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The Inhibition of Polo Kinase by Matrimony Maintains G2 Arrest in the Meiotic Cell Cycle

Many meiotic systems in female animals include a lengthy arrest in G2 that separates the end of pachytene from nuclear envelope breakdown (NEB). However, the mechanisms by which a meiotic cell can arrest for long periods of time (decades in human females) have remained a mystery. The Drosophila Matr...

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Autores principales: Xiang, Youbin, Takeo, Satomi, Florens, Laurence, Hughes, Stacie E, Huo, Li-Jun, Gilliland, William D, Swanson, Selene K, Teeter, Kathy, Schwartz, Joel W, Washburn, Michael P, Jaspersen, Sue L, Hawley, R. Scott
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2007
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2100146/
https://www.ncbi.nlm.nih.gov/pubmed/18052611
http://dx.doi.org/10.1371/journal.pbio.0050323
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author Xiang, Youbin
Takeo, Satomi
Florens, Laurence
Hughes, Stacie E
Huo, Li-Jun
Gilliland, William D
Swanson, Selene K
Teeter, Kathy
Schwartz, Joel W
Washburn, Michael P
Jaspersen, Sue L
Hawley, R. Scott
author_facet Xiang, Youbin
Takeo, Satomi
Florens, Laurence
Hughes, Stacie E
Huo, Li-Jun
Gilliland, William D
Swanson, Selene K
Teeter, Kathy
Schwartz, Joel W
Washburn, Michael P
Jaspersen, Sue L
Hawley, R. Scott
author_sort Xiang, Youbin
collection PubMed
description Many meiotic systems in female animals include a lengthy arrest in G2 that separates the end of pachytene from nuclear envelope breakdown (NEB). However, the mechanisms by which a meiotic cell can arrest for long periods of time (decades in human females) have remained a mystery. The Drosophila Matrimony (Mtrm) protein is expressed from the end of pachytene until the completion of meiosis I. Loss-of-function mtrm mutants result in precocious NEB. Coimmunoprecipitation experiments reveal that Mtrm physically interacts with Polo kinase (Polo) in vivo, and multidimensional protein identification technology mass spectrometry analysis reveals that Mtrm binds to Polo with an approximate stoichiometry of 1:1. Mutation of a Polo-Box Domain (PBD) binding site in Mtrm ablates the function of Mtrm and the physical interaction of Mtrm with Polo. The meiotic defects observed in mtrm/+ heterozygotes are fully suppressed by reducing the dose of polo(+), demonstrating that Mtrm acts as an inhibitor of Polo. Mtrm acts as a negative regulator of Polo during the later stages of G2 arrest. Indeed, both the repression of Polo expression until stage 11 and the inactivation of newly synthesized Polo by Mtrm until stage 13 play critical roles in maintaining and properly terminating G2 arrest. Our data suggest a model in which the eventual activation of Cdc25 by an excess of Polo at stage 13 triggers NEB and entry into prometaphase.
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spelling pubmed-21001462007-12-04 The Inhibition of Polo Kinase by Matrimony Maintains G2 Arrest in the Meiotic Cell Cycle Xiang, Youbin Takeo, Satomi Florens, Laurence Hughes, Stacie E Huo, Li-Jun Gilliland, William D Swanson, Selene K Teeter, Kathy Schwartz, Joel W Washburn, Michael P Jaspersen, Sue L Hawley, R. Scott PLoS Biol Research Article Many meiotic systems in female animals include a lengthy arrest in G2 that separates the end of pachytene from nuclear envelope breakdown (NEB). However, the mechanisms by which a meiotic cell can arrest for long periods of time (decades in human females) have remained a mystery. The Drosophila Matrimony (Mtrm) protein is expressed from the end of pachytene until the completion of meiosis I. Loss-of-function mtrm mutants result in precocious NEB. Coimmunoprecipitation experiments reveal that Mtrm physically interacts with Polo kinase (Polo) in vivo, and multidimensional protein identification technology mass spectrometry analysis reveals that Mtrm binds to Polo with an approximate stoichiometry of 1:1. Mutation of a Polo-Box Domain (PBD) binding site in Mtrm ablates the function of Mtrm and the physical interaction of Mtrm with Polo. The meiotic defects observed in mtrm/+ heterozygotes are fully suppressed by reducing the dose of polo(+), demonstrating that Mtrm acts as an inhibitor of Polo. Mtrm acts as a negative regulator of Polo during the later stages of G2 arrest. Indeed, both the repression of Polo expression until stage 11 and the inactivation of newly synthesized Polo by Mtrm until stage 13 play critical roles in maintaining and properly terminating G2 arrest. Our data suggest a model in which the eventual activation of Cdc25 by an excess of Polo at stage 13 triggers NEB and entry into prometaphase. Public Library of Science 2007-12 2007-12-04 /pmc/articles/PMC2100146/ /pubmed/18052611 http://dx.doi.org/10.1371/journal.pbio.0050323 Text en © 2007 Xiang et al. http://creativecommons.org/licenses/by/4.0/ 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 properly credited.
spellingShingle Research Article
Xiang, Youbin
Takeo, Satomi
Florens, Laurence
Hughes, Stacie E
Huo, Li-Jun
Gilliland, William D
Swanson, Selene K
Teeter, Kathy
Schwartz, Joel W
Washburn, Michael P
Jaspersen, Sue L
Hawley, R. Scott
The Inhibition of Polo Kinase by Matrimony Maintains G2 Arrest in the Meiotic Cell Cycle
title The Inhibition of Polo Kinase by Matrimony Maintains G2 Arrest in the Meiotic Cell Cycle
title_full The Inhibition of Polo Kinase by Matrimony Maintains G2 Arrest in the Meiotic Cell Cycle
title_fullStr The Inhibition of Polo Kinase by Matrimony Maintains G2 Arrest in the Meiotic Cell Cycle
title_full_unstemmed The Inhibition of Polo Kinase by Matrimony Maintains G2 Arrest in the Meiotic Cell Cycle
title_short The Inhibition of Polo Kinase by Matrimony Maintains G2 Arrest in the Meiotic Cell Cycle
title_sort inhibition of polo kinase by matrimony maintains g2 arrest in the meiotic cell cycle
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2100146/
https://www.ncbi.nlm.nih.gov/pubmed/18052611
http://dx.doi.org/10.1371/journal.pbio.0050323
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