1. Those data indicate that the overexpression of PLK3-mediated degradation of abnormal PrP is largely dependent on chaperone-mediated autophagy pathway. PMID: 27344333
2. study revealed an interesting mutual regulation between Plk3 and SIAH2 and uncovered a regulatory network that functions to fine-tune the cellular hypoxic response. PMID: 28515325
3. the differential effects of hypoxic stress on Plk3 activity in Human Limbal Stem and HCE cells. Instead of apoptosis, hypoxic stress suppresses Plk3 activity to protect limbal stem cells from death and to allow the process of Human Limbal Stem cell differentiation. PMID: 27281822
4. Data suggest that HOXA-AS2 could be an oncogene for gastric cancer partly through suppressing P21, PLK3, and DDIT3 expression. PMID: 26384350
5. PLK3 predominantly is expressed in Cholangiocarcinomas (CCA) cells and that high PLK3 expression correlates with prolonged overall survival. PMID: 25818805
6. The role of Plk3 in oncogenesis: the aberrant expression of Plk3 was found in different types of tumors. PMID: 25915845
7. hyperosmotic stress-activated Plk3 elicited gammaH2AX. PMID: 25202016
8. Plk3 binds to CtIP phosphorylated at S327 via its Polo box domains, which is necessary for robust damage-induced CtIP phosphorylation at S327 and subsequent CtIP phosphorylation at T847. PMID: 25267294
9. have identified and validated as in vitro PLK2 and PLK3 substrates HSP90, GRP-94, beta-tubulin, calumenin, and 14-3-3 epsilon PMID: 22828320
10. Here, the authors report phosphorylation of Thr4 by Polo-like kinase 3 in mammalian cells. PMID: 22549466
11. Bcl-xL phosphorylation at Ser49 by polo-like kinase 3 during cell cycle progression and checkpoints PMID: 21840391
12. Calcium- and integrin-binding protein 1 regulates microtubule organization and centrosome segregation through polo like kinase 3 during cell cycle progression. PMID: 20951827
13. hyperosmotic stress can activate the Plk3 signaling pathway that subsequently regulates the AP-1 complex by directly phosphorylating ATF-2 independent from the effects of JNK and p38 activation. PMID: 21098032
14. Plk3 functions as an essential component of the hypoxia regulatory pathway by direct phosphorylation of HIF-1alpha PMID: 20889502
15. upregulation of CIB1 in cancer cells may inhibit Plk3 activity, leading to abnormal cell cycle regulation in breast cancer cells. PMID: 20473878
16. Plk3 as a new player in the regulation of the PI3K/PDK1/Akt signaling axis by phosphorylation and stabilization of PTEN. PMID: 20940307
17. The Plk3 overexpression suppressed cellular growth in a long-term colony-forming assay. And overexpression of Plk3 caused long-term growth suppression in Ras-transformed NIH3T3. PMID: 19556223
18. These results suggest that Polo-like kinase regulates the dissociation of cohesin from chromosomes early in mitosis. (cohesin) PMID: 11931760
19. Results suggest that Plk3 plays an important role in the regulation of microtubule dynamics and centrosomal function in the cell and that deregulated expression of Plk3 results in cell cycle arrest and apoptosis. PMID: 11971976
20. Plk3 is a multifunctional protein that associates with multiple complexes and that contributes to response to stress incurred by DNA damage and mitotic spindle disruption, albeit via different pathways. PMID: 12242661
21. Plk3 is rapidly activated by reactive oxygen species in fibroblasts, correlating with increased p53 protein levels. Plk3 physically interacts with Chk2 and the interaction is enhanced upon DNA damage. PMID: 12548019
22. Plk3 has a role in coordinating the translocation and perhaps the timing of both Cdc25C and its target Cdc2/cyclin B to the nucleus upon entry into mitosis PMID: 14968113
23. Plk3 may be a key protein kinase mediating MEK1 function in the Golgi fragmentation pathway during cell division. PMID: 15021912
24. Plk3 is a RelA-NF-kappaB-regulated gene that induces apoptosis in both p53-dependent and -independent signaling pathways PMID: 15671037
25. Introduction of plk3 gene into tumor cells with RV vectors can slow down cell proliferation, prevent cells into cell cycle and protect cells from apoptosis in serum-free culture. PMID: 16388739
26. the Polo box domain of Plk3 is more potent in inhibiting cell proliferation and inducing apoptosis than that of Plk1 PMID: 16478733
27. Plk3 is in a pathway linking ATM, Plk3, Chk2, Cdc25C and Cdc2 in cellular response to DNA damage. PMID: 16481012
28. Plk3 localizes to the nucleolus and is involved in regulation of the G1/S phase transition. PMID: 17264206
29. Results show that Plk3 mediates UV irradiation-induced c-Jun activation by phosphorylating c-Jun, suggesting that Plk3 plays an important role in mediating programmed cell death of corneal epithelial cells after UV irradiation. PMID: 17804415
30. topoisomerase IIalpha is a novel physiological substrate for Plk3, and Plk1 and Plk3 play different roles in cell-cycle regulation. PMID: 18062778
31. hypoxia/reoxygenation induces Plk3 activation instead of the JNK effect to directly phosphorylate and activate c-Jun, subsequently contributing to apoptosis in human corneal epithelial cells PMID: 18650425
32. The Plk3-VRK1 kinase module might represent two consecutive steps of a signaling cascade that participates in the regulation of Golgi fragmentation. PMID: 19103756

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HGNC: 2154

OMIM: 602913

KEGG: hsa:1263

STRING: 9606.ENSP00000361275

UniGene: Hs.632415