AI Article Synopsis
- Mitotic exit in budding yeast is essential for maintaining genome integrity and involves cyclin B destruction and proper nuclear positioning.
- The mitotic exit network (MEN) activates during anaphase through the association of the Dbf2-Mob1 kinase complex with the Nud1 scaffold protein at spindle pole bodies (SPBs).
- A newly identified hyperactive allele of Cdc15 allows its recruitment to SPBs throughout the cell cycle, disrupting the normal coupling between nuclear position and mitotic exit in cells with mispositioned spindles, emphasizing the role of scaffold regulation in signaling pathways.
Article Abstract
Mitotic exit is a critical cell cycle transition that requires the careful coordination of nuclear positioning and cyclin B destruction in budding yeast for the maintenance of genome integrity. The mitotic exit network (MEN) is a Ras-like signal transduction pathway that promotes this process during anaphase. A crucial step in MEN activation occurs when the Dbf2-Mob1 protein kinase complex associates with the Nud1 scaffold protein at the yeast spindle pole bodies (SPBs; centrosome equivalents) and thereby becomes activated. This requires prior priming phosphorylation of Nud1 by Cdc15 at SPBs. Cdc15 activation, in turn, requires both the Tem1 GTPase and the Polo kinase Cdc5, but how Cdc15 associates with SPBs is not well understood. We have identified a hyperactive allele of , , that recruits Cdc15 to SPBs in all stages of the cell cycle in a -independent manner. This allele leads to early recruitment of Dbf2-Mob1 during metaphase and requires known Cdc15 phospho-sites on Nud1. The presence of leads to loss of coupling between nuclear position and mitotic exit in cells with mispositioned spindles. Our findings highlight the importance of scaffold regulation in signaling pathways to prevent improper activation.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8750578 | PMC |
| http://dx.doi.org/10.3390/cells11010046 | DOI Listing |
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