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      Cyclin B1–Cdk1 Activation Continues after Centrosome Separation to Control Mitotic Progression

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          There is no author summary for this article yet. Authors can add summaries to their articles on ScienceOpen to make them more accessible to a non-specialist audience.

          Abstract

          Activation of cyclin B1–cyclin-dependent kinase 1 (Cdk1), triggered by a positive feedback loop at the end of G2, is the key event that initiates mitotic entry. In metaphase, anaphase-promoting complex/cyclosome–dependent destruction of cyclin B1 inactivates Cdk1 again, allowing mitotic exit and cell division. Several models describe Cdk1 activation kinetics in mitosis, but experimental data on how the activation proceeds in mitotic cells have largely been lacking. We use a novel approach to determine the temporal development of cyclin B1–Cdk1 activity in single cells. By quantifying both dephosphorylation of Cdk1 and phosphorylation of the Cdk1 target anaphase-promoting complex/cyclosome 3, we disclose how cyclin B1–Cdk1 continues to be activated after centrosome separation. Importantly, we discovered that cytoplasmic cyclin B1–Cdk1 activity can be maintained even when cyclin B1 translocates to the nucleus in prophase. These experimental data are fitted into a model describing cyclin B1–Cdk1 activation in human cells, revealing a striking resemblance to a bistable circuit. In line with the observed kinetics, cyclin B1–Cdk1 levels required to enter mitosis are lower than the amount of cyclin B1–Cdk1 needed for mitotic progression. We propose that gradually increasing cyclin B1–Cdk1 activity after centrosome separation is critical to coordinate mitotic progression.

          Author Summary

          When active, the enzyme cyclin B1–cyclin-dependent kinase 1 (Cdk1) commits a growing cell to the process of mitotic cell division and chromosome separation. Cyclin B1–Cdk1 activation is controlled in many ways, but once its activity rises above a certain level, further activation of cyclin B1–Cdk1 is catalyzed by a positive-feedback loop. This generates highly active cyclin B1–Cdk1 and triggers the start of mitosis, which can only be completed when cyclin B1–Cdk1 activity is properly shut off again. However, it is not clear how cyclin B1–Cdk1 activity develops in human cells or how the switch between its inactive and active states is controlled. Our work combines activation measurements with a kinetic model to study how cyclin B1–Cdk1 activity accumulates just before and during mitosis. We show that cyclin B1–Cdk1 activity develops gradually in early mitosis and that different activity levels are required for initiation of, and progression through, mitosis. We also demonstrate that once cyclin B1–Cdk1 activation is truly launched, it is bound to continue and will not lightly drop back again. We propose that the successive cyclin B1–Cdk1 activity levels by themselves may coordinate the progression through the distinct phases of mitosis.

          Abstract

          The gradual increase of cyclin B1-Cdk1 activation in human cells is proposed to be critical for the progression of mitosis.

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          Self-perpetuating states in signal transduction: positive feedback, double-negative feedback and bistability.

          James Ferrell (2002)
          Cell signaling systems that contain positive-feedback loops or double-negative feedback loops can, in principle, convert graded inputs into switch-like, irreversible responses. Systems of this sort are termed "bistable". Recently, several groups have engineered artificial bistable systems into Escherichia coli and Saccharomyces cerevisiae, and have shown that the systems exhibit interesting and potentially useful properties. In addition, two naturally occurring signaling systems, the p42 mitogen-activated protein kinase and c-Jun amino-terminal kinase pathways in Xenopus oocytes, have been shown to exhibit bistable responses. Here we review the basic properties of bistable circuits, the requirements for construction of a satisfactory bistable switch, and the recent progress towards constructing and analysing bistable signaling systems.
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            Universal control mechanism regulating onset of M-phase.

            P Nurse (1990)
            The onset of M-phase is regulated by a mechanism common to all eukaryotic cells. Entry into M-phase is determined by activation of the p34cdc2 protein kinase which requires p34cdc2 dephosphorylation and association with cyclin.
            Article 0 comments Cited 247 times – based on 0 reviews     Review now
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              Targets of the cyclin-dependent kinase Cdk1.

              Jeffrey Ubersax, Erika Woodbury, Phuong N. Quang (2003)
              The events of cell reproduction are governed by oscillations in the activities of cyclin-dependent kinases (Cdks). Cdks control the cell cycle by catalysing the transfer of phosphate from ATP to specific protein substrates. Despite their importance in cell-cycle control, few Cdk substrates have been identified. Here, we screened a budding yeast proteomic library for proteins that are directly phosphorylated by Cdk1 in whole-cell extracts. We identified about 200 Cdk1 substrates, several of which are phosphorylated in vivo in a Cdk1-dependent manner. The identities of these substrates reveal that Cdk1 employs a global regulatory strategy involving phosphorylation of other regulatory molecules as well as phosphorylation of the molecular machines that drive cell-cycle events. Detailed analysis of these substrates is likely to yield important insights into cell-cycle regulation.
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                Author and article information

                Contributors
                : Role: Academic Editor
                Journal
                Journal ID (nlm-ta): PLoS Biol
                Journal ID (publisher-id): pbio
                Title: PLoS Biology
                Publisher: Public Library of Science (San Francisco, USA )
                ISSN (Print): 1544-9173
                ISSN (Electronic): 1545-7885
                Publication date (Print): May 2007
                Publication date (Electronic): 1 May 2007
                Volume: 5
                Issue: 5
                Electronic Location Identifier: e123
                Affiliations
                [1 ] Department of Cell and Molecular Biology, Karolinska Institutet, Stockholm, Sweden
                [2 ] Division of Molecular Biology/P2, The Netherlands Cancer Institute, Amsterdam, The Netherlands
                Dana-Farber Cancer Institute, United States of America
                Author notes
                * To whom correspondence should be addressed. E-mail: a.lindqvist@ 123456umcutrecht.nl
                Article
                Publisher ID: 06-PLBI-RA-1260R3 Serial Item and Contribution ID: plbi-05-05-17
                DOI: 10.1371/journal.pbio.0050123
                PMC ID: 1858714
                PubMed ID: 17472438
                SO-VID: 70c61c21-9470-45a9-808a-a991d71628f1
                Copyright © Copyright: © 2007 Lindqvist et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
                History
                Date received : 14 July 2006
                Date accepted : 5 March 2007
                Page count
                Pages: 11
                Categories
                Subject: Research Article
                Subject: Biophysics
                Subject: In Vitro
                Custom metadata
                citation Lindqvist A, van Zon W, Karlsson Rosenthal C, Wolthuis RMF (2007) Cyclin B1–Cdk1 activation continues after centrosome separation to control mitotic progression. PLoS Biol 5(5): e123. doi: 10.1371/journal.pbio.0050123

                ScienceOpen disciplines: Life sciences
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                ScienceOpen disciplines: Life sciences

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