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Science 28 October 1994:
Vol. 266. no. 5185, pp. 621 - 628
DOI: 10.1126/science.7939715

Articles

Science, Vol 266, Issue 5185, 621-628
Copyright © 1994 by American Association for the Advancement of Science


articles

Formation of a monomeric DNA binding domain by Skn-1 bZIP and homeodomain elements

TK Blackwell, B Bowerman, Priess JR, and H Weintraub

Department of Basic Sciences, Fred Hutchinson Cancer Research Center, Seattle, WA 98104.

Maternally expressed Skn-1 protein is required for the correct specification of certain blastomere fates in early Caenorhabditis elegans embryos. Skn-1 contains a basic region similar to those of basic leucine zipper (bZIP) proteins but, paradoxically, it lacks a leucine zipper dimerization segment. Random sequence selection methods were used to show that Skn-1 binds to specific DNA sequences as a monomer. The Skn-1 basic region lies at the carboxyl terminus of an 85-amino acid domain that binds preferentially to a bZIP half-site and also recognizes adjacent 5' AT-rich sequences in the minor groove, apparently with an amino (NH2)-terminal "arm" related to those of homeodomain proteins. The intervening residues appear to stabilize interactions of these two subdomains with DNA. The Skn-1 DNA binding domain thus represents an alternative strategy for promoting binding of a basic region segment recognition helix to its cognate half-site. The results point to an underlying modularity in subdomains within established DNA binding domains.


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