Open AccessAurora kinase A is essential for meiosis in mouse oocytes
Author(s) -
Cecilia S. Blengini,
Patricia Ibrahimian,
Michaela Vaškovičová,
Dávid Drutovič,
P Solc,
Karen Schindler
Publication year - 2021
Publication title -
plos genetics
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 3.587
H-Index - 233
eISSN - 1553-7404
pISSN - 1553-7390
DOI - 10.1371/journal.pgen.1009327
Subject(s) - biology , meiosis , microbiology and biotechnology , oocyte , spindle apparatus , aurora b kinase , aurora kinase , aurora inhibitor , chromosome segregation , kinase , aurora a kinase , mitosis , genetics , chromosome , cell division , cell cycle , embryo , gene , cell
The Aurora protein kinases are well-established regulators of spindle building and chromosome segregation in mitotic and meiotic cells. In mouse oocytes, there is significant Aurora kinase A (AURKA) compensatory abilities when the other Aurora kinase homologs are deleted. Whether the other homologs, AURKB or AURKC can compensate for loss of AURKA is not known. Using a conditional mouse oocyte knockout model, we demonstrate that this compensation is not reciprocal because female oocyte-specific knockout mice are sterile, and their oocytes fail to complete meiosis I. In determining AURKA-specific functions, we demonstrate that its first meiotic requirement is to activate Polo-like kinase 1 at acentriolar microtubule organizing centers (aMTOCs; meiotic spindle poles). This activation induces fragmentation of the aMTOCs, a step essential for building a bipolar spindle. We also show that AURKA is required for regulating localization of TACC3, another protein required for spindle building. We conclude that AURKA has multiple functions essential to completing MI that are distinct from AURKB and AURKC.