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Query: UMLS:C0033036 (
APC
)
10,214
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The Anaphase-Promoting Complex/Cyclosome (
APC
/C) is an E3 ubiquitin ligase and a key regulator of cell cycle progression. By triggering the degradation of mitotic cyclins,
APC
/C controls cell cycle-dependent oscillations in
cyclin-dependent kinase
(
CDK
) activity. Thus, the dynamic activities of both
APC
/C and
CDK
sit at the core of the cell cycle oscillator. The
APC
/C controls a large number of substrates and is regulated through multiple mechanisms, including cofactor-dependent activation. These cofactors, Cdc20 and Cdh1, recognize substrates, while the specific E2 enzymes UBE2C/UbcH10 and UBE2S cooperate with
APC
/C to build K11-linked ubiquitin chains on substrates to target them for proteasomal degradation. However, whether deubiquitinating enzymes (DUBs) can antagonize
APC
/C substrate ubiquitination during mitosis has remained largely unknown. We recently demonstrated that Cezanne/OTUD7B is a cell cycle-regulated DUB that opposes the ubiquitination of
APC
/C substrates. Cezanne binds
APC
/C substrates, reverses their ubiquitination and protects them from degradation. Accordingly, Cezanne depletion accelerates
APC
/C substrate degradation, leading to errors in mitotic progression and formation of micronuclei. Moreover, Cezanne is significantly amplified and overexpressed in breast cancers. This suggests a potential role for
APC
/C antagonism in the pathogenesis of disease.
APC
/C contributes to chromosome segregation fidelity in mitosis raising the possibility that copy-number and expression changes in Cezanne observed in cancer contribute to the etiology of disease. Collectively, these observations identify a new player in cell cycle progression, define mechanisms of tempered
APC
/C substrate destruction and highlight the importance of this regulation in maintaining chromosome stability.
...
PMID:Impressionist portraits of mitotic exit: APC/C, K11-linked ubiquitin chains and Cezanne. 3087 63
Cell division cycle (
C
dc)
k
inase
s
ubunit (CKS) proteins bind cyclin-dependent kinases (CDKs) and play important roles in cell division control and development, though their precise molecular functions are not fully understood. Mammals express two closely related paralogs called CKS1 and CKS2, but only CKS2 is expressed in the germ line, indicating that it is solely responsible for regulating
CDK
functions in meiosis. Using
cks2
-/-
knockout mice, we show that CKS2 is a crucial regulator of maturation-promoting factor (MPF; CDK1-cyclin A/B) activity in meiosis.
cks2
-/-
oocytes display reduced and delayed MPF activity during meiotic progression, leading to defects in germinal vesicle breakdown (GVBD), anaphase-promoting complex/cyclosome (
APC
/C) activation, and meiotic spindle assembly.
cks2
-/-
germ cells express significantly reduced levels of the MPF components CDK1 and cyclins A1/B1. Additionally, injection of MPF plus CKS2, but not MPF alone, restored normal GVBD in
cks2
-/-
oocytes, demonstrating that GVBD is driven by a CKS2-dependent function of MPF. Moreover, we generated
cks2
cks1/cks1
knock-in mice and found that CKS1 can compensate for CKS2 in meiosis
in vivo
, but homozygous embryos arrested development at the 2- to 5-cell stage. Collectively, our results show that CKS2 is a crucial regulator of MPF functions in meiosis and that its paralog, CKS1, must be excluded from the germ line for proper embryonic development.
...
PMID:CKS1 Germ Line Exclusion Is Essential for the Transition from Meiosis to Early Embryonic Development. 3098 59
Cell cycle regulation is essential for the development of multicellular organisms, but many cells in adulthood, including neurons, exit from cell cycle. Although cell cycle-related proteins are suppressed after cell cycle exit in general, recent studies have revealed that growth arrest triggers extra-cell cycle regulatory function (EXCERF) in some cell cycle proteins, such as p27(kip1), p57(kip2), anaphase-promoting complex/cyclosome (
APC
/C), and cyclin E. While p27 is known to control G1 length and cell cycle exit via inhibition of
cyclin-dependent kinase
(
CDK
) activities, p27 acquires additional cytoplasmic functions in growth-arrested neurons. Here, we introduce the EXCERFs of p27 in post-mitotic neurons, mainly focusing on its actin and microtubule regulatory functions. We also show that a small amount of p27 is associated with the Golgi apparatus positive for Rab6, p115, and GM130, but not endosomes positive for Rab5, Rab7, Rab8, Rab11, SNX6, or LAMTOR1. p27 is also colocalized with Dcx, a microtubule-associated protein. Based on these results, we discuss here the possible role of p27 in membrane trafficking and microtubule-dependent transport in post-mitotic cortical neurons. Collectively, we propose that growth arrest leads to two different fates in cell cycle proteins; either suppressing their expression or activating their EXCERFs. The latter group of proteins, including p27, play various roles in neuronal migration, morphological changes and axonal transport, whereas the re-activation of the former group of proteins in post-mitotic neurons primes for cell death.
...
PMID:Growth Arrest Triggers Extra-Cell Cycle Regulatory Function in Neurons: Possible Involvement of p27
kip1
in Membrane Trafficking as Well as Cytoskeletal Regulation. 3108 Aug 1
In the eukaryotic cell cycle, a threshold level of cyclin B accumulation triggers the G2-to-M transition, and subsequent cyclin B destruction triggers mitotic exit. The anaphase-promoting complex/cyclosome (
APC
/C) is the E3 ubiquitin ligase that, together with its co-activator Cdc20, targets cyclin B for destruction during mitotic exit. Here, we show that two pathways act in concert to protect cyclin B from Cdc20-activated
APC
/C in G2, in order to enable cyclin B accumulation and the G2-to-M transition. The first pathway involves the Mad1-Mad2 spindle checkpoint complex, acting in a distinct manner from checkpoint signaling after mitotic entry but employing a common molecular mechanism-the promotion of Mad2-Cdc20 complex formation. The second pathway involves
cyclin-dependent kinase
phosphorylation of Cdc20, which is known to reduce Cdc20's affinity for the
APC
/C. Cooperation of these two mechanisms, which target distinct
APC
/C binding interfaces of Cdc20, enables cyclin B accumulation and the G2-to-M transition.
...
PMID:The G2-to-M Transition Is Ensured by a Dual Mechanism that Protects Cyclin B from Degradation by Cdc20-Activated APC/C. 3158 29
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