2006
DOI: 10.1038/ncb1410
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Early mitotic degradation of Nek2A depends on Cdc20-independent interaction with the APC/C

Abstract: The temporal control of mitotic protein degradation remains incompletely understood. In particular, it is unclear why the mitotic checkpoint prevents the anaphase-promoting complex/cyclosome (APC/C)-mediated degradation of cyclin B and securin in early mitosis, but not cyclin A. Here, we show that another APC/C substrate, NIMA-related kinase 2A (Nek2A), is also destroyed in pro-metaphase in a checkpoint-independent manner and that this depends on an exposed carboxy-terminal methionine-arginine (MR) dipeptide t… Show more

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Cited by 150 publications
(182 citation statements)
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“…After mitotic entry, Nek2A is specifically targeted for proteasomal degradation as a result of APC/C-mediated ubiquitylation, whereas Nek2B remains stable as it lacks the degradation motifs present in the C terminus of Nek2A (24,25). These degradation motifs, a KEN-box and the C-terminal MR dipeptide, are present in Nek2C, and we predicted that this isoform would also be degraded in mitosis.…”
Section: Nek2c Is Degraded In Mitotic Egg Extracts and Prometaphase-amentioning
confidence: 99%
See 1 more Smart Citation
“…After mitotic entry, Nek2A is specifically targeted for proteasomal degradation as a result of APC/C-mediated ubiquitylation, whereas Nek2B remains stable as it lacks the degradation motifs present in the C terminus of Nek2A (24,25). These degradation motifs, a KEN-box and the C-terminal MR dipeptide, are present in Nek2C, and we predicted that this isoform would also be degraded in mitosis.…”
Section: Nek2c Is Degraded In Mitotic Egg Extracts and Prometaphase-amentioning
confidence: 99%
“…This is followed by a short motif (amino acids 333-370) shown to be required for centrosome targeting and microtubule binding (22). However, the position of splicing means that a binding site for protein phosphatase 1 (PP1 3 ; amino acids 383-386) and two APC/Cdependent degradation motifs, a KEN box (amino acids 391-399), and an MR-tail (amino acids 444 -445), are present in Nek2A but missing from Nek2B (23)(24)(25). This falls in line with observations that Nek2A is degraded upon mitotic entry, whereas Nek2B remains stable.…”
mentioning
confidence: 99%
“…At the G 1 /S transition vertebrates express two major splice variants, Nek2A and Nek2B (19,20). These variants differ in their extreme C termini, which has important implications for their regulation, as the C terminus of Nek2A, but not Nek2B, contains both a binding site for protein phosphatase 1 and motifs that target the protein for ubiquitin-mediated degradation after mitotic entry (21)(22)(23).…”
mentioning
confidence: 99%
“…SAC-independent Nek2A degradation requires the carboxyl-terminal dipeptide of Nek2A (Met-Arg), and the di-peptide mediates the recruitment of Nek2A to APC/C to activate ubiquitylation (58,59). Thus, Nek2A is degraded independently of the SAC.…”
Section: Discussionmentioning
confidence: 99%