Drosophila ORC specifically binds to ACE3, an origin of DNA replication control element

  1. Richard J. Austin,
  2. Terry L. Orr-Weaver, and
  3. Stephen P. Bell
  1. Department of Biology, Massachusetts Institute of Technology, and The Whitehead Institute, Cambridge, Massachusetts 02139 USA

Abstract

In the yeast Saccharomyces cerevisiae, sequence-specific DNA binding by the origin recognition complex (ORC) is responsible for selecting origins of DNA replication. In metazoans, origin selection is poorly understood and it is unknown whether specific DNA binding by metazoan ORC controls replication. To address this problem, we used in vivo and in vitro approaches to demonstrate that Drosophila ORC (DmORC) binds to replication elements that direct repeated initiation of replication to amplify the Drosophila chorion gene loci in the follicle cells of egg chambers. Using immunolocalization, we observe that ACE3, a 440-bp chorion element that contains information sufficient to drive amplification, directs DmORC localization in follicle cells. Similarly, in vivo cross-linking and chromatin immunoprecipitation assays demonstrate association of DmORC with both ACE3 and two other amplification control elements, AER-d and ACE1. To demonstrate that the in vivo localization of DmORC is related to its DNA-binding properties, we find that purified DmORC binds to ACE3 and AER-d in vitro, and like its S. cerevisiae counterpart, this binding is dependent on ATP. Our findings suggest that sequence-specific DNA binding by ORC regulates initiation of metazoan DNA replication. Furthermore, adaptation of this experimental approach will allow for the identification of additional metazoan ORC DNA-binding sites and potentially origins of replication.

Keywords

Footnotes

  • Corresponding author.

  • E-MAIL spbell{at}mit.edu; FAX (617) 253-8699

    • Received July 7, 1999.
    • Accepted August 26, 1999.
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