ORC binding to TRF2 stimulates OriP replication.
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Journal: 2006/September - EMBO Reports
ISSN: 1469-221X
Abstract:
In higher eukaryotes, the origin recognition complex (ORC) lacks sequence-specific DNA binding, and it remains unclear what other factors specify an origin of DNA replication. The Epstein-Barr virus origin of plasmid replication (OriP) recruits ORC, but the precise mechanism of ORC recruitment and origin activation is not clear. We now show that ORC is recruited selectively to the dyad symmetry (DS) region of OriP as a consequence of direct interactions with telomere repeat factor 2 (TRF2) and ORC1. TRF-binding sites within DS stimulate replication initiation and facilitate ORC recruitment in vitro and in vivo. TRF2, but not TRF1 or hRap1, recruits ORC from nuclear extracts. The amino-terminal domain of TRF2 associated with a specific region of ORC1 and was necessary for stimulation of DNA replication. These results support a model in which TRF2 stimulates OriP replication activity by direct binding with ORC subunits.
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EMBO Rep 7(7): 716-721
PMID: 16799465

ORC binding to TRF2 stimulates OriP replication

The Wistar Institute, 3601 Spruce Street, Philadelphia, Pennsylvania 19104, USA
Tel: +1 215 898 9491; Fax: +1 215 898 0663; E-mail: gro.ratsiw@namrebeil
These authors contributed equally to this work
Received 2006 Jan 13; Revised 2006 May 12; Accepted 2006 May 15.
Copyright © 2006, European Molecular Biology Organization

Abstract

In higher eukaryotes, the origin recognition complex (ORC) lacks sequence-specific DNA binding, and it remains unclear what other factors specify an origin of DNA replication. The Epstein–Barr virus origin of plasmid replication (OriP) recruits ORC, but the precise mechanism of ORC recruitment and origin activation is not clear. We now show that ORC is recruited selectively to the dyad symmetry (DS) region of OriP as a consequence of direct interactions with telomere repeat factor 2 (TRF2) and ORC1. TRF-binding sites within DS stimulate replication initiation and facilitate ORC recruitment in vitro and in vivo. TRF2, but not TRF1 or hRap1, recruits ORC from nuclear extracts. The amino-terminal domain of TRF2 associated with a specific region of ORC1 and was necessary for stimulation of DNA replication. These results support a model in which TRF2 stimulates OriP replication activity by direct binding with ORC subunits.

Keywords: ORC, TRF2, origin, replication, EBV
Abstract
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Acknowledgments

We acknowledge the technical support of Wistar Cancer Center Core Facilities, and financial support from the Leukemia Research Foundation (C.A.), the Leukemia-Lymphoma Society (Z.D.), the NIH Training Program in Genetics (5-T32-GM08216-18; J.N.), the Pennsylvania Department of Health, the DOD (DAMD17-03-1-0313) and the NIH (CA93606) to P.M.L.

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