Literature DB >> 29162720

Direct interactions of mitotic arrest deficient 1 (MAD1) domains with each other and MAD2 conformers are required for mitotic checkpoint signaling.

Wenbin Ji1, Yibo Luo1, Ejaz Ahmad1, Song-Tao Liu2.   

Abstract

As a sensitive signaling system, the mitotic checkpoint ensures faithful chromosome segregation by delaying anaphase onset even when a single kinetochore is unattached to mitotic spindle microtubules. The key signal amplification reaction for the checkpoint is the conformational conversion of "open" mitotic arrest deficient 2 (O-MAD2) into "closed" MAD2 (C-MAD2). The reaction has been 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 well-characterized middle region of MAD1 containing the MAD2-interaction motif (MIM), both N- and C-terminal domains (NTD and CTD) of MAD1 also contribute to mitotic checkpoint signaling. Unlike the MIM, which stably associated only with C-MAD2, the NTD and CTD in MAD1 surprisingly bound both O- and C-MAD2, suggesting that these two domains interact with both substrates and products of the O-to-C conversion. MAD1NTD and MAD1CTD also interacted with each other and with the MPS1 protein kinase, which phosphorylated both NTD and CTD. This phosphorylation decreased the NTD:CTD interaction and also CTD's interaction with MPS1. Of note, mutating the phosphorylation sites in the MAD1CTD, including Thr-716, compromised MAD2 binding and the checkpoint responses. We further noted that Ser-610 and Tyr-634 also contribute to the mitotic checkpoint signaling. Our results have uncovered that the MAD1NTD and MAD1CTD directly interact with each other and with MAD2 conformers and are regulated by MPS1 kinase, providing critical insights into mitotic checkpoint signaling.
© 2018 by The American Society for Biochemistry and Molecular Biology, Inc.

Entities:  

Keywords:  MAD1; MAD2; MPS1 kinase; checkpoint control; kinetochore; mitosis; mitotic checkpoint; mitotic spindle; signal transduction

Mesh:

Substances:

Year:  2017        PMID: 29162720      PMCID: PMC5767855          DOI: 10.1074/jbc.RA117.000555

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  69 in total

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Review 10.  The spindle assembly checkpoint.

Authors:  Pablo Lara-Gonzalez; Frederick G Westhorpe; Stephen S Taylor
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3.  DNA Methylation in Babies Born to Nonsmoking Mothers Exposed to Secondhand Smoke during Pregnancy: An Epigenome-Wide Association Study.

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5.  Mitotic checkpoint gene expression is tuned by codon usage bias.

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Review 6.  MAD1: Kinetochore Receptors and Catalytic Mechanisms.

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7.  Cyclin B1 scaffolds MAD1 at the kinetochore corona to activate the mitotic checkpoint.

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8.  Kinetochore phosphatases suppress autonomous Polo-like kinase 1 activity to control the mitotic checkpoint.

Authors:  Marilia H Cordeiro; Richard J Smith; Adrian T Saurin
Journal:  J Cell Biol       Date:  2020-12-07       Impact factor: 10.539

Review 9.  Role of Stress-Survival Pathways and Transcriptomic Alterations in Progression of Colorectal Cancer: A Health Disparities Perspective.

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10.  Molecular mechanism of Mad1 kinetochore targeting by phosphorylated Bub1.

Authors:  Elyse S Fischer; Conny W H Yu; Dom Bellini; Stephen H McLaughlin; Christian M Orr; Armin Wagner; Stefan M V Freund; David Barford
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  10 in total

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