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DNA Dynamics and Chromosome Structure

Multiple Functional Elements Comprise a Mammalian Chromosomal Replicator

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Pages 1832-1842 | Received 16 Jul 2002, Accepted 09 Dec 2002, Published online: 27 Mar 2023
 

Abstract

The structure of replication origins in metazoans is only nominally similar to that in model organisms, such as Saccharomyces cerevisiae. By contrast to the compact origins of budding yeast, in metazoans multiple elements act as replication start sites or control replication efficiency. We first reported that replication forks diverge from an origin 5′ to the human c-myc gene and that a 2.4-kb core fragment of the origin displays autonomous replicating sequence activity in plasmids and replicator activity at an ectopic chromosomal site. Here we have used clonal HeLa cell lines containing mutated c-myc origin constructs integrated at the same chromosomal location to identify elements important for DNA replication. Replication activity was measured before or after integration of the wild-type or mutated origins using PCR-based nascent DNA abundance assays. We find that deletions of several segments of the c-myc origin, including the DNA unwinding element and transcription factor binding sites, substantially reduced replicator activity, whereas deletion of the c-myc promoter P1 had only a modest effect. Substitution mutagenesis indicated that the sequence of the DNA unwinding element, rather than the spacing of flanking sequences, is critical. These results identify multiple functional elements essential for c-myc replicator activity.

ACKNOWLEDGMENTS

Financial support from the National Institutes of Health (GM53819 to M.L.) and the Wright State University School of Medicine is gratefully acknowledged.

We thank Yanlin Huang and David Kowalski (Department of Cancer Genetics, Roswell Park Cancer Institute) for access to the WEBTHERMODYN program and Steven Berberich and John Turchi for their comments on the manuscript.

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