Plk1 is an early trigger for G2/M transition. Plk1 supports the functional maturation of the centrosome in late G2/early
prophase and establishment of the bipolar spindle. Plk1 phosphorylates and activates cdc25C, a
phosphatase that dephosphorylates and activates the cyclinB/
cdc2 complex. Plk phosphorylates and activates components of the
anaphase-promoting complex (APC). The APC, which is activated by Fizzy-Cdc20 family proteins, is a cell cycle
ubiquitin-protein ligase (E3) that degrades
mitotic cyclins, chromosomal proteins that maintain cohesion of
sister chromatids, and
anaphase inhibitors. Abnormal spindle (Asp), a Polo kinase substrate, is a
microtubule-associated protein essential for correct behavior of
spindle poles and M-phase microtubules. Plk1 localizes to the central region of the spindle in late mitosis and associates with
kinesin-like protein CHO1/MKLP1. The homologous
motor protein in
Drosophila is the pavarotti gene product (PAR). Studies have shown that the loss of PLK1 expression can induce
pro-apoptotic pathways and inhibit growth.
Meiosis Based on yeast and murine studies of
meiosis, human PLK1 may also have a regulatory function in meiosis. S. cerevisiae polo kinase CDC5 is required to phosphorylate and remove meiotic cohesion during the first cell division. In CDC5 depleted cells, kinetochores are bioriented during meiosis I, and Mam1, a protein essential for coorientation, fails to associate with kinetochores. CDC5 is believed to have roles in sister-kinetochore coorientation and
chromosome segregation during meiosis I. PLK1 functions during
meiotic centrosome biogenesis in mouse
spermatocytes, thus facilitating accurate
chromosome segregation during
spermatogenesis. == Role in tumorigenesis ==