Structure of an intermediate conformer of the spindle checkpoint protein Mad2

Hara, Mayuko; Özkan, Engin; Sun, Hongbin; Yu, Hongtao; Luo, Xuelian

doi:10.1073/pnas.1512197112

Cited by 33 publications

(53 citation statements)

References 45 publications

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“…Similarly, the interaction of Cdc20 with Mad2 is critical for the SAC. Mad2 is a 23.5-kDa protein that contains a Hop1p, Rev7p, and MAD2 (HORMA) domain of multiple conformational states, including an open (o-Mad2) and a closed (c-Mad2) conformation [36,37]. In the latter conformational state, Mad2 binds to Cdc20 and to its upstream regulator Mad1.…”

Section: Multiple Contacts Mediate the Cdc20-mcc Interactionmentioning

confidence: 99%

Cdc20: At the Crossroads between Chromosome Segregation and Mitotic Exit

Kapanidou

Curtis

Bolaños-García

2017

Trends in Biochemical Sciences

131

113

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Cell-division cycle protein 20 homologue (Cdc20) has important functions in chromosome segregation and mitotic exit. Cdc20 is the target of the spindle assembly checkpoint (SAC) and a key cofactor of the anaphase-promoting complex or cyclosome (APC/C) E3 ubiquitin ligase, thus regulating APC/C ubiquitin activity on specific substrates for their subsequent degradation by the proteasome. Here we discuss the roles of Cdc20 in SAC signalling and mitotic exit, describe how the integration of traditional approaches with emerging technologies has revealed new details of Cdc20 functions, comment about the potential of Cdc20 as a therapeutic target for the treatment of human malignancies, and discuss recent advances and controversies in the mechanistic understanding of the control of chromosome segregation during cell division.

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Section: Multiple Contacts Mediate the Cdc20-mcc Interactionmentioning

confidence: 99%

Cdc20: At the Crossroads between Chromosome Segregation and Mitotic Exit

Kapanidou

Curtis

Bolaños-García

2017

Trends in Biochemical Sciences

131

113

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“…3b). MAD2 N10 , which might mimic an intermediate conformation during O to C-MAD2 conversion (10), binds to all three MAD1 fragments (Fig. 3c).…”

Section: Mad1-ntd and -Ctd Bind To Both O-mad2mentioning

confidence: 97%

“…C-MAD2 then utilizes its dimerization domain to recruit O-MAD2 and converts the latter into C-MAD2, resulting in signal amplification for the mitotic checkpoint (6,7,12). The conversion may go through multiple intermediate states (I-MAD2) (6,7,10,13,32). At least two structures of I-MAD2:C-MAD2 dimers have been solved, one possibly representing the initial O-MAD2 "docking" complex and the other containing a later stage of I-MAD2 state (MAD2 N10 ) (10,32).…”

Section: The Functions Of Mad1-ntd and Ctd In Mad2 O-c Conversionmentioning

confidence: 99%

“…The solved MAD2 N10 structure indicates a topology similar to O-MAD2 but its internal core more closely resembles that of C-MAD2 (10). However, one long suspected intermediate state with partially unfolded N-or Ctermini, which is more amenable for MAD2 refolding or its interaction with CDC20, has not been identified based on studies of various MAD2 conformational dimers therefore was considered as only a fleeting state (10). Such a state, as suggested (29,30), may be coupled with formation of the CDC20:MAD2 complex or the MCC, making the MAD2 O-C conversion reaction more rapid and energy favorable.…”

Section: The Functions Of Mad1-ntd and Ctd In Mad2 O-c Conversionmentioning

confidence: 99%

“…During prometaphase intracellular C-MAD2 concentration is increased to promote formation of the mitotic checkpoint complex (MCC), which binds and inhibits the anaphase promoting complex/cyclosome (APC/C) (1)(2)(3)(4). In the current model, the MAD2 O-C conversion is catalyzed by a 2:2 MAD1:C-MAD2 tetramer localized at unattached kinetochores, whereby cytoplasmic O-MAD2 hetero-dimerizes with the C-MAD2 moiety in the catalyst and morphs into C-MAD2 through unknown mechanism but possibly involving some intermediate folding states (I-MAD2) (6,7,10).…”

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confidence: 99%

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Coordination between discrete Mitotic Arrest Deficient 1 (MAD1) domains is required for efficient mitotic checkpoint signaling

Luo

Ahmad

et al. 2017

Preprint

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As a sensitive signaling system, the mitotic checkpoint ensures faithful chromosome segregation by delaying anaphase onset when even a single kinetochore is unattached. The key signal amplification reaction for the checkpoint is the conformational conversion of open MAD2 (O-MAD2) into closed MAD2 (C-MAD2). The reaction was suggested to be catalyzed by an unusual catalyst, a MAD1:C-MAD2 tetramer, but how the catalysis is executed and regulated remains elusive. Here we report that in addition to the wellcharacterized middle region (MIM), both aminoand carboxyl-terminal domains (NTD and CTD) of MAD1 also contribute to the mitotic checkpoint. In contrast to MIM that stably associates with C-MAD2, MAD1-NTD and CTD surprisingly bind to both O-MAD2 and C-MAD2, suggesting their interactions with substrates and products of the O-C conversion. MAD1-NTD also interacts with CTD. MPS1 kinase interacts with and phosphorylates both NTD and CTD. The phosphorylation reduces the NTD:CTD interaction and CTD interaction with MPS1. Mutating CTD phosphorylation sites including Thr716 compromises MAD2 binding and the checkpoint responses. Ser610 and Tyr634 also contribute to the checkpoint. Our results have uncovered previously unknown interactions of MAD1-NTD and CTD with MAD2 conformers and their regulation by MPS1 kinase, providing novel insights into the mitotic checkpoint signaling. _______________________________________

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The role of the HORMA domain proteins ATG13 and ATG101 in initiating autophagosome biogenesis

Nguyen,

Faesen

2023

FEBS Letters

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Autophagy is a process of regulated degradation. It eliminates damaged and unnecessary cellular components by engulfing them with a de novo‐generated organelle: the double‐membrane autophagosome. The last three decades have provided us with a detailed parts list of the autophagy initiation machinery, have developed important insights into how these processes function and have identified regulatory proteins. It is now clear that autophagosome biogenesis requires the timely assembly of a complex machinery. However, it is unclear how a putative stable machine is assembled and disassembled, and how the different parts cooperate to perform its overall function. Although they have long been somewhat enigmatic in their precise role, HORMA domain proteins (first identified in Hop1p, Rev7p and MAD2 proteins) autophagy‐related protein 13 (ATG13) and ATG101 of the ULK‐kinase complex have emerged as important coordinators of the autophagy‐initiating subcomplexes. Here, we will particularly focus on ATG13 and ATG101 and the role of their unusual metamorphosis in initiating autophagosome biogenesis. We will also explore how this metamorphosis could potentially be purposefully rate‐limiting and speculate on how it could regulate the spontaneous self‐assembly of the autophagy‐initiating machinery.

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Structure of an intermediate conformer of the spindle checkpoint protein Mad2

Cited by 33 publications

References 45 publications

Cdc20: At the Crossroads between Chromosome Segregation and Mitotic Exit

Cdc20: At the Crossroads between Chromosome Segregation and Mitotic Exit

Coordination between discrete Mitotic Arrest Deficient 1 (MAD1) domains is required for efficient mitotic checkpoint signaling

The role of the HORMA domain proteins ATG13 and ATG101 in initiating autophagosome biogenesis

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