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Multi-step Loading of Human Minichromosome Maintenance Proteins in Live Human Cells
Authors:Ioanna-Eleni Symeonidou  Panagiotis Kotsantis  Vassilis Roukos  Maria-Anna Rapsomaniki  Hernán E Grecco  Philippe Bastiaens  Stavros Taraviras  Zoi Lygerou
Institution:From the Laboratory of General Biology and ;Laboratory of Physiology, School of Medicine, University of Patras, 26500 Rio, Patras, Greece and ;the §Department of Systemic Cell Biology, Max Planck Institute of Molecular Physiology, Otto-Hahn-Strasse 11, 44227 Dortmund, Germany
Abstract:Once-per-cell cycle replication is regulated through the assembly onto chromatin of multisubunit protein complexes that license DNA for a further round of replication. Licensing consists of the loading of the hexameric MCM2–7 complex onto chromatin during G1 phase and is dependent on the licensing factor Cdt1. In vitro experiments have suggested a two-step binding mode for minichromosome maintenance (MCM) proteins, with transient initial interactions converted to stable chromatin loading. Here, we assess MCM loading in live human cells using an in vivo licensing assay on the basis of fluorescence recovery after photobleaching of GFP-tagged MCM protein subunits through the cell cycle. We show that, in telophase, MCM2 and MCM4 maintain transient interactions with chromatin, exhibiting kinetics similar to Cdt1. These are converted to stable interactions from early G1 phase. The immobile fraction of MCM2 and MCM4 increases during G1 phase, suggestive of reiterative licensing. In late G1 phase, a large fraction of MCM proteins are loaded onto chromatin, with maximal licensing observed just prior to S phase onset. Fluorescence loss in photobleaching experiments show subnuclear concentrations of MCM-chromatin interactions that differ as G1 phase progresses and do not colocalize with sites of DNA synthesis in S phase.
Keywords:Cell Biology  Cell Cycle  Chromatin  DNA Replication  Imaging  Fluorescence Recovery after Photobleaching  Licensing  Live-cell Imaging  Minichromosome Maintenance Complex  Genome Stability
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