BubR1 blocks substrate recruitment to the APC/C in a KEN-box-dependent manner

Lara-González, Pablo; Scott, Maria I. F.; Diez, Maria; Sen, Onur; Taylor, Stephen S.

doi:10.1242/jcs.094763

Cited by 102 publications

(142 citation statements)

References 53 publications

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“…4A). These results were consistent with published reports showing that the KEN1 box, but not the KEN2 box, of BubR1 was required for MCC formation in human cells (23). Strikingly, despite retaining proper Bub3 binding, Myc-BubR1 ⌬PheD bound to Cdc20 and Mad2 much less efficiently, at 70 and 30% of the WT levels (Fig.…”

Section: Bubr1 Phe and D Boxes Contribute To Mcc Homeostasis In Mitotsupporting

confidence: 93%

“…Using a seat belt-like structural element, Mad2 in its active, closed conformation traps the Mad2-interacting motif of Cdc20 in a topological embrace (26 -28). The N-terminal region of BubR1 (BubR1N) contains two KEN boxes and interacts directly with Cdc20 through the first KEN box (KEN1) (16,23). Cdc20-bound Mad2 also makes direct contact with Mad3 (and quite possibly BubR1N) (17,29), buttressing the weak Cdc20-KEN1 interaction.…”

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confidence: 99%

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The Cdc20-binding Phe Box of the Spindle Checkpoint Protein BubR1 Maintains the Mitotic Checkpoint Complex During Mitosis

Díaz-Martínez¹,

Tian²,

et al. 2015

Journal of Biological Chemistry

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Background:The spindle checkpoint protein BubR1 inhibits the anaphase-promoting complex through binding to Cdc20. Results:We identify a new Cdc20-binding motif within BubR1 termed the Phe box. Conclusion: The Phe box maintains steady-state levels of BubR1-containing checkpoint complexes in human cells. Significance: Our study provides key insights into the homeostatic mechanisms of a key spindle checkpoint complex.

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Section: Bubr1 Phe and D Boxes Contribute To Mcc Homeostasis In Mitotsupporting

confidence: 93%

mentioning

confidence: 99%

The Cdc20-binding Phe Box of the Spindle Checkpoint Protein BubR1 Maintains the Mitotic Checkpoint Complex During Mitosis

Díaz-Martínez¹,

Tian²,

et al. 2015

Journal of Biological Chemistry

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“…BubR1 contains two Cdc20 binding sites, a conserved site in the N-terminal Mad3-homology domain and an internal site that is present only in higher eukaryotes. The two Cdc20 binding sites of BubR1 have been shown to be able, respectively, to mediate inhibition of Cdc20 activation of APC/C in Mad2-dependent (13,41) and Mad2-independent manners (42). We tested the contributions of the individual Cdc20 binding sites of BubR1 in Bub3-stimulated inhibition of APC/C Cdc20 ubiquitination of cyclin B in vitro.…”

Section: Resultsmentioning

confidence: 99%

“…Our evidence in the current study has established that Bub3 promotes this BubR1-Cdc20 interaction, thereby uncovering a previously unknown role for Bub3 in production of the mitotic checkpoint inhibitor through action at the most downstream step of the signaling pathway. Two previous studies proposed that the first KEN box in the N-terminal Cdc20 binding site of BubR1 is responsible for BubR1 binding to Cdc20 (14,41). Based on this, it is plausible that Bub3 binding may alter the conformation of the initially rod-shaped BubR1 N terminus (34,50) in a way to either promote the initial assembly or stabilization of a BubR1-Cdc20 complex for generating the characteristic, selective inhibition of APC/C Cdc20 .…”

Section: Discussionmentioning

confidence: 99%

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Bimodal activation of BubR1 by Bub3 sustains mitotic checkpoint signaling

Han¹,

Vitre²,

Fachinetti³

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

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Significance The mitotic checkpoint (or the spindle assembly checkpoint) ensures genome integrity by preventing premature chromosome segregation. The pathway is triggered locally by kinetochores, multiprotein complexes assembled onto centromeres. Unattached kinetochores produce Mad2 bound to Cdc20, the mitotic activator of the E3 ubiquitin ligase APC/C. The initial Mad2–Cdc20 complex is then converted into the final mitotic checkpoint inhibitor Bub3–BubR1–Cdc20 that blocks APC/C (anaphase promoting complex or cyclosome)-dependent ubiquitination of cyclin B and securin, thereby stabilizing them and preventing an advance to anaphase. In this study, we identify dual mechanisms by which Bub3 promotes mitotic checkpoint signaling. Bub3 binding to BubR1 promotes two distinct BubR1–Cdc20 interactions, one acting at unattached kinetochores and the other cytoplasmically to facilitate production of the mitotic checkpoint inhibitor.

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Stable MCC binding to the APC /C is required for a functional spindle assembly checkpoint

Hein

Nilsson

2014

EMBO Reports

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The spindle assembly checkpoint (SAC) delays progression into anaphase until all chromosomes have aligned on the metaphase plate by inhibiting Cdc20, the mitotic co-activator of the APC/C. Mad2 and BubR1 bind and inhibit Cdc20, thereby forming the mitotic checkpoint complex (MCC), which can bind stably to the APC/C. Whether MCC formation per se is sufficient for a functional SAC or MCC association with the APC/C is required remains unclear. Here, we analyze the role of two conserved motifs in Cdc20, IR and C-Box, in binding of the MCC to the APC/C. Mutants in both motifs assemble the MCC normally, but IR motif integrity is particularly important for stable binding to the APC/C. Cells expressing Cdc20 with a mutated IR motif have a compromised SAC, as uninhibited Cdc20 can compete with the MCC for APC/C binding and activate it. We thus show that stable MCC association with the APC/C is critical for a functional SAC.

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BubR1 blocks substrate recruitment to the APC/C in a KEN-box-dependent manner

Cited by 102 publications

References 53 publications

The Cdc20-binding Phe Box of the Spindle Checkpoint Protein BubR1 Maintains the Mitotic Checkpoint Complex During Mitosis

The Cdc20-binding Phe Box of the Spindle Checkpoint Protein BubR1 Maintains the Mitotic Checkpoint Complex During Mitosis

Bimodal activation of BubR1 by Bub3 sustains mitotic checkpoint signaling

Stable MCC binding to the APC /C is required for a functional spindle assembly checkpoint

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