment-specific characteristics. Advances in understanding target gene selection have been hampered by the lack of genes known to be directly regulated by the HOM-C proteins. Here we present evidence that the gene 1.28 is likely to be a direct target of Deformed in the maxillary segment. We identified a 664-bp Deformed Response Element (1.28 DRE) that directs maxillary-specific expression of a reporter gene in transgenic embryos. The 1.28 DRE contains in vitro binding sites for Deformed and DEAF-1. The Deformed binding sites do not have the consensus sequence for cooperative binding with the cofactor Extradenticle, and we do not detect cooperative binding to these sites, though we cannot rule out an independent role for Extradenticle. Removing the four Deformed binding sites renders the 1.28 DRE inactive in vivo, demonstrating that these sites are necessary for activation of this enhancer element, and supporting the proposition that 1.28 is activated by Deformed. We show that the DEAF-1 binding region is not required for enhancer function. Comparisons of the 1.28 DRE with other known Deformed-responsive enhancers indicate that there are multiple ways to construct Deformed Response Elements.





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