Article
- The EMBO Journal (2004) 23, 191 - 201
- doi:10.1038/sj.emboj.7600029
Published online: 11 December 2003
Subject Category:
An episomal mammalian replicon: sequence-independent binding of the origin recognition complex
Daniel Schaarschmidt1, Jens Baltin1, Isa M Stehle2, Hans J Lipps2 and Rolf Knippers1
- Department of Biology, Universität Konstanz, Konstanz, Germany
- Institute of Cell Biology, Universität Witten/Herdecke, Witten, Germany
Correspondence to:
Daniel Schaarschmidt, Department of Biology, Universität Konstanz, Universitätsstrase 10, Konstanz D-78464, Germany. Tel.: 49 7531 88 2127; Fax: 49 7531 88 4036; E-mail: daniel.schaarschmidt@uni-konstanz.de
Received 10 September 2003; Accepted 17 November 2003
Abstract
An extrachromosomally replicating plasmid was used to investigate the specificity by which the origin recognition complex (ORC) interacts with DNA sequences in mammalian cells in vivo. We first showed that the plasmid pEPI-1 replicates semiconservatively in a once-per-cell-cycle manner and is stably transmitted over many cell generations in culture without selection. Chromatin immunoprecipitations and quantitative polymerase chain reaction analysis revealed that, in G1-phase cells, Orc1 and Orc2, as well as Mcm3, another component of the prereplication complex, are bound to multiple sites on the plasmid. These binding sites are functional because they show the S-phase-dependent dissociation of Orc1 and Mcm3 known to be characteristic for prereplication complexes in mammalian cells. In addition, we identified replicative nascent strands and showed that they correspond to many plasmid DNA regions. This work has implications for current models of replication origins in mammalian systems. It indicates that specific DNA sequences are not required for the chromatin binding of ORC in vivo. The conclusion is that epigenetic mechanisms determine the sites where mammalian DNA replication is initiated.
Keywords:
- initiation of DNA replication,
- origin of replication,
- mammalian episome
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