Your search keyword '"Peters JM"' showing total 35 results

1. Posing the APC/C E3 Ubiquitin Ligase to Orchestrate Cell Division.

Author

Watson ER, Brown NG, Peters JM, Stark H, and Schulman BA

Subjects

Anaphase-Promoting Complex-Cyclosome chemistry, Carrier Proteins chemistry, Humans, Models, Molecular, Protein Binding, Protein Conformation, Ubiquitin-Protein Ligases chemistry, Ubiquitination, Anaphase-Promoting Complex-Cyclosome metabolism, Carrier Proteins metabolism, Mitosis, Ubiquitin-Protein Ligases metabolism

Abstract

The anaphase promoting complex/cyclosome (APC/C) E3 ligase controls mitosis and nonmitotic pathways through interactions with proteins that coordinate ubiquitylation. Since the discovery that the catalytic subunits of APC/C are conformationally dynamic cullin and RING proteins, many unexpected and intricate regulatory mechanisms have emerged. Here, we review structural knowledge of this regulation, focusing on: (i) coactivators, E2 ubiquitin (Ub)-conjugating enzymes, and inhibitors engage or influence multiple sites on APC/C including the cullin-RING catalytic core; and (ii) the outcomes of these interactions rely on mobility of coactivators and cullin-RING domains, which permits distinct conformations specifying different functions. Thus, APC/C is not simply an interaction hub, but is instead a dynamic, multifunctional molecular machine whose structure is remodeled by binding partners to achieve temporal ubiquitylation regulating cell division., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2019

2. Experimental and computational framework for a dynamic protein atlas of human cell division.

Author

Cai Y, Hossain MJ, Hériché JK, Politi AZ, Walther N, Koch B, Wachsmuth M, Nijmeijer B, Kueblbeck M, Martinic-Kavur M, Ladurner R, Alexander S, Peters JM, and Ellenberg J

Subjects

Gene Editing, Green Fluorescent Proteins analysis, Green Fluorescent Proteins metabolism, HeLa Cells, Humans, Imaging, Three-Dimensional, Microscopy, Fluorescence, Molecular Imaging, Time Factors, Cell Cycle Proteins analysis, Cell Cycle Proteins metabolism, Mitosis

Abstract

Essential biological functions, such as mitosis, require tight coordination of hundreds of proteins in space and time. Localization, the timing of interactions and changes in cellular structure are all crucial to ensure the correct assembly, function and regulation of protein complexes 1-4 . Imaging of live cells can reveal protein distributions and dynamics but experimental and theoretical challenges have prevented the collection of quantitative data, which are necessary for the formulation of a model of mitosis that comprehensively integrates information and enables the analysis of the dynamic interactions between the molecular parts of the mitotic machinery within changing cellular boundaries. Here we generate a canonical model of the morphological changes during the mitotic progression of human cells on the basis of four-dimensional image data. We use this model to integrate dynamic three-dimensional concentration data of many fluorescently knocked-in mitotic proteins, imaged by fluorescence correlation spectroscopy-calibrated microscopy 5 . The approach taken here to generate a dynamic protein atlas of human cell division is generic; it can be applied to systematically map and mine dynamic protein localization networks that drive cell division in different cell types, and can be conceptually transferred to other cellular functions.

Published

2018

3. Mechanism of APC/CCDC20 activation by mitotic phosphorylation.

Author

Qiao R, Weissmann F, Yamaguchi M, Brown NG, VanderLinden R, Imre R, Jarvis MA, Brunner MR, Davidson IF, Litos G, Haselbach D, Mechtler K, Stark H, Schulman BA, and Peters JM

Subjects

Anaphase-Promoting Complex-Cyclosome chemistry, Binding Sites, Cdc20 Proteins chemistry, Enzyme Activation, HeLa Cells, Humans, Mutagenesis, Site-Directed methods, Phosphorylation, Protein Binding, Transfection methods, Anaphase-Promoting Complex-Cyclosome metabolism, Cdc20 Proteins metabolism, Mitosis physiology

Abstract

Chromosome segregation and mitotic exit are initiated by the 1.2-MDa ubiquitin ligase APC/C (anaphase-promoting complex/cyclosome) and its coactivator CDC20 (cell division cycle 20). To avoid chromosome missegregation, APC/C(CDC20) activation is tightly controlled. CDC20 only associates with APC/C in mitosis when APC/C has become phosphorylated and is further inhibited by a mitotic checkpoint complex until all chromosomes are bioriented on the spindle. APC/C contains 14 different types of subunits, most of which are phosphorylated in mitosis on multiple sites. However, it is unknown which of these phospho-sites enable APC/C(CDC20) activation and by which mechanism. Here we have identified 68 evolutionarily conserved mitotic phospho-sites on human APC/C bound to CDC20 and have used the biGBac technique to generate 47 APC/C mutants in which either all 68 sites or subsets of them were replaced by nonphosphorylatable or phospho-mimicking residues. The characterization of these complexes in substrate ubiquitination and degradation assays indicates that phosphorylation of an N-terminal loop region in APC1 is sufficient for binding and activation of APC/C by CDC20. Deletion of the N-terminal APC1 loop enables APC/C(CDC20) activation in the absence of mitotic phosphorylation or phospho-mimicking mutations. These results indicate that binding of CDC20 to APC/C is normally prevented by an autoinhibitory loop in APC1 and that its mitotic phosphorylation relieves this inhibition. The predicted location of the N-terminal APC1 loop implies that this loop controls interactions between the N-terminal domain of CDC20 and APC1 and APC8. These results reveal how APC/C phosphorylation enables CDC20 to bind and activate the APC/C in mitosis.

Published

2016

4. Peroxisome proliferator-activated receptor β/δ cross talks with E2F and attenuates mitosis in HRAS-expressing cells.

Author

Zhu B, Khozoie C, Bility MT, Ferry CH, Blazanin N, Glick AB, Gonzalez FJ, and Peters JM

Subjects

Animals, Cells, Cultured, Keratinocytes metabolism, Mice, Proto-Oncogene Proteins p21(ras) genetics, Signal Transduction, E2F4 Transcription Factor metabolism, G2 Phase Cell Cycle Checkpoints, Mitosis, PPAR delta metabolism, PPAR-beta metabolism, Proto-Oncogene Proteins p21(ras) biosynthesis, Receptor Cross-Talk

Abstract

The role of peroxisome proliferator-activated receptor β/δ (PPARβ/δ) in Harvey sarcoma ras (Hras)-expressing cells was examined. Ligand activation of PPARβ/δ caused a negative selection with respect to cells expressing higher levels of the Hras oncogene by inducing a mitotic block. Mitosis-related genes that are predominantly regulated by E2F were induced to a higher level in HRAS-expressing Pparβ/δ-null keratinocytes compared to HRAS-expressing wild-type keratinocytes. Ligand-activated PPARβ/δ repressed expression of these genes by direct binding with p130/p107, facilitating nuclear translocation and increasing promoter recruitment of p130/p107. These results demonstrate a novel mechanism of PPARβ/δ cross talk with E2F signaling. Since cotreatment with a PPARβ/δ ligand and various mitosis inhibitors increases the efficacy of increasing G₂/M arrest, targeting PPARβ/δ in conjunction with mitosis inhibitors could become a suitable option for development of new multitarget strategies for inhibiting RAS-dependent tumorigenesis.

Published

2012

5. Systematic phosphorylation analysis of human mitotic protein complexes.

Author

Hegemann B, Hutchins JR, Hudecz O, Novatchkova M, Rameseder J, Sykora MM, Liu S, Mazanek M, Lénárt P, Hériché JK, Poser I, Kraut N, Hyman AA, Yaffe MB, Mechtler K, and Peters JM

Subjects

HeLa Cells, Humans, Phosphorylation physiology, Cell Cycle Proteins metabolism, Mitosis physiology, Protein Kinases metabolism

Abstract

Progression through mitosis depends on a large number of protein complexes that regulate the major structural and physiological changes necessary for faithful chromosome segregation. Most, if not all, of the mitotic processes are regulated by a set of mitotic protein kinases that control protein activity by phosphorylation. Although many mitotic phosphorylation events have been identified in proteome-scale mass spectrometry studies, information on how these phosphorylation sites are distributed within mitotic protein complexes and which kinases generate these phosphorylation sites is largely lacking. We used systematic protein-affinity purification combined with mass spectrometry to identify 1818 phosphorylation sites in more than 100 mitotic protein complexes. In many complexes, the phosphorylation sites were concentrated on a few subunits, suggesting that these subunits serve as "switchboards" to relay the kinase-regulatory signals within the complexes. Consequent bioinformatic analyses identified potential kinase-substrate relationships for most of these sites. In a subsequent in-depth analysis of key mitotic regulatory complexes with the Aurora kinase B (AURKB) inhibitor Hesperadin and a new Polo-like kinase (PLK1) inhibitor, BI 4834, we determined the kinase dependency for 172 phosphorylation sites on 41 proteins. Combination of the results of the cellular studies with Scansite motif prediction enabled us to identify 14 sites on six proteins as direct candidate substrates of AURKB or PLK1.

Published

2011

6. Spatial exclusivity combined with positive and negative selection of phosphorylation motifs is the basis for context-dependent mitotic signaling.

Author

Alexander J, Lim D, Joughin BA, Hegemann B, Hutchins JR, Ehrenberger T, Ivins F, Sessa F, Hudecz O, Nigg EA, Fry AM, Musacchio A, Stukenberg PT, Mechtler K, Peters JM, Smerdon SJ, and Yaffe MB

Subjects

Amino Acid Motifs, Animals, Humans, Peptide Library, Phosphorylation physiology, Xenopus laevis, Evolution, Molecular, Mitosis physiology, Protein Serine-Threonine Kinases metabolism, Signal Transduction physiology, Xenopus Proteins metabolism

Abstract

The timing and localization of events during mitosis are controlled by the regulated phosphorylation of proteins by the mitotic kinases, which include Aurora A, Aurora B, Nek2 (never in mitosis kinase 2), Plk1 (Polo-like kinase 1), and the cyclin-dependent kinase complex Cdk1/cyclin B. Although mitotic kinases can have overlapping subcellular localizations, each kinase appears to phosphorylate its substrates on distinct sites. To gain insight into the relative importance of local sequence context in kinase selectivity, identify previously unknown substrates of these five mitotic kinases, and explore potential mechanisms for substrate discrimination, we determined the optimal substrate motifs of these major mitotic kinases by positional scanning oriented peptide library screening (PS-OPLS). We verified individual motifs with in vitro peptide kinetic studies and used structural modeling to rationalize the kinase-specific selection of key motif-determining residues at the molecular level. Cross comparisons among the phosphorylation site selectivity motifs of these kinases revealed an evolutionarily conserved mutual exclusion mechanism in which the positively and negatively selected portions of the phosphorylation motifs of mitotic kinases, together with their subcellular localizations, result in proper substrate targeting in a coordinated manner during mitosis.

Published

2011

7. Live-cell imaging RNAi screen identifies PP2A-B55alpha and importin-beta1 as key mitotic exit regulators in human cells.

Author

Schmitz MH, Held M, Janssens V, Hutchins JR, Hudecz O, Ivanova E, Goris J, Trinkle-Mulcahy L, Lamond AI, Poser I, Hyman AA, Mechtler K, Peters JM, and Gerlich DW

Subjects

Cell Nucleus Division drug effects, Cell Nucleus Division physiology, Chromosomes metabolism, Cyclin-Dependent Kinases antagonists & inhibitors, Cyclin-Dependent Kinases metabolism, Flavonoids pharmacology, Golgi Apparatus metabolism, HeLa Cells, Histones metabolism, Humans, Image Processing, Computer-Assisted methods, Interphase physiology, Leupeptins pharmacology, Microscopy, Confocal methods, Microscopy, Fluorescence methods, Mitosis drug effects, Models, Biological, Phosphorylation physiology, Piperidines pharmacology, Protein Binding physiology, Protein Phosphatase 2 genetics, RNA, Small Interfering genetics, Spindle Apparatus metabolism, Transfection, beta Karyopherins genetics, Mitosis physiology, Protein Phosphatase 2 metabolism, RNA Interference, beta Karyopherins metabolism

Abstract

When vertebrate cells exit mitosis various cellular structures are re-organized to build functional interphase cells. This depends on Cdk1 (cyclin dependent kinase 1) inactivation and subsequent dephosphorylation of its substrates. Members of the protein phosphatase 1 and 2A (PP1 and PP2A) families can dephosphorylate Cdk1 substrates in biochemical extracts during mitotic exit, but how this relates to postmitotic reassembly of interphase structures in intact cells is not known. Here, we use a live-cell imaging assay and RNAi knockdown to screen a genome-wide library of protein phosphatases for mitotic exit functions in human cells. We identify a trimeric PP2A-B55alpha complex as a key factor in mitotic spindle breakdown and postmitotic reassembly of the nuclear envelope, Golgi apparatus and decondensed chromatin. Using a chemically induced mitotic exit assay, we find that PP2A-B55alpha functions downstream of Cdk1 inactivation. PP2A-B55alpha isolated from mitotic cells had reduced phosphatase activity towards the Cdk1 substrate, histone H1, and was hyper-phosphorylated on all subunits. Mitotic PP2A complexes co-purified with the nuclear transport factor importin-beta1, and RNAi depletion of importin-beta1 delayed mitotic exit synergistically with PP2A-B55alpha. This demonstrates that PP2A-B55alpha and importin-beta1 cooperate in the regulation of postmitotic assembly mechanisms in human cells.

Published

2010

8. Systematic analysis of human protein complexes identifies chromosome segregation proteins.

Author

Hutchins JR, Toyoda Y, Hegemann B, Poser I, Hériché JK, Sykora MM, Augsburg M, Hudecz O, Buschhorn BA, Bulkescher J, Conrad C, Comartin D, Schleiffer A, Sarov M, Pozniakovsky A, Slabicki MM, Schloissnig S, Steinmacher I, Leuschner M, Ssykor A, Lawo S, Pelletier L, Stark H, Nasmyth K, Ellenberg J, Durbin R, Buchholz F, Mechtler K, Hyman AA, and Peters JM

Subjects

Anaphase-Promoting Complex-Cyclosome, Centrosome metabolism, Chromosomes, Artificial, Bacterial, Databases, Genetic, Genomics, Green Fluorescent Proteins, HeLa Cells, Humans, Open Reading Frames, Protein Binding, Protein Interaction Mapping, Protein Subunits metabolism, RNA Interference, Chromosome Segregation, Mitosis, Multiprotein Complexes metabolism, Spindle Apparatus metabolism, Tubulin metabolism, Ubiquitin-Protein Ligase Complexes metabolism

Abstract

Chromosome segregation and cell division are essential, highly ordered processes that depend on numerous protein complexes. Results from recent RNA interference screens indicate that the identity and composition of these protein complexes is incompletely understood. Using gene tagging on bacterial artificial chromosomes, protein localization, and tandem-affinity purification-mass spectrometry, the MitoCheck consortium has analyzed about 100 human protein complexes, many of which had not or had only incompletely been characterized. This work has led to the discovery of previously unknown, evolutionarily conserved subunits of the anaphase-promoting complex and the gamma-tubulin ring complex--large complexes that are essential for spindle assembly and chromosome segregation. The approaches we describe here are generally applicable to high-throughput follow-up analyses of phenotypic screens in mammalian cells.

Published

2010

9. Structure of the anaphase-promoting complex/cyclosome interacting with a mitotic checkpoint complex.

Author

Herzog F, Primorac I, Dube P, Lenart P, Sander B, Mechtler K, Stark H, and Peters JM

Subjects

Anaphase, Anaphase-Promoting Complex-Cyclosome, Cdc20 Proteins, Cell Cycle Proteins chemistry, Cell Cycle Proteins metabolism, HeLa Cells, Humans, Image Processing, Computer-Assisted, Imaging, Three-Dimensional, Microscopy, Electron, Models, Molecular, Protein Binding, Protein Conformation, Protein Structure, Tertiary, Ubiquitin-Conjugating Enzymes chemistry, Ubiquitin-Conjugating Enzymes metabolism, Ubiquitination, Mitosis, Spindle Apparatus metabolism, Ubiquitin-Protein Ligase Complexes chemistry, Ubiquitin-Protein Ligase Complexes metabolism

Abstract

Once all chromosomes are connected to the mitotic spindle (bioriented), anaphase is initiated by the protein ubiquitylation activity of the anaphase-promoting complex/cyclosome (APC/C) and its coactivator Cdc20 (APC/C(Cdc20)). Before chromosome biorientation, anaphase is delayed by a mitotic checkpoint complex (MCC) that inhibits APC/C(Cdc20). We used single-particle electron microscopy to obtain three-dimensional models of human APC/C in various functional states: bound to MCC, to Cdc20, or to neither (apo-APC/C). These experiments revealed that MCC associates with the Cdc20 binding site on APC/C, locks the otherwise flexible APC/C in a "closed" state, and prevents binding and ubiquitylation of a wide range of different APC/C substrates. These observations clarify the structural basis for the inhibition of APC/C by spindle checkpoint proteins.

Published

2009

10. Polo on the Rise-from Mitotic Entry to Cytokinesis with Plk1.

Author

Petronczki M, Lénárt P, and Peters JM

Subjects

Animals, Humans, Kinetochores enzymology, Neoplasms enzymology, Neoplasms therapy, Protein Transport, Polo-Like Kinase 1, Cell Cycle Proteins metabolism, Cytokinesis, Mitosis, Protein Serine-Threonine Kinases metabolism, Proto-Oncogene Proteins metabolism

Abstract

Polo-like kinase 1 (Plk1) is a key regulator of cell division in eukaryotic cells. New techniques, including the application of small-molecule inhibitors, have greatly expanded our knowledge of the functions, targets, and regulation of this key mitotic enzyme. In this review, we focus on how Plk1 is recruited to centrosomes, kinetochores, and the spindle midzone and what the specific tasks of Plk1 at these distinct subcellular structures might be. In particular, we highlight new work on the role of Plk1 in cytokinesis in human cells. Finally, we describe how better understanding of Plk1 functions allows critical evaluation of Plk1 as a potential drug target for cancer therapy.

Published

2008

11. Polo and Aurora kinases: lessons derived from chemical biology.

Author

Taylor S and Peters JM

Subjects

Animals, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Aurora Kinase B, Aurora Kinases, Chromosome Segregation drug effects, Enzyme Inhibitors chemistry, Humans, Polo-Like Kinase 1, Cell Cycle Proteins antagonists & inhibitors, Cell Cycle Proteins metabolism, Enzyme Inhibitors pharmacology, Mitosis drug effects, Protein Serine-Threonine Kinases antagonists & inhibitors, Protein Serine-Threonine Kinases metabolism, Proto-Oncogene Proteins antagonists & inhibitors, Proto-Oncogene Proteins metabolism

Abstract

During the cell division cycle, mitotic entry, spindle assembly, chromosome segregation, and cytokinesis must all be carefully coordinated to ensure that the two daughter cells inherit all the genetic material required for further growth and development. Central to this coordination are several protein kinases including Aurora A, Aurora B, and the Polo-like kinase, Plk1. A number of small-molecule Aurora and Plk1 inhibitors have been developed because these kinases are seen as attractive anticancer drug targets. These inhibitors are now being widely used as chemical biology tools to understand how these kinases ensure faithful genome transmission.

Published

2008

12. Aurora B controls the association of condensin I but not condensin II with mitotic chromosomes.

Author

Lipp JJ, Hirota T, Poser I, and Peters JM

Subjects

Adenosine Triphosphatases chemistry, Aurora Kinase B, Aurora Kinases, Chromatin metabolism, Chromosomes, Human metabolism, DNA-Binding Proteins chemistry, Fluorescent Dyes metabolism, Green Fluorescent Proteins metabolism, HeLa Cells, Humans, Indoles pharmacology, Kinetics, Microscopy, Video, Multiprotein Complexes chemistry, Phosphorylation, Protein Subunits chemistry, Substrate Specificity, Sulfonamides pharmacology, Adenosine Triphosphatases metabolism, Chromosomes, Human enzymology, DNA-Binding Proteins metabolism, Mitosis, Multiprotein Complexes metabolism, Protein Serine-Threonine Kinases metabolism

Abstract

The assembly of mitotic chromosomes is controlled by condensin complexes. In vertebrates, condensin I binds to chromatin in prometaphase, confers rigidity to chromosomes and enables the release of cohesin complexes from chromosome arms, whereas condensin II associates with chromosomes in prophase and promotes their condensation. Both complexes are essential for chromosome segregation in anaphase. Although the association of condensins with chromatin is important for the assembly and segregation of mitotic chromosomes, it is poorly understood how this process is controlled. Here we show that the mitotic kinase Aurora B regulates the association of condensin I, but not the interaction of condensin II with chromatin. Quantitative time-lapse imaging of cells expressing GFP-tagged condensin subunits revealed that Aurora B is required for efficient loading of condensin I onto chromosomes in prometaphase and for maintenance of the complex on chromosomes in later stages of mitosis. The three non-SMC subunits of condensin I are Aurora B substrates in vitro and their mitosis-specific phosphorylation depends on Aurora B in vivo. Our data indicate that Aurora B contributes to chromosome rigidity and segregation by promoting the binding of condensin I to chromatin. We have also addressed how Aurora B might mediate the dissociation of cohesin from chromosome arms.

Published

2007

13. The small-molecule inhibitor BI 2536 reveals novel insights into mitotic roles of polo-like kinase 1.

Author

Lénárt P, Petronczki M, Steegmaier M, Di Fiore B, Lipp JJ, Hoffmann M, Rettig WJ, Kraut N, and Peters JM

Subjects

Dose-Response Relationship, Drug, Enzyme Inhibitors metabolism, HeLa Cells, Humans, Image Processing, Computer-Assisted, Microscopy, Electron, Transmission, Microscopy, Fluorescence, Microtubules metabolism, Protein Serine-Threonine Kinases metabolism, Proto-Oncogene Proteins metabolism, Pteridines metabolism, Spindle Apparatus metabolism, Polo-Like Kinase 1, Cell Cycle Proteins antagonists & inhibitors, Cell Cycle Proteins metabolism, Enzyme Inhibitors pharmacology, F-Box Proteins metabolism, Microtubules drug effects, Mitosis physiology, Protein Serine-Threonine Kinases antagonists & inhibitors, Proto-Oncogene Proteins antagonists & inhibitors, Pteridines pharmacology, Spindle Apparatus drug effects

Abstract

Background: The mitotic kinases, Cdk1, Aurora A/B, and Polo-like kinase 1 (Plk1) have been characterized extensively to further understanding of mitotic mechanisms and as potential targets for cancer therapy. Cdk1 and Aurora kinase studies have been facilitated by small-molecule inhibitors, but few if any potent Plk1 inhibitors have been identified., Results: We describe the cellular effects of a novel compound, BI 2536, a potent and selective inhibitor of Plk1. The fact that BI 2536 blocks Plk1 activity fully and instantaneously enabled us to study controversial and unknown functions of Plk1. Cells treated with BI 2536 are delayed in prophase but eventually import Cdk1-cyclin B into the nucleus, enter prometaphase, and degrade cyclin A, although BI 2536 prevents degradation of the APC/C inhibitor Emi1. BI 2536-treated cells lack prophase microtubule asters and thus polymerize mitotic microtubules only after nuclear-envelope breakdown and form monopolar spindles that do not stably attach to kinetochores. Mad2 accumulates at kinetochores, and cells arrest with an activated spindle-assembly checkpoint. BI 2536 prevents Plk1's enrichment at kinetochores and centrosomes, and when added to metaphase cells, it induces detachment of microtubules from kinetochores and leads to spindle collapse., Conclusions: Our results suggest that Plk1's accumulation at centrosomes and kinetochores depends on its own activity and that this activity is required for maintaining centrosome and kinetochore function. Our data also show that Plk1 is not required for prophase entry, but delays transition to prometaphase, and that Emi1 destruction in prometaphase is not essential for APC/C-mediated cyclin A degradation.

Published

2007

14. Human Scc4 is required for cohesin binding to chromatin, sister-chromatid cohesion, and mitotic progression.

Author

Watrin E, Schleiffer A, Tanaka K, Eisenhaber F, Nasmyth K, and Peters JM

Subjects

Amino Acid Sequence, Animals, Antibodies, Cell Cycle Proteins chemistry, Cell Cycle Proteins physiology, Centromere physiology, Chromosomal Proteins, Non-Histone analysis, Chromosomal Proteins, Non-Histone genetics, Chromosomal Proteins, Non-Histone immunology, DNA-Binding Proteins, HeLa Cells, Humans, Interphase physiology, Mice, Molecular Sequence Data, Prometaphase physiology, Protein Kinases physiology, Protein Serine-Threonine Kinases, Rats, Saccharomyces cerevisiae Proteins chemistry, Sequence Alignment, Xenopus, Xenopus Proteins genetics, Xenopus Proteins immunology, Cohesins, Cell Cycle Proteins metabolism, Chromatids physiology, Chromatin metabolism, Chromosomal Proteins, Non-Histone metabolism, Chromosomal Proteins, Non-Histone physiology, Mitosis physiology, Nuclear Proteins metabolism

Abstract

Background: Sister-chromatid cohesion depends on the cohesin complex whose association with chromatin is mediated by Scc2 and Scc4 in budding yeast. Both cohesin and Scc2 have been conserved from yeast to humans, but no Scc4 orthologs have been identified. Mutation of Scc2 orthologs causes defects in cohesion, transcription, and development, resulting in Cornelia de Lange syndrome in humans., Results: We have identified a family of tetratricopeptide repeat proteins that share weak sequence similarities with yeast Scc4. This family includes MAU-2, which is required for development of the nervous system in Caenorhabditis elegans. We show that the human member of this family is associated with Scc2, is bound to chromatin from telophase until prophase, and is required for association of cohesin with chromatin during interphase. Cells lacking Scc4 lose sister-chromatid cohesion precociously and arrest in prometaphase. Mitotic chromosomes in Scc4-depleted cells lack cohesin, even though the cohesin-protecting proteins Sgo1 and Bub1 are normally enriched at centromeres and separase does not seem to be active., Conclusion: Our data indicate that human Scc4 is required for the association of cohesin with chromatin, which is a prerequisite for the establishment of sister-chromatid cohesion and for chromosome biorientation in mitosis. The proteinaceous machinery that is required for loading of cohesin onto chromatin is therefore conserved from yeast to humans. The finding that Caenorhabditis elegans MAU-2 is an ortholog of Scc4 further supports the notion that the Scc2-Scc4 complex is required for developmental processes in metazoans.

Published

2006

15. Separase: a universal trigger for sister chromatid disjunction but not chromosome cycle progression.

Author

Wirth KG, Wutz G, Kudo NR, Desdouets C, Zetterberg A, Taghybeeglu S, Seznec J, Ducos GM, Ricci R, Firnberg N, Peters JM, and Nasmyth K

Subjects

Anaphase genetics, Animals, Carrier Proteins genetics, Cell Line, Chromosomal Proteins, Non-Histone genetics, Embryonic Development genetics, Female, Fibroblasts, Genes, Lethal genetics, Hematopoietic Stem Cells metabolism, Hepatocytes, Liver Regeneration genetics, Male, Mice, Mice, Knockout, Nuclear Proteins genetics, Polyploidy, Securin, Separase, Cohesins, Cell Cycle genetics, Cell Cycle Proteins genetics, Chromosome Segregation genetics, DNA Replication Timing genetics, Endopeptidases genetics, Mitosis genetics

Abstract

Separase is a protease whose liberation from its inhibitory chaperone Securin triggers sister chromatid disjunction at anaphase onset in yeast by cleaving cohesin's kleisin subunit. We have created conditional knockout alleles of the mouse Separase and Securin genes. Deletion of both copies of Separase but not Securin causes embryonic lethality. Loss of Securin reduces Separase activity because deletion of just one copy of the Separase gene is lethal to embryos lacking Securin. In embryonic fibroblasts, Separase depletion blocks sister chromatid separation but does not prevent other aspects of mitosis, cytokinesis, or chromosome replication. Thus, fibroblasts lacking Separase become highly polyploid. Hepatocytes stimulated to proliferate in vivo by hepatectomy also become unusually large and polyploid in the absence of Separase but are able to regenerate functional livers. Separase depletion in bone marrow causes aplasia and the presumed death of hematopoietic cells other than erythrocytes. Destruction of sister chromatid cohesion by Separase may be a universal feature of mitosis in eukaryotic cells.

Published

2006

16. Condensin I stabilizes chromosomes mechanically through a dynamic interaction in live cells.

Author

Gerlich D, Hirota T, Koch B, Peters JM, and Ellenberg J

Subjects

Centromere physiology, Chromosomal Instability physiology, Chromosome Segregation physiology, HeLa Cells, Humans, Adenosine Triphosphatases physiology, Chromosomes, Human physiology, DNA-Binding Proteins physiology, Mitosis physiology, Multiprotein Complexes physiology

Abstract

Background: Restructuring chromatin into morphologically distinct chromosomes is essential for cell division, but the molecular mechanisms underlying this process are poorly understood. Condensin complexes have been proposed as key factors, although controversial conclusions about their contribution to chromosome structure were reached by different experimental approaches in fixed cells or cell extracts. Their function under physiological conditions still needs to be defined., Results: Here, we investigated the specific functions of condensin I and II in live cells by fluorescence microscopy and RNAi depletion. Photobleaching and quantitative time-lapse imaging showed that GFP-tagged condensin II bound stably to chromosomes throughout mitosis. By contrast, the canonical condensin I interacted dynamically with chromatin after completion of prophase compaction, reaching steady-state levels on chromosomes before congression. In condensin I-depleted cells, compaction was normal, but chromosomes were mechanically labile and unable to withstand spindle forces during alignment. However, normal levels of condensin II were not required for chromosome stability., Conclusions: We conclude that while condensin I seems dispensable for normal chromosome compaction, its dynamic binding after nuclear envelope breakdown locks already condensed chromatin in a rigid state required for mechanically stable spindle attachment.

Published

2006

17. Dissociation of cohesin from chromosome arms and loss of arm cohesion during early mitosis depends on phosphorylation of SA2.

Author

Hauf S, Roitinger E, Koch B, Dittrich CM, Mechtler K, and Peters JM

Subjects

Amino Acid Substitution, Anaphase physiology, Cell Cycle Proteins metabolism, Chromosomal Proteins, Non-Histone, Chromosomes, Human genetics, HeLa Cells, Humans, Molecular Sequence Data, Phosphoproteins, Phosphorylation, Saccharomyces cerevisiae Proteins, Sister Chromatid Exchange, Cohesins, Antigens, Nuclear metabolism, Cell Cycle Proteins genetics, Chromosomes, Human physiology, Fungal Proteins genetics, Mitosis physiology, Nuclear Proteins genetics

Abstract

Cohesin is a protein complex that is required to hold sister chromatids together. Cleavage of the Scc1 subunit of cohesin by the protease separase releases the complex from chromosomes and thereby enables the separation of sister chromatids in anaphase. In vertebrate cells, the bulk of cohesin dissociates from chromosome arms already during prophase and prometaphase without cleavage of Scc1. Polo-like kinase 1 (Plk1) and Aurora-B are required for this dissociation process, and Plk1 can phosphorylate the cohesin subunits Scc1 and SA2 in vitro, consistent with the possibility that cohesin phosphorylation by Plk1 triggers the dissociation of cohesin from chromosome arms. However, this hypothesis has not been tested yet, and in budding yeast it has been found that phosphorylation of Scc1 by the Polo-like kinase Cdc5 enhances the cleavability of cohesin, but does not lead to separase-independent dissociation of cohesin from chromosomes. To address the functional significance of cohesin phosphorylation in human cells, we have searched for phosphorylation sites on all four subunits of cohesin by mass spectrometry. We have identified numerous mitosis-specific sites on Scc1 and SA2, mutated them, and expressed nonphosphorylatable forms of both proteins stably at physiological levels in human cells. The analysis of these cells lines, in conjunction with biochemical experiments in vitro, indicate that Scc1 phosphorylation is dispensable for cohesin dissociation from chromosomes in early mitosis but enhances the cleavability of Scc1 by separase. In contrast, our data reveal that phosphorylation of SA2 is essential for cohesin dissociation during prophase and prometaphase, but is not required for cohesin cleavage by separase. The similarity of the phenotype obtained after expression of nonphosphorylatable SA2 in human cells to that seen after the depletion of Plk1 suggests that SA2 is the critical target of Plk1 in the cohesin dissociation pathway.

Published

2005

18. Shugoshin prevents dissociation of cohesin from centromeres during mitosis in vertebrate cells.

Author

McGuinness BE, Hirota T, Kudo NR, Peters JM, and Nasmyth K

Subjects

Amino Acid Sequence, Anaphase physiology, Animals, Base Sequence, Chromosomal Proteins, Non-Histone, DNA Primers, HeLa Cells, Humans, Mice, Molecular Sequence Data, Peptide Fragments chemistry, Proteins chemistry, Proteins genetics, RNA, Small Interfering genetics, Sister Chromatid Exchange, Cohesins, Cell Cycle Proteins physiology, Centromere physiology, Fungal Proteins physiology, Mitosis physiology, Nuclear Proteins physiology

Abstract

Cohesion between sister chromatids is essential for their bi-orientation on mitotic spindles. It is mediated by a multisubunit complex called cohesin. In yeast, proteolytic cleavage of cohesin's alpha kleisin subunit at the onset of anaphase removes cohesin from both centromeres and chromosome arms and thus triggers sister chromatid separation. In animal cells, most cohesin is removed from chromosome arms during prophase via a separase-independent pathway involving phosphorylation of its Scc3-SA1/2 subunits. Cohesin at centromeres is refractory to this process and persists until metaphase, whereupon its alpha kleisin subunit is cleaved by separase, which is thought to trigger anaphase. What protects centromeric cohesin from the prophase pathway? Potential candidates are proteins, known as shugoshins, that are homologous to Drosophila MEI-S332 and yeast Sgo1 proteins, which prevent removal of meiotic cohesin complexes from centromeres at the first meiotic division. A vertebrate shugoshin-like protein associates with centromeres during prophase and disappears at the onset of anaphase. Its depletion by RNA interference causes HeLa cells to arrest in mitosis. Most chromosomes bi-orient on a metaphase plate, but precocious loss of centromeric cohesin from chromosomes is accompanied by loss of all sister chromatid cohesion, the departure of individual chromatids from the metaphase plate, and a permanent cell cycle arrest, presumably due to activation of the spindle checkpoint. Remarkably, expression of a version of Scc3-SA2 whose mitotic phosphorylation sites have been mutated to alanine alleviates the precocious loss of sister chromatid cohesion and the mitotic arrest of cells lacking shugoshin. These data suggest that shugoshin prevents phosphorylation of cohesin's Scc3-SA2 subunit at centromeres during mitosis. This ensures that cohesin persists at centromeres until activation of separase causes cleavage of its alpha kleisin subunit. Centromeric cohesion is one of the hallmarks of mitotic chromosomes. Our results imply that it is not an intrinsically stable property, because it can easily be destroyed by mitotic kinases, which are kept in check by shugoshin.

Published

2005

19. Distinct functions of condensin I and II in mitotic chromosome assembly.

Author

Hirota T, Gerlich D, Koch B, Ellenberg J, and Peters JM

Subjects

Cell Cycle Proteins metabolism, Cell Line, Chromatin metabolism, Chromosomal Proteins, Non-Histone genetics, Cytoplasm metabolism, Fungal Proteins metabolism, HeLa Cells, Heterochromatin metabolism, Humans, Microscopy, Confocal, Microscopy, Video, Nuclear Proteins metabolism, Prometaphase, Prophase, RNA Interference, Cohesins, Chromosomal Proteins, Non-Histone metabolism, Chromosomes metabolism, Mitosis

Abstract

Condensin is a protein complex associated with mitotic chromosomes that has been implicated in chromosome condensation. In vertebrates, two types of condensin complexes have recently been identified, called condensin I and II. Here, we show that in mammalian cells condensin II associates with chromatin in prophase, in contrast to condensin I which is cytoplasmic and can thus interact with chromosomes only after nuclear envelope breakdown. RNA interference experiments in conjunction with imaging of live and fixed cells revealed that condensin II is required for chromosome condensation in early prophase, whereas condensin I appears to be dispensable at this stage. By contrast, condensin I is required for the complete dissociation of cohesin from chromosome arms, for chromosome shortening and for normal timing of progression through prometaphase and metaphase, whereas normal condensin II levels are dispensable for these processes. After depletion of both condensin complexes, the onset of chromosome condensation is delayed until the end of prophase, but is then initiated rapidly before nuclear envelope breakdown. These results reveal that condensin II and I associate with chromosomes sequentially and have distinct functions in mitotic chromosome assembly.

Published

2004

20. The E2-C vihar is required for the correct spatiotemporal proteolysis of cyclin B and itself undergoes cyclical degradation.

Author

Máthé E, Kraft C, Giet R, Deák P, Peters JM, and Glover DM

Subjects

Anaphase-Promoting Complex-Cyclosome, Animals, Base Sequence, Blotting, Western, Cells, Cultured, Centrosome metabolism, DNA Primers, Drosophila metabolism, Drosophila Proteins genetics, HeLa Cells, Humans, Immunohistochemistry, Immunoprecipitation, In Situ Hybridization, Molecular Sequence Data, Mutagenesis, Peptide Hydrolases metabolism, Phylogeny, Plasmids genetics, RNA Interference, Sequence Analysis, DNA, Spindle Apparatus metabolism, Ubiquitin-Conjugating Enzymes genetics, Cyclin B metabolism, Drosophila embryology, Drosophila Proteins metabolism, Mitosis physiology, Ubiquitin-Conjugating Enzymes metabolism, Ubiquitin-Protein Ligase Complexes metabolism

Abstract

Background: Proteolytic degradation of mitotic regulatory proteins first requires these targets to be ubiquitinated. This is regulated at the level of conjugation of ubiquitin to substrates by the anaphase-promoting complex/cyclosome (APC/C) ubiquitin-protein ligase. Substrate specificity and temporal activity of the APC/C has been thought to lie primarily with its two activators, Cdc20/Fizzy and Cdh1/Fizzy-related., Results: Here, we show that reduction in the E2 ubiquitin-conjugating enzyme (UBC) of the E2-C family that is encoded by the Drosophila gene vihar (vih), by either mutation or RNAi, leads to an accumulation of cells in a metaphase-like state. Cyclin B accumulates to high levels in all mitotic vih cells, particularly at the spindle poles. Vihar E2-C is present in the cytoplasm of mitotic cells but also associates with centrosomes, and its own degradation is initiated at the metaphase-anaphase transition. Expression of destruction D box mutants of vihar in the syncytial embryo results in mitotic arrest at late anaphase. In contrast to hypomorphic mutants, Cyclin B is degraded at the spindle poles and accumulates in the equatorial region of the spindle., Conclusions: In Drosophila, the Vihar E2 UBC contributes to the spatiotemporal control of Cyclin B degradation that first occurs at the spindle poles. APC/C-mediated proteolysis of Vihar E2-C autoinactivates the APC/C at the centrosome before a second wave of proteolysis to degrade Cyclin B on the rest of the spindle and elsewhere in the cell.

Published

2004

21. Regulation of sister chromatid cohesion between chromosome arms.

Author

Giménez-Abián JF, Sumara I, Hirota T, Hauf S, Gerlich D, de la Torre C, Ellenberg J, and Peters JM

Subjects

Animals, Aurora Kinase B, Aurora Kinases, Cell Cycle Proteins metabolism, Cells, Cultured cytology, Chromosomal Proteins, Non-Histone, Endopeptidases metabolism, Fungal Proteins, HeLa Cells cytology, Humans, Immunoblotting, Metaphase physiology, Microscopy, Fluorescence, Nuclear Proteins physiology, Protein Kinases, Protein Serine-Threonine Kinases, Proto-Oncogene Proteins, RNA Interference, Rats, Separase, Cohesins, Polo-Like Kinase 1, Chromatids physiology, Chromosomes, Human physiology, Mitosis physiology, Models, Biological, Nuclear Proteins metabolism

Abstract

Sister chromatid separation in anaphase depends on the removal of cohesin complexes from chromosomes. In vertebrates, the bulk of cohesin is already removed from chromosome arms during prophase and prometaphase, whereas cohesin remains at centromeres until metaphase, when cohesin is cleaved by the protease separase. In unperturbed mitoses, arm cohesion nevertheless persists throughout metaphase and is principally sufficient to maintain sister chromatid cohesion. How arm cohesion is maintained until metaphase is unknown. Here we show that small amounts of cohesin can be detected in the interchromatid region of metaphase chromosome arms. If prometaphase is prolonged by treatment of cells with microtubule poisons, these cohesin complexes dissociate from chromosome arms, and arm cohesion is dissolved. If cohesin dissociation in prometaphase-arrested cells is prevented by depletion of Plk1 or inhibition of Aurora B, arm cohesion is maintained. These observations imply that, in unperturbed mitoses, small amounts of cohesin maintain arm cohesion until metaphase. When cells lacking Plk1 and Aurora B activity enter anaphase, chromatids lose cohesin. This loss is prevented by proteasome inhibitors, implying that it depends on separase activation. Separase may therefore be able to cleave cohesin at centromeres and on chromosome arms.

Published

2004

22. Mitotic regulation of the human anaphase-promoting complex by phosphorylation.

Author

Kraft C, Herzog F, Gieffers C, Mechtler K, Hagting A, Pines J, and Peters JM

Subjects

Anaphase-Promoting Complex-Cyclosome, Apc1 Subunit, Anaphase-Promoting Complex-Cyclosome, Apc7 Subunit, Anaphase-Promoting Complex-Cyclosome, CDC2 Protein Kinase metabolism, Humans, Mass Spectrometry, Phosphoprotein Phosphatases metabolism, Phosphorylation, Protein Binding, Protein-Tyrosine Kinases metabolism, Thymidine metabolism, Ubiquitin metabolism, Ubiquitin-Protein Ligases chemistry, Ubiquitin-Protein Ligases metabolism, Mitosis physiology, Ubiquitin-Protein Ligase Complexes chemistry, Ubiquitin-Protein Ligase Complexes metabolism

Abstract

The anaphase-promoting complex (APC) or cyclosome is a ubiquitin ligase that initiates anaphase and mitotic exit. APC activation is thought to depend on APC phosphorylation and Cdc20 binding. We have identified 43 phospho-sites on APC of which at least 34 are mitosis specific. Of these, 32 sites are clustered in parts of Apc1 and the tetratricopeptide repeat (TPR) subunits Cdc27, Cdc16, Cdc23 and Apc7. In vitro, at least 15 of the mitotic phospho-sites can be generated by cyclin-dependent kinase 1 (Cdk1), and 3 by Polo-like kinase 1 (Plk1). APC phosphorylation by Cdk1, but not by Plk1, is sufficient for increased Cdc20 binding and APC activation. Immunofluorescence microscopy using phospho-antibodies indicates that APC phosphorylation is initiated in prophase during nuclear uptake of cyclin B1. In prometaphase phospho-APC accumulates on centrosomes where cyclin B ubiquitination is initiated, appears throughout the cytosol and disappears during mitotic exit. Plk1 depletion neither prevents APC phosphorylation nor cyclin A destruction in vivo. These observations imply that APC activation is initiated by Cdk1 already in the nuclei of late prophase cells.

Published

2003

23. The small molecule Hesperadin reveals a role for Aurora B in correcting kinetochore-microtubule attachment and in maintaining the spindle assembly checkpoint.

Author

Hauf S, Cole RW, LaTerra S, Zimmer C, Schnapp G, Walter R, Heckel A, van Meel J, Rieder CL, and Peters JM

Subjects

Anaphase drug effects, Anaphase genetics, Animals, Aurora Kinase B, Aurora Kinases, Cell Cycle Proteins drug effects, Cell Cycle Proteins genetics, Chromosome Segregation drug effects, Chromosome Segregation genetics, Eukaryotic Cells cytology, Eukaryotic Cells drug effects, Genes, cdc drug effects, Genes, cdc physiology, HeLa Cells, Humans, Kinetochores drug effects, Microtubules drug effects, Microtubules genetics, Mitosis drug effects, Nocodazole pharmacology, Paclitaxel pharmacology, Phenotype, Polyploidy, Protein Kinases drug effects, Protein Kinases metabolism, Protein Serine-Threonine Kinases drug effects, Protein Serine-Threonine Kinases genetics, Pyrimidines pharmacology, RNA, Small Interfering genetics, Separase, Spindle Apparatus drug effects, Spindle Apparatus genetics, Thiones pharmacology, Aneugens pharmacology, Endopeptidases, Eukaryotic Cells enzymology, Indoles pharmacology, Kinetochores enzymology, Microtubules enzymology, Mitosis genetics, Protein Serine-Threonine Kinases metabolism, Spindle Apparatus enzymology, Sulfonamides pharmacology

Abstract

The proper segregation of sister chromatids in mitosis depends on bipolar attachment of all chromosomes to the mitotic spindle. We have identified the small molecule Hesperadin as an inhibitor of chromosome alignment and segregation. Our data imply that Hesperadin causes this phenotype by inhibiting the function of the mitotic kinase Aurora B. Mammalian cells treated with Hesperadin enter anaphase in the presence of numerous monooriented chromosomes, many of which may have both sister kinetochores attached to one spindle pole (syntelic attachment). Hesperadin also causes cells arrested by taxol or monastrol to enter anaphase within <1 h, whereas cells in nocodazole stay arrested for 3-5 h. Together, our data suggest that Aurora B is required to generate unattached kinetochores on monooriented chromosomes, which in turn could promote bipolar attachment as well as maintain checkpoint signaling.

Published

2003

24. The anaphase-promoting complex: proteolysis in mitosis and beyond.

Author

Peters JM

Subjects

Anaphase-Promoting Complex-Cyclosome, Animals, Cell Cycle Proteins metabolism, Cyclins physiology, Peptide Hydrolases metabolism, Separase, Signal Transduction, Transforming Growth Factor beta physiology, Ubiquitins metabolism, Endopeptidases, Ligases physiology, Mitosis physiology, Proteasome Endopeptidase Complex, Ubiquitin-Protein Ligase Complexes

Abstract

Key events in mitosis such as sister chromatid separation and subsequent inactivation of cyclin-dependent kinase 1 are regulated by ubiquitin-dependent proteolysis. These events are mediated by the anaphase-promoting complex (APC), a cell cycle-regulated ubiquitin ligase that assembles multiubiquitin chains on regulatory proteins such as securin and cyclins and thereby targets them for destruction by the 26S proteasome.

Published

2002

25. Emi1 is a mitotic regulator that interacts with Cdc20 and inhibits the anaphase promoting complex.

Author

Reimann JD, Freed E, Hsu JY, Kramer ER, Peters JM, and Jackson PK

Subjects

Adenosine Triphosphatases genetics, Amino Acid Sequence, Anaphase-Promoting Complex-Cyclosome, Animals, Cdc20 Proteins, Conserved Sequence, Cyclin A metabolism, Cyclin B metabolism, Drosophila, In Vitro Techniques, Membrane Proteins genetics, Mice, Molecular Sequence Data, Oocytes cytology, Oocytes physiology, Rabbits, Ubiquitin-Protein Ligases, Xenopus, Xenopus Proteins, Cell Cycle Proteins genetics, Cell Cycle Proteins metabolism, Drosophila Proteins, Ligases metabolism, Mitosis physiology, Proteins metabolism, Ubiquitin-Protein Ligase Complexes

Abstract

We have discovered an early mitotic inhibitor, Emi1, which regulates mitosis by inhibiting the anaphase promoting complex/cyclosome (APC). Emi1 is a conserved F box protein containing a zinc binding region essential for APC inhibition. Emi1 accumulates before mitosis and is ubiquitylated and destroyed in mitosis, independent of the APC. Emi1 immunodepletion from cycling Xenopus extracts strongly delays cyclin B accumulation and mitotic entry, whereas nondestructible Emi1 stabilizes APC substrates and causes a mitotic block. Emi1 binds the APC activator Cdc20, and Cdc20 can rescue an Emi1-induced block to cyclin B destruction. Our results suggest that Emi1 regulates progression through early mitosis by preventing premature APC activation, and may help explain the well-known delay between cyclin B/Cdc2 activation and cyclin B destruction.

Published

2001

26. Anaphase-promoting complex/cyclosome-dependent proteolysis of human cyclin A starts at the beginning of mitosis and is not subject to the spindle assembly checkpoint.

Author

Geley S, Kramer E, Gieffers C, Gannon J, Peters JM, and Hunt T

Subjects

Amino Acid Sequence, Anaphase physiology, Anaphase-Promoting Complex-Cyclosome, Cyclin B metabolism, Cyclin B1, Green Fluorescent Proteins, HeLa Cells, Humans, Interphase physiology, Luminescent Proteins metabolism, Metaphase physiology, Molecular Sequence Data, Ubiquitin-Protein Ligases, Cyclin A metabolism, Ligases metabolism, Mitosis physiology, Spindle Apparatus physiology, Ubiquitin-Protein Ligase Complexes

Abstract

Cyclin A is a stable protein in S and G2 phases, but is destabilized when cells enter mitosis and is almost completely degraded before the metaphase to anaphase transition. Microinjection of antibodies against subunits of the anaphase-promoting complex/cyclosome (APC/C) or against human Cdc20 (fizzy) arrested cells at metaphase and stabilized both cyclins A and B1. Cyclin A was efficiently polyubiquitylated by Cdc20 or Cdh1-activated APC/C in vitro, but in contrast to cyclin B1, the proteolysis of cyclin A was not delayed by the spindle assembly checkpoint. The degradation of cyclin B1 was accelerated by inhibition of the spindle assembly checkpoint. These data suggest that the APC/C is activated as cells enter mitosis and immediately targets cyclin A for degradation, whereas the spindle assembly checkpoint delays the degradation of cyclin B1 until the metaphase to anaphase transition. The "destruction box" (D-box) of cyclin A is 10-20 residues longer than that of cyclin B. Overexpression of wild-type cyclin A delayed the metaphase to anaphase transition, whereas expression of cyclin A mutants lacking a D-box arrested cells in anaphase.

Published

2001

27. Splitting the chromosome: cutting the ties that bind sister chromatids.

Author

Nasmyth K, Peters JM, and Uhlmann F

Subjects

Animals, Cell Cycle Proteins metabolism, Chromatids ultrastructure, DNA Replication physiology, Fungal Proteins metabolism, Nuclear Proteins metabolism, Protein Conformation, Spindle Apparatus metabolism, Cohesins, Chromatids metabolism, Chromosomal Proteins, Non-Histone metabolism, Mitosis physiology

Abstract

In eukaryotic cells, replicated DNA molecules remain physically connected from their synthesis in S phase until they are separated during anaphase. This phenomenon, called sister chromatid cohesion, is essential for the temporal separation of DNA replication and mitosis and for the equal separation of the duplicated genome. Recent work has identified a number of chromosomal proteins required for cohesion. In this review we discuss how these proteins may connect sister chromatids and how they are removed from chromosomes to allow sister chromatid separation at the onset of anaphase.

Published

2001

28. Nonperiodic activity of the human anaphase-promoting complex-Cdh1 ubiquitin ligase results in continuous DNA synthesis uncoupled from mitosis.

Author

Sorensen CS, Lukas C, Kramer ER, Peters JM, Bartek J, and Lukas J

Subjects

Anaphase-Promoting Complex-Cyclosome, Antibodies pharmacology, Blotting, Western, Cdc20 Proteins, Cell Cycle Proteins metabolism, Cyclin E metabolism, Cyclin-Dependent Kinase 2, Cyclin-Dependent Kinases metabolism, E2F Transcription Factors, Flow Cytometry, Fluorescent Antibody Technique, Humans, Interphase drug effects, Macromolecular Substances, Protein Binding, Protein Serine-Threonine Kinases metabolism, Retinoblastoma-Binding Protein 1, Transcription Factor DP1, Transcription Factors metabolism, Tumor Cells, Cultured, Ubiquitin-Protein Ligases, CDC2-CDC28 Kinases, Carrier Proteins, Cell Cycle drug effects, DNA Replication drug effects, DNA-Binding Proteins, Drosophila Proteins, Ligases metabolism, Mitosis drug effects, Saccharomyces cerevisiae Proteins, Trans-Activators, Ubiquitin-Protein Ligase Complexes

Abstract

Ubiquitin-proteasome-mediated destruction of rate-limiting proteins is required for timely progression through the main cell cycle transitions. The anaphase-promoting complex (APC), periodically activated by the Cdh1 subunit, represents one of the major cellular ubiquitin ligases which, in Saccharomyces cerevisiae and Drosophila spp., triggers exit from mitosis and during G(1) prevents unscheduled DNA replication. In this study we investigated the importance of periodic oscillation of the APC-Cdh1 activity for the cell cycle progression in human cells. We show that conditional interference with the APC-Cdh1 dissociation at the G(1)/S transition resulted in an inability to accumulate a surprisingly broad range of critical mitotic regulators including cyclin B1, cyclin A, Plk1, Pds1, mitosin (CENP-F), Aim1, and Cdc20. Unexpectedly, although constitutively assembled APC-Cdh1 also delayed G(1)/S transition and lowered the rate of DNA synthesis during S phase, some of the activities essential for DNA replication became markedly amplified, mainly due to a progressive increase of E2F-dependent cyclin E transcription and a rapid turnover of the p27(Kip1) cyclin-dependent kinase inhibitor. Consequently, failure to inactivate APC-Cdh1 beyond the G(1)/S transition not only inhibited productive cell division but also supported slow but uninterrupted DNA replication, precluding S-phase exit and causing massive overreplication of the genome. Our data suggest that timely oscillation of the APC-Cdh1 ubiquitin ligase activity represents an essential step in coordinating DNA replication with cell division and that failure of mechanisms regulating association of APC with the Cdh1 activating subunit can undermine genomic stability in mammalian cells.

Published

2000

29. Mitotic regulation of the APC activator proteins CDC20 and CDH1.

Author

Kramer ER, Scheuringer N, Podtelejnikov AV, Mann M, and Peters JM

Subjects

Anaphase-Promoting Complex-Cyclosome, Animals, Cdc20 Proteins, Cdh1 Proteins, Cell Cycle physiology, Cell Cycle Proteins genetics, Cyclin B metabolism, Embryo, Nonmammalian cytology, Fungal Proteins genetics, HeLa Cells metabolism, Humans, Kinetics, Ligases genetics, Ligases metabolism, Mutation, Phosphorylation, Ubiquitin-Protein Ligases, Xenopus embryology, Cell Cycle Proteins metabolism, Fungal Proteins metabolism, Mitosis, Saccharomyces cerevisiae Proteins, Ubiquitin-Protein Ligase Complexes

Abstract

The ordered activation of the ubiquitin protein ligase anaphase-promoting complex (APC) or cyclosome by CDC20 in metaphase and by CDH1 in telophase is essential for anaphase and for exit from mitosis, respectively. Here, we show that CDC20 can only bind to and activate the mitotically phosphorylated form of the Xenopus and the human APC in vitro. In contrast, the analysis of phosphorylated and nonphosphorylated forms of CDC20 suggests that CDC20 phosphorylation is neither sufficient nor required for APC activation. On the basis of these results and the observation that APC phosphorylation correlates with APC activation in vivo, we propose that mitotic APC phosphorylation is an important mechanism that controls the proper timing of APC(CDC20) activation. We further show that CDH1 is phosphorylated in vivo during S, G2, and M phase and that CDH1 levels fluctuate during the cell cycle. In vitro, phosphorylated CDH1 neither binds to nor activates the APC as efficiently as does nonphosphorylated CDH1. Nonphosphorylatable CDH1 mutants constitutively activate APC in vitro and in vivo, whereas mutants mimicking the phosphorylated form of CDH1 are constitutively inactive. These results suggest that mitotic kinases have antagonistic roles in regulating APC(CDC20) and APC(CDH1); the phosphorylation of APC subunits is required to allow APC activation by CDC20, whereas the phosphorylation of CDH1 prevents activation of the APC by CDH1. These mechanisms can explain the temporal order of APC activation by CDC20 and CDH1 and may help to ensure that exit from mitosis is not initiated before anaphase has occurred.

Published

2000

30. Subunits and substrates of the anaphase-promoting complex.

Author

Peters JM

Subjects

Anaphase-Promoting Complex-Cyclosome, Cyclins metabolism, Ligases chemistry, Substrate Specificity, Ubiquitin-Protein Ligases, Anaphase physiology, Ligases metabolism, Mitosis physiology, Ubiquitin-Protein Ligase Complexes, Ubiquitins metabolism

Abstract

The initiation of anaphase and exit from mitosis depend on a ubiquitination complex called the anaphase-promoting complex (APC) or cyclosome. The APC is composed of more than 10 constitutive subunits and associates with additional regulatory factors in mitosis and during the G1 phase of the cell cycle. At the metaphase-anaphase transition the APC ubiquitinates proteins such as Pds1 in budding yeast and Cut2 in fission yeast whose subsequent degradation by the 26S proteasome is essential for the initiation of sister chromatid separation. Later in anaphase and telophase the APC promotes the inactivation of the mitotic cyclin-dependent protein kinase 1 by ubiquitinating its activating subunit cyclin B. The APC also mediates the ubiquitin-dependent proteolysis of several other mitotic regulators, including other protein kinases, APC activators, spindle-associated proteins, and inhibitors of DNA replication., (Copyright 1999 Academic Press.)

Published

1999

31. Regulation of the cyclin B degradation system by an inhibitor of mitotic proteolysis.

Author

Vorlaufer E and Peters JM

Subjects

Anaphase genetics, Anaphase-Promoting Complex-Cyclosome, Animals, Calcium-Calmodulin-Dependent Protein Kinases metabolism, Cyclin B genetics, Enzyme Activation drug effects, Hydrolysis drug effects, Ligases metabolism, Metaphase drug effects, Mitosis drug effects, Okadaic Acid pharmacology, Ovum, Phosphoprotein Phosphatases antagonists & inhibitors, Phosphoprotein Phosphatases physiology, Protein Phosphatase 1, Protein Phosphatase 2, Proto-Oncogene Proteins c-mos pharmacology, Ubiquitin-Protein Ligases, Ubiquitins metabolism, Xenopus, Cyclin B metabolism, Mitosis physiology, Protease Inhibitors pharmacology, Ubiquitin-Protein Ligase Complexes

Abstract

The initiation of anaphase and exit from mitosis depend on the anaphase-promoting complex (APC), which mediates the ubiquitin-dependent proteolysis of anaphase-inhibiting proteins and mitotic cyclins. We have analyzed whether protein phosphatases are required for mitotic APC activation. In Xenopus egg extracts APC activation occurs normally in the presence of protein phosphatase 1 inhibitors, suggesting that the anaphase defects caused by protein phosphatase 1 mutation in several organisms are not due to a failure to activate the APC. Contrary to this, the initiation of mitotic cyclin B proteolysis is prevented by inhibitors of protein phosphatase 2A such as okadaic acid. Okadaic acid induces an activity that inhibits cyclin B ubiquitination. We refer to this activity as inhibitor of mitotic proteolysis because it also prevents the degradation of other APC substrates. A similar activity exists in extracts of Xenopus eggs that are arrested at the second meiotic metaphase by the cytostatic factor activity of the protein kinase mos. In Xenopus eggs, the initiation of anaphase II may therefore be prevented by an inhibitor of APC-dependent ubiquitination.

Published

1998

32. Identification of BIME as a subunit of the anaphase-promoting complex.

Author

Peters JM, King RW, Höög C, and Kirschner MW

Subjects

Amino Acid Sequence, Animals, Aspergillus chemistry, Aspergillus cytology, Aspergillus metabolism, Cell Cycle Proteins metabolism, Cyclins metabolism, Electrophoresis, Polyacrylamide Gel, Fungal Proteins analysis, Fungal Proteins genetics, Fungal Proteins metabolism, Ligases metabolism, Molecular Sequence Data, Mutation, Ovum, Phosphorylation, Ubiquitin-Protein Ligases, Xenopus laevis, Anaphase, Cell Cycle Proteins chemistry, Fungal Proteins chemistry, Ligases chemistry, Mitosis

Abstract

The initiation of anaphase and exit from mitosis require the activation of a proteolytic system that ubiquitinates and degrades cyclin B. The regulated component of this system is a large ubiquitin ligase complex, termed the anaphase-promoting complex (APC) or cyclosome. Purified Xenopus laevis APC was found to be composed of eight major subunits, at least four of which became phosphorylated in mitosis. In addition to CDC27, CDC16, and CDC23, APC contained a homolog of Aspergillus nidulans BIME, a protein essential for anaphase. Because mutation of bimE can bypass the interphase arrest induced by either nimA mutation or unreplicated DNA, it appears that ubiquitination catalyzed by APC may also negatively regulate entry into mitosis.

Published

1996

33. An NSF-like ATPase, p97, and NSF mediate cisternal regrowth from mitotic Golgi fragments.

Author

Rabouille C, Levine TP, Peters JM, and Warren G

Subjects

Animals, Carrier Proteins pharmacology, Golgi Apparatus ultrastructure, Golgi Matrix Proteins, Membrane Proteins pharmacology, Microscopy, Electron, Molecular Weight, N-Ethylmaleimide-Sensitive Proteins, Rats, Soluble N-Ethylmaleimide-Sensitive Factor Attachment Proteins, Xenopus, Adenosine Triphosphatases physiology, Carrier Proteins physiology, Golgi Apparatus enzymology, Intracellular Membranes physiology, Mitosis physiology, Vesicular Transport Proteins

Abstract

Golgi cisternae regrew in a cell-free system from mitotic Golgi fragments incubated with buffer alone. Pretreatment with NEM or salt washing inhibited regrowth, but this could be restored either by p97, an NSF-like ATPase, or by NSF together with SNAPs and p115, a vesicle docking protein. The morphology of cisternae regrown with p97 and NSF-SNAPs-p115 differed, suggesting that they play distinct roles in rebuilding Golgi cisternae after mitosis.

Published

1995

34. A 20S complex containing CDC27 and CDC16 catalyzes the mitosis-specific conjugation of ubiquitin to cyclin B.

Author

King RW, Peters JM, Tugendreich S, Rolfe M, Hieter P, and Kirschner MW

Subjects

Anaphase physiology, Animals, Apc3 Subunit, Anaphase-Promoting Complex-Cyclosome, Apc6 Subunit, Anaphase-Promoting Complex-Cyclosome, Ligases analysis, Ligases genetics, Ligases metabolism, Macromolecular Substances, Ovum, Recombinant Proteins pharmacology, Saccharomyces cerevisiae Proteins, Subcellular Fractions metabolism, Ubiquitin-Activating Enzymes, Ubiquitin-Conjugating Enzymes, Ubiquitin-Protein Ligases, Xenopus, Cell Cycle Proteins metabolism, Cyclins metabolism, Mitosis physiology, Ubiquitins metabolism

Abstract

Cyclin B is degraded at the onset of anaphase by a ubiquitin-dependent proteolytic system. We have fractionated mitotic Xenopus egg extracts to identify components required for this process. We find that UBC4 and at least one other ubiquitin-conjugating enzyme can support cyclin B ubiquitination. The mitotic specificity of cyclin ubiquitination is determined by a 20S complex that contains homologs of budding yeast CDC16 and CDC27. Because these proteins are required for anaphase in yeast and mammalian cells, we refer to this complex as the anaphase-promoting complex (APC). CDC27 antibodies deplete APC activity, while immunopurified CDC27 complexes are sufficient to complement either interphase extracts or a mixture of recombinant UBC4 and the ubiquitin-activating enzyme E1. These results suggest that APC functions as a regulated ubiquitin-protein ligase that targets cyclin B for destruction in mitosis.

Published

1995

35. Mammotrophic activity in rat serum during the oestrous cycle, pregnancy and lactation

Author

Peters Jm, Uyldert Ie, and A. Th. Ariëns

Subjects

Litter (animal), medicine.medical_specialty, Time Factors, Endocrinology, Diabetes and Metabolism, Mammary gland, Mitosis, Biology, Organ culture, Endocrinology, Organ Culture Techniques, Estrus, Pregnancy, Internal medicine, Lactation, medicine, Weaning, Animals, Estrous cycle, General Medicine, medicine.disease, Placental Lactogen, Prolactin, Rats, medicine.anatomical_structure, Pregnancy, Animal, Female

Abstract

The mammotrophic activity of various serum samples was assessed on the mammary gland of pregnant rats, in organ culture. Insulin was added to the medium. Serum samples from virgin rats showed little activity, and variation in mammotrophic activity during the oestrous cycle was slight. During pregnancy a significant increase in proliferative activity was not seen during the first week, but around day 8–9 mammotrophic activity increased sharply. The activity showed maxima around days 12 and 19. A decrease in the activity between these maxima was not consistently observed. Mammotrophic activity was still present in sera collected during parturition, and 30 min after parturition. It had disappeared completely within 24 h. The mammotrophic factor detectable by organ culture in the serum of pregnant rats could be rat chorionic mammotrophin. Activity in the serum on day 0 and 1 of lactation was comparable to that of virgin rats, but some activity appeared on day 2. High activities were found frequently around day 4 to 6 of lactation. On other days the activity showed fluctuations without a definite pattern. Litter size was of minor importance but the combination of a large litter size and fasting-overnight seemed to suppress the presence of mammotrophic activity in the serum. Nursing was important: after weaning the activity has disappeared, while renewed nursing after weaning resulted in the appearance of high levels of activity. The mitotic activity obtained with lactating rat serum in the culture was suppressed by addition of rabbit anti-rat prolactin serum to the medium. This suggests that the main mammotrophic factor detectable by organ culture in the serum of lactating rats, is prolactin.

Published

1976