Recruitment of the human Cdt1 replication licensing protein by the loop domain of Hec1 is required for stable kinetochore–microtubule attachment

Varma, Dileep; Chandrasekaran, Srikripa; Sundin, Lynsie J.R.; Reidy, Karen T.; Wan, Xiaohu; Chasse, Dawn; Nevis, Kathleen R.; DeLuca, Jennifer G.; Salmon, E. D.; Cook, Jeanette Gowen

doi:10.1038/ncb2489

Cited by 93 publications

(147 citation statements)

References 42 publications

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“…At least three substrates (CDT1, p21, and SET8) have known roles in mitosis (21)(22)(23)64), and it is possible that other CRL4 CDT2 substrates also have mitotic roles, making general substrate stabilization important for mitosis. Independent of these mitotic roles, the known substrates of replication-cou-FIGURE 6.…”

Section: Discussionmentioning

confidence: 99%

“…We show here that CDK1 activity (directly and/or indirectly) inhibits CRL4 CDT2 activity itself by preventing its accumulation on chromatin, an event necessary for CRL4 CDT2 activity. Activation of CDK1 as S phase completes is necessary for the normal reaccumulation of substrates, such as CDT1 and SET8, and we show that, like CDT1, failure to reaccumulate SET8 de novo prior to mitosis leads to mitotic progression defects (21). The temporal control of CRL4 CDT2 activity ensures the accumulation of CRL4 CDT2 substrates during mitosis, thereby preventing chromosome instability.…”

mentioning

confidence: 96%

“…1). Importantly, CDT1, p21, and SET8 also function during mitosis, making their reaccumulation critical for normal mitotic progression (21)(22)(23). Replication-coupled destruction is triggered by the ubiquitin E3 ligase, CRL4…”

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confidence: 99%

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CDK1-dependent Inhibition of the E3 Ubiquitin Ligase CRL4CDT2 Ensures Robust Transition from S Phase to Mitosis

Rizzardi¹,

Coleman²,

Varma

et al. 2015

Journal of Biological Chemistry

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Background: CRL4CDT2 mediates replication-coupled destruction during S phase. CRL4 CDT2 substrates reaccumulate by an unexplored mechanism. Results: CDK1 activity blocks CRL4CDT2 by preventing chromatin recruitment of the substrate receptor, CDT2. Conclusion: CDK1 activity facilitates CRL4 CDT2 substrate reaccumulation upon S phase exit; several of these substrates are then required for normal mitotic progression. Significance: We provide the first evidence that CDK1 regulates the activity of CRL4 CDT2 .

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Section: Discussionmentioning

confidence: 99%

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confidence: 96%

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CDK1-dependent Inhibition of the E3 Ubiquitin Ligase CRL4CDT2 Ensures Robust Transition from S Phase to Mitosis

Rizzardi¹,

Coleman²,

Varma

et al. 2015

Journal of Biological Chemistry

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“…The loop is required to recruit the Dam1 complex to kinetochores in vivo (Maure et al 2011), but it is not necessarily a direct binding site and the requirement may be due to a structural change that occurs when the loop is deleted. In other organisms, the loop has been implicated in interacting with the Ska1 complex, the Dis1/TOG/Stu2 protein, and the Cdt1 replication factor (Hsu and Toda 2011;Varma et al 2012;Zhang et al 2012), so its precise role is unclear.…”

Section: Kmnmentioning

confidence: 99%

The Composition, Functions, and Regulation of the Budding Yeast Kinetochore

2013

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The propagation of all organisms depends on the accurate and orderly segregation of chromosomes in mitosis and meiosis. Budding yeast has long served as an outstanding model organism to identify the components and underlying mechanisms that regulate chromosome segregation. This review focuses on the kinetochore, the macromolecular protein complex that assembles on centromeric chromatin and maintains persistent load-bearing attachments to the dynamic tips of spindle microtubules. The kinetochore also serves as a regulatory hub for the spindle checkpoint, ensuring that cell cycle progression is coupled to the achievement of proper microtubule-kinetochore attachments. Progress in understanding the composition and overall architecture of the kinetochore, as well as its properties in making and regulating microtubule attachments and the spindle checkpoint, is discussed. TABLE OF CONTENTS Abstract 817Introduction 818

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“…The second example is DNA replication factor Cdt1 (UniProt ID: Q9H211) (Varma et al, 2012). Besides its primary function as DNA replication factor, this MP's secondary function is a role in mitosis where it localizes to kinetochores through binding to the Hec1 component of the Ndc80 complex.…”

Section: Prediction Accuracy Of Mpsmentioning

confidence: 99%

Genome-scale prediction of moonlighting proteins using diverse protein association information

Khan¹

2016

Bioinformatics

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Motivation: Moonlighting proteins (MPs) show multiple cellular functions within a single polypeptide chain. To understand the overall landscape of their functional diversity, it is important to establish a computational method that can identify MPs on a genome scale. Previously, we have systematically characterized MPs using functional and omics-scale information. In this work, we develop a computational prediction model for automatic identification of MPs using a diverse range of protein association information. Results: We incorporated a diverse range of protein association information to extract characteristic features of MPs, which range from gene ontology (GO), protein-protein interactions, gene expression, phylogenetic profiles, genetic interactions and network-based graph properties to protein structural properties, i.e. intrinsically disordered regions in the protein chain. Then, we used machine learning classifiers using the broad feature space for predicting MPs. Because many known MPs lack some proteomic features, we developed an imputation technique to fill such missing features. Results on the control dataset show that MPs can be predicted with over 98% accuracy when GO terms are available. Furthermore, using only the omics-based features the method can still identify MPs with over 75% accuracy. Last, we applied the method on three genomes: Saccharomyces cerevisiae, Caenorhabditis elegans and Homo sapiens, and found that about 2-10% of proteins in the genomes are potential MPs. Availability and Implementation: Code available at http://kiharalab.org/MPprediction

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Recruitment of the human Cdt1 replication licensing protein by the loop domain of Hec1 is required for stable kinetochore–microtubule attachment

Cited by 93 publications

References 42 publications

CDK1-dependent Inhibition of the E3 Ubiquitin Ligase CRL4CDT2 Ensures Robust Transition from S Phase to Mitosis

CDK1-dependent Inhibition of the E3 Ubiquitin Ligase CRL4CDT2 Ensures Robust Transition from S Phase to Mitosis

The Composition, Functions, and Regulation of the Budding Yeast Kinetochore

Genome-scale prediction of moonlighting proteins using diverse protein association information

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