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Publication : Cyclin B3 promotes anaphase I onset in oocyte meiosis.

First Author  Karasu ME Year  2019
Journal  J Cell Biol Volume  218
Issue  4 Pages  1265-1281
PubMed ID  30723090 Mgi Jnum  J:273304
Mgi Id  MGI:6286631 Doi  10.1083/jcb.201808091
Citation  Karasu ME, et al. (2019) Cyclin B3 promotes anaphase I onset in oocyte meiosis. J Cell Biol 218(4):1265-1281
abstractText  Meiosis poses unique challenges because two rounds of chromosome segregation must be executed without intervening DNA replication. Mammalian cells express numerous temporally regulated cyclins, but how these proteins collaborate to control meiosis remains poorly understood. Here, we show that female mice genetically ablated for cyclin B3 are viable-indicating that the protein is dispensable for mitotic divisions-but are sterile. Mutant oocytes appear normal until metaphase I but then display a highly penetrant failure to transition to anaphase I. They arrest with hallmarks of defective anaphase-promoting complex/cyclosome (APC/C) activation, including no separase activity, high CDK1 activity, and high cyclin B1 and securin levels. Partial APC/C activation occurs, however, as exogenously expressed APC/C substrates can be degraded. Cyclin B3 forms active kinase complexes with CDK1, and meiotic progression requires cyclin B3-associated kinase activity. Cyclin B3 homologues from frog, zebrafish, and fruit fly rescue meiotic progression in cyclin B3-deficient mouse oocytes, indicating conservation of the biochemical properties and possibly cellular functions of this germline-critical cyclin.
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