We have characterized plk1 in mouse oocytes during meiotic maturation and after parthenogenetic activation until entry into the first mitotic division. Plk1 protein expression remains unchanged during maturation. However, two different isoforms can be identified by SDS-PAGE. A fast migrating form, present in the germinal vesicle, seems characteristic of interphase. A slower form appears as early as 30 min before germinal vesicle breakdown (GVBD), is maximal at GVBD, and is maintained throughout meiotic maturation. This form gradually disappears after exit from meiosis. The slow form corresponds to a phosphorylation since it disappears after alkaline phosphatase treatment. Plk1 activation, therefore, takes place before GVBD and MAPK activation since plk1 kinase activity correlates with its slow migrating phosphorylated form. However, plk1 phosphorylation is inhibited after treatment with two specific p34(cdc2) inhibitors, roscovitine and butyrolactone, suggesting plk1 involvement in the MPF autoamplification loop. During meiosis plk1 undergoes a cellular redistribution consistent with its putative targets. At the germinal vesicle stage, plk1 is found diffusely distributed in the cytoplasm and enriched in the nucleus and during prometaphase is localized to the spindle poles. At anaphase it relocates to the equatorial plate and is restricted to the postmitotic bridge at telophase. After parthenogenetic activation, plk1 becomes dephosphorylated and its activity drops progressively. Upon entry into the first mitotic M-phase at nuclear envelope breakdown plk1 is phosphorylated and there is an increase in its kinase activity. At the two-cell stage, the fast migrating form with weak kinase activity is present. In this work we show that plk1 is present in mouse oocytes during meiotic maturation and the first mitotic division. The variation of plk1 activity and subcellular localization during this period suggest its implication in the organization and progression of M-phase.
Characterization of polo-like kinase 1 during meiotic maturation of the mouse oocyte.
G. Pahlavan,Zbigniew Polanski,Zbigniew Polanski,P. Kalab,R. Golsteyn,Erich A. Nigg,B. Maro
Published 2000 in Developmental Biology
ABSTRACT
PUBLICATION RECORD
- Publication year
2000
- Venue
Developmental Biology
- Publication date
2000-04-15
- Fields of study
Biology, Medicine
- Identifiers
- External record
- Source metadata
Semantic Scholar, PubMed
CITATION MAP
EXTRACTION MAP
CLAIMS
CONCEPTS
- butyrolactone
A cyclin-dependent kinase inhibitor used as an experimental compound in the oocyte assays.
Aliases: butyrolactone I
- first mitotic m-phase
The first mitotic cell-cycle phase entered after activation of the oocyte.
Aliases: first mitotic phase
- germinal vesicle breakdown (gvbd)
The dissolution of the oocyte germinal vesicle that marks resumption of meiosis.
Aliases: germinal vesicle breakdown
- kinase activity
The enzymatic activity of a kinase to phosphorylate substrates.
Aliases: enzyme activity
- mapk activation
Activation of the mitogen-activated protein kinase signaling pathway state in the oocyte.
Aliases: mitogen-activated protein kinase activation
- meiotic maturation
The developmental progression of an oocyte through meiotic stages toward maturation.
- mouse oocyte
The female mouse germ cell examined during meiotic maturation and activation.
Aliases: oocyte
- mpf autoamplification loop
The positive-feedback regulatory loop that amplifies maturation-promoting factor activity.
Aliases: MPF loop
- parthenogenetic activation
Activation of an egg or oocyte without fertilization.
Aliases: parthenogenesis-induced activation
- phosphorylation
A post-translational modification in which phosphate groups are added to a protein.
- plk1
Polo-like kinase 1, a serine/threonine kinase examined in mouse oocytes during maturation and activation.
Aliases: polo-like kinase 1
- roscovitine
A cyclin-dependent kinase inhibitor used as an experimental compound in the oocyte assays.
- subcellular localization
The intracellular distribution pattern of a protein within a cell.
Aliases: localization
REFERENCES
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