Aurora-C Kinase Deficiency Causes Cytokinesis Failure in Meiosis I and Production of Large Polyploid Oocytes in Mice

We previously isolated Aurora-C/Aie1 in a screen for kinases expressed in mouse sperm and eggs. Here, we show the localization of endogenous Aurora-C and examine its roles during female mouse meiosis. Aurora-C was detected at the centromeres and along the chromosome arms in prometaphase I–metaphase...

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Autores principales: Yang, Kuo-Tai, Li, Shu-Kuei, Chang, Chih-Chieh, Tang, Chieh-Ju C., Lin, Yi-Nan, Lee, Sheng-Chung, Tang, Tang K.
Formato: Texto
Lenguaje:English
Publicado: The American Society for Cell Biology 2010
Materias:
Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2903667/
https://www.ncbi.nlm.nih.gov/pubmed/20484572
http://dx.doi.org/10.1091/mbc.E10-02-0170
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author Yang, Kuo-Tai
Li, Shu-Kuei
Chang, Chih-Chieh
Tang, Chieh-Ju C.
Lin, Yi-Nan
Lee, Sheng-Chung
Tang, Tang K.
author_facet Yang, Kuo-Tai
Li, Shu-Kuei
Chang, Chih-Chieh
Tang, Chieh-Ju C.
Lin, Yi-Nan
Lee, Sheng-Chung
Tang, Tang K.
author_sort Yang, Kuo-Tai
collection PubMed
description We previously isolated Aurora-C/Aie1 in a screen for kinases expressed in mouse sperm and eggs. Here, we show the localization of endogenous Aurora-C and examine its roles during female mouse meiosis. Aurora-C was detected at the centromeres and along the chromosome arms in prometaphase I–metaphase I and was concentrated at centromeres at metaphase II, in which Aurora-C also was phosphorylated at Thr171. During the anaphase I–telophase I transition, Aurora-C was dephosphorylated and relocalized to the midzone and midbody. Microinjection of the kinase-deficient Aurora-C (AurC-KD) mRNA into mouse oocytes significantly inhibited Aurora-C activity and caused multiple defects, including chromosome misalignment, abnormal kinetochore–microtubule attachment, premature chromosome segregation, and cytokinesis failure in meiosis I. Furthermore, AurC-KD reduced Aurora-C and histone H3 phosphorylation and inhibited kinetochore localization of Bub1 and BubR1. Similar effects also were observed in the oocytes injected with INCNEP-delIN mRNAs, in which the Aurora-C binding motif was removed. The most dramatic effect observed in AurC-KD–injected oocytes is cytokinesis failure in meiosis I, resulting in producing large polyploid oocytes, a pattern similar to Aurora-C deficiency human spermatozoa. Surprisingly, we detected no Aurora-B protein in mouse oocytes. We propose that Aurora-C, but not Aurora-B, plays essential roles in female mouse meiosis.
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spelling pubmed-29036672010-09-30 Aurora-C Kinase Deficiency Causes Cytokinesis Failure in Meiosis I and Production of Large Polyploid Oocytes in Mice Yang, Kuo-Tai Li, Shu-Kuei Chang, Chih-Chieh Tang, Chieh-Ju C. Lin, Yi-Nan Lee, Sheng-Chung Tang, Tang K. Mol Biol Cell Articles We previously isolated Aurora-C/Aie1 in a screen for kinases expressed in mouse sperm and eggs. Here, we show the localization of endogenous Aurora-C and examine its roles during female mouse meiosis. Aurora-C was detected at the centromeres and along the chromosome arms in prometaphase I–metaphase I and was concentrated at centromeres at metaphase II, in which Aurora-C also was phosphorylated at Thr171. During the anaphase I–telophase I transition, Aurora-C was dephosphorylated and relocalized to the midzone and midbody. Microinjection of the kinase-deficient Aurora-C (AurC-KD) mRNA into mouse oocytes significantly inhibited Aurora-C activity and caused multiple defects, including chromosome misalignment, abnormal kinetochore–microtubule attachment, premature chromosome segregation, and cytokinesis failure in meiosis I. Furthermore, AurC-KD reduced Aurora-C and histone H3 phosphorylation and inhibited kinetochore localization of Bub1 and BubR1. Similar effects also were observed in the oocytes injected with INCNEP-delIN mRNAs, in which the Aurora-C binding motif was removed. The most dramatic effect observed in AurC-KD–injected oocytes is cytokinesis failure in meiosis I, resulting in producing large polyploid oocytes, a pattern similar to Aurora-C deficiency human spermatozoa. Surprisingly, we detected no Aurora-B protein in mouse oocytes. We propose that Aurora-C, but not Aurora-B, plays essential roles in female mouse meiosis. The American Society for Cell Biology 2010-07-15 /pmc/articles/PMC2903667/ /pubmed/20484572 http://dx.doi.org/10.1091/mbc.E10-02-0170 Text en © 2010 by The American Society for Cell Biology
spellingShingle Articles
Yang, Kuo-Tai
Li, Shu-Kuei
Chang, Chih-Chieh
Tang, Chieh-Ju C.
Lin, Yi-Nan
Lee, Sheng-Chung
Tang, Tang K.
Aurora-C Kinase Deficiency Causes Cytokinesis Failure in Meiosis I and Production of Large Polyploid Oocytes in Mice
title Aurora-C Kinase Deficiency Causes Cytokinesis Failure in Meiosis I and Production of Large Polyploid Oocytes in Mice
title_full Aurora-C Kinase Deficiency Causes Cytokinesis Failure in Meiosis I and Production of Large Polyploid Oocytes in Mice
title_fullStr Aurora-C Kinase Deficiency Causes Cytokinesis Failure in Meiosis I and Production of Large Polyploid Oocytes in Mice
title_full_unstemmed Aurora-C Kinase Deficiency Causes Cytokinesis Failure in Meiosis I and Production of Large Polyploid Oocytes in Mice
title_short Aurora-C Kinase Deficiency Causes Cytokinesis Failure in Meiosis I and Production of Large Polyploid Oocytes in Mice
title_sort aurora-c kinase deficiency causes cytokinesis failure in meiosis i and production of large polyploid oocytes in mice
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2903667/
https://www.ncbi.nlm.nih.gov/pubmed/20484572
http://dx.doi.org/10.1091/mbc.E10-02-0170
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