Mitotic Spindle Form and Function

Winey, Mark; Bloom, Kerry

doi:10.1534/genetics.111.128710

Cited by 125 publications

(150 citation statements)

References 236 publications

(376 reference statements)

Supporting

Mentioning

143

Contrasting

Unclassified

Order By: Relevance

“…Loss of its function causes arrest at the M/G1 transition, and it is required for cytokinesis even when this block to G1 entry is overridden by overexpression of a CDK inhibitor (Gruneberg et al 2000;Luca et al 2001;Yoshida et al 2002). It associates with the cytoplasmic face of the SPB, which is embedded in the nuclear envelope (Winey and Bloom 2012). Nud1 recruits other components of the MEN to the SPB, and this localization is critical for MEN activation Cenamor et al 1999;Shou et al 1999;Visintin and Amon 2001;Molk et al 2004;Rock and Amon 2011;Valerio-Santiago and Monje-Casas 2011).…”

Section: Menmentioning

confidence: 99%

“…I mention some critical subjects largely in overview that are described extensively elsewhere. These include the late mitotic spindle and contraction of the cytokinetic apparatus, which are covered in other YeastBook chapters by Bi and Park (2012) and Winey and Bloom (2012), respectively, and are also reviewed extensively elsewhere (Tolliday et al 2001;Walther and Wendland 2003;Balasubramanian et al 2004;Moseley and Goode 2006;Moseley and Nurse 2009;Roncero and Sanchez 2010).…”

mentioning

confidence: 99%

See 1 more Smart Citation

Mitotic Exit and Separation of Mother and Daughter Cells

2012

View full text Add to dashboard Cite

Productive cell proliferation involves efficient and accurate splitting of the dividing cell into two separate entities. This orderly process reflects coordination of diverse cytological events by regulatory systems that drive the cell from mitosis into G1. In the budding yeast Saccharomyces cerevisiae, separation of mother and daughter cells involves coordinated actomyosin ring contraction and septum synthesis, followed by septum destruction. These events occur in precise and rapid sequence once chromosomes are segregated and are linked with spindle organization and mitotic progress by intricate cell cycle control machinery. Additionally, critical parts of the mother/daughter separation process are asymmetric, reflecting a form of fate specification that occurs in every cell division. This chapter describes central events of budding yeast cell separation, as well as the control pathways that integrate them and link them with the cell cycle.

show abstract

Section: Menmentioning

confidence: 99%

mentioning

confidence: 99%

Mitotic Exit and Separation of Mother and Daughter Cells

2012

View full text Add to dashboard Cite

show abstract

“…They switch stochastically between phases of assembly and disassembly, a behavior called dynamic instability (Mitchison and Kirschner 1984). Microtubules are nucleated by the centrosome, which is called the spindle pole body (SPB) in yeast (Winey and Bloom 2012). Microtubules have an inherent polarity with the minus end embedded in the SPB and the dynamic plus end distal.…”

mentioning

confidence: 99%

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

2013

View full text Add to dashboard Cite

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

show abstract

“…Those include dramatic changes in morphogenesis leading to the formation of the bud, the nascent daughter cell with its associated septin ring marking the future site of cytokinesis (reviewed in Bi and Park 2012;Howell and Lew 2012). Additionally, the duplication of the spindle pole body, the first structures associated with assembly of the mitotic spindle (reviewed by Winey and Bloom 2012), and the initiation of DNA replication are triggered following START (reviewed by Remus and Diffley 2009). Although the separation of function is by no means absolute, in general, many genes involved in morphogenesis, including enzymes required for cell wall biosynthesis and septin ring components, are regulated by SBF, whereas genes for DNA replication and repair, including nucleotide biosynthetic enzymes and proteins acting at the replication fork, are regulated by MBF.…”

Section: The G1/s Gene Clustermentioning

confidence: 99%

Topology and Control of the Cell-Cycle-Regulated Transcriptional Circuitry

Haase

Wittenberg

2014

Genetics

View full text Add to dashboard Cite

Nearly 20% of the budding yeast genome is transcribed periodically during the cell division cycle. The precise temporal execution of this large transcriptional program is controlled by a large interacting network of transcriptional regulators, kinases, and ubiquitin ligases. Historically, this network has been viewed as a collection of four coregulated gene clusters that are associated with each phase of the cell cycle. Although the broad outlines of these gene clusters were described nearly 20 years ago, new technologies have enabled major advances in our understanding of the genes comprising those clusters, their regulation, and the complex regulatory interplay between clusters. More recently, advances are being made in understanding the roles of chromatin in the control of the transcriptional program. We are also beginning to discover important regulatory interactions between the cell-cycle transcriptional program and other cell-cycle regulatory mechanisms such as checkpoints and metabolic networks. Here we review recent advances and contemporary models of the transcriptional network and consider these models in the context of eukaryotic cellcycle controls. TABLE OF CONTENTS Abstract 65Introduction 66

show abstract

Mitotic Spindle Form and Function

Cited by 125 publications

References 236 publications

Mitotic Exit and Separation of Mother and Daughter Cells

Mitotic Exit and Separation of Mother and Daughter Cells

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

Topology and Control of the Cell-Cycle-Regulated Transcriptional Circuitry

Contact Info

Product

Resources

About