Single-Molecule Studies of Origin Licensing Reveal Mechanisms Ensuring Bidirectional Helicase Loading

Author(s)

Friedman, Larry J.; Gelles, Jeff; Ticau, Simina; Ivica, Nikola; Bell, Stephen P

Abstract

Loading of the ring-shaped Mcm2–7 replicative helicase around DNA licenses eukaryotic origins of replication. During loading, Cdc6, Cdt1, and the origin-recognition complex (ORC) assemble two heterohexameric Mcm2–7 complexes into a head-to-head double hexamer that facilitates bidirectional replication initiation. Using multi-wavelength single-molecule fluorescence to monitor the events of helicase loading, we demonstrate that double-hexamer formation is the result of sequential loading of individual Mcm2–7 complexes. Loading of each Mcm2–7 molecule involves the ordered association and dissociation of distinct Cdc6 and Cdt1 proteins. In contrast, one ORC molecule directs loading of both helicases in each double hexamer. Based on single-molecule FRET, arrival of the second Mcm2–7 results in rapid double-hexamer formation that anticipates Cdc6 and Cdt1 release, suggesting that Mcm-Mcm interactions recruit the second helicase. Our findings reveal the complex protein dynamics that coordinate helicase loading and indicate that distinct mechanisms load the oppositely oriented helicases that are central to bidirectional replication initiation.

Date issued

2015-04

URI

http://hdl.handle.net/1721.1/105277

Department

Massachusetts Institute of Technology. Department of Biology

Journal

Cell

Publisher

Elsevier

Citation

Ticau, Simina, Larry J. Friedman, Nikola A. Ivica, Jeff Gelles, and Stephen P. Bell. “Single-Molecule Studies of Origin Licensing Reveal Mechanisms Ensuring Bidirectional Helicase Loading.” Cell 161, no. 3 (April 2015): 513–525.

Version: Author's final manuscript

ISSN

00928674