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Cdc25b and Cdc25c Differ Markedly in Their Properties as Initiators of Mitosis

We have used time-lapse fluorescence microscopy to study the properties of the Cdc25B and Cdc25C phosphatases that have both been implicated as initiators of mitosis in human cells. To differentiate between the functions of the two proteins, we have microinjected expression constructs encoding Cdc25...

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Autores principales: Karlsson, Christina, Katich, Stephanie, Hagting, Anja, Hoffmann, Ingrid, Pines, Jonathon
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 1999
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2150562/
https://www.ncbi.nlm.nih.gov/pubmed/10444066
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author Karlsson, Christina
Katich, Stephanie
Hagting, Anja
Hoffmann, Ingrid
Pines, Jonathon
author_facet Karlsson, Christina
Katich, Stephanie
Hagting, Anja
Hoffmann, Ingrid
Pines, Jonathon
author_sort Karlsson, Christina
collection PubMed
description We have used time-lapse fluorescence microscopy to study the properties of the Cdc25B and Cdc25C phosphatases that have both been implicated as initiators of mitosis in human cells. To differentiate between the functions of the two proteins, we have microinjected expression constructs encoding Cdc25B or Cdc25C or their GFP-chimeras into synchronized tissue culture cells. This assay allows us to express the proteins at defined points in the cell cycle. We have followed the microinjected cells by time-lapse microscopy, in the presence or absence of DNA synthesis inhibitors, and assayed whether they enter mitosis prematurely or at the correct time. We find that overexpressing Cdc25B alone rapidly causes S phase and G2 phase cells to enter mitosis, whether or not DNA replication is complete, whereas overexpressing Cdc25C does not cause premature mitosis. Overexpressing Cdc25C together with cyclin B1 does shorten the G2 phase and can override the unreplicated DNA checkpoint, but much less efficiently than overexpressing Cdc25B. These results suggest that Cdc25B and Cdc25C do not respond identically to the same cell cycle checkpoints. This difference may be related to the differential localization of the proteins; Cdc25C is nuclear throughout interphase, whereas Cdc25B is nuclear in the G1 phase and cytoplasmic in the S and G2 phases. We have found that the change in subcellular localization of Cdc25B is due to nuclear export and that this is dependent on cyclin B1. Our data suggest that although both Cdc25B and Cdc25C can promote mitosis, they are likely to have distinct roles in the controlling the initiation of mitosis.
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spelling pubmed-21505622008-05-01 Cdc25b and Cdc25c Differ Markedly in Their Properties as Initiators of Mitosis Karlsson, Christina Katich, Stephanie Hagting, Anja Hoffmann, Ingrid Pines, Jonathon J Cell Biol Original Article We have used time-lapse fluorescence microscopy to study the properties of the Cdc25B and Cdc25C phosphatases that have both been implicated as initiators of mitosis in human cells. To differentiate between the functions of the two proteins, we have microinjected expression constructs encoding Cdc25B or Cdc25C or their GFP-chimeras into synchronized tissue culture cells. This assay allows us to express the proteins at defined points in the cell cycle. We have followed the microinjected cells by time-lapse microscopy, in the presence or absence of DNA synthesis inhibitors, and assayed whether they enter mitosis prematurely or at the correct time. We find that overexpressing Cdc25B alone rapidly causes S phase and G2 phase cells to enter mitosis, whether or not DNA replication is complete, whereas overexpressing Cdc25C does not cause premature mitosis. Overexpressing Cdc25C together with cyclin B1 does shorten the G2 phase and can override the unreplicated DNA checkpoint, but much less efficiently than overexpressing Cdc25B. These results suggest that Cdc25B and Cdc25C do not respond identically to the same cell cycle checkpoints. This difference may be related to the differential localization of the proteins; Cdc25C is nuclear throughout interphase, whereas Cdc25B is nuclear in the G1 phase and cytoplasmic in the S and G2 phases. We have found that the change in subcellular localization of Cdc25B is due to nuclear export and that this is dependent on cyclin B1. Our data suggest that although both Cdc25B and Cdc25C can promote mitosis, they are likely to have distinct roles in the controlling the initiation of mitosis. The Rockefeller University Press 1999-08-09 /pmc/articles/PMC2150562/ /pubmed/10444066 Text en © 1999 The Rockefeller University Press This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 4.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/4.0/).
spellingShingle Original Article
Karlsson, Christina
Katich, Stephanie
Hagting, Anja
Hoffmann, Ingrid
Pines, Jonathon
Cdc25b and Cdc25c Differ Markedly in Their Properties as Initiators of Mitosis
title Cdc25b and Cdc25c Differ Markedly in Their Properties as Initiators of Mitosis
title_full Cdc25b and Cdc25c Differ Markedly in Their Properties as Initiators of Mitosis
title_fullStr Cdc25b and Cdc25c Differ Markedly in Their Properties as Initiators of Mitosis
title_full_unstemmed Cdc25b and Cdc25c Differ Markedly in Their Properties as Initiators of Mitosis
title_short Cdc25b and Cdc25c Differ Markedly in Their Properties as Initiators of Mitosis
title_sort cdc25b and cdc25c differ markedly in their properties as initiators of mitosis
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2150562/
https://www.ncbi.nlm.nih.gov/pubmed/10444066
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