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  • About
  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the Networked Digital Library of Theses and Dissertations.
    Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.
121

Elucidation of the Multi-Faceted Roles of the SIN (Septation Initiation Network); Understanding How the SIN Promotes Cytokinesis and Inhibits Interphase Growth in the Fission Yeast Schizosaccharomyces pombe: A Dissertation

Ray, Samriddha 17 August 2010 (has links)
Cytokinesis is the cytoplasmic division of one cell into two independent daughter cells. Precise regulation of cytokinesis during cell cycle is essential for healthy and rapid multiplication of any organism. Schizosaccharomyces pombe has emerged as an excellent model system to study eukaryotic cell division regulation. This rod shaped organism grows by bipolar elongation in interphase when its actin cytoskeleton is concentrated at the cell ends (poles). However, growth stops in mitosis and the actin cytoskeleton is rearranged to facilitate assembly of the contractile actomyosin ring at the cell middle. Although several studies have focused on the separate processes of growth and division, it was unclear how cells regulate the cytoskeletal remodeling during the transition between the different stages of the cell cycle. The Septation Initiation Network (SIN) is a signaling cascade essential for fission yeast cytokinesis (Balasubramanian et al., 1998; Mishra et al., 2004) and the MOR (morphogenesis) signaling pathway is essential for interphase bipolar growth (Kanai et al, 2005). Interestingly, inactivation of the SIN not only failed to maintain the cytokinetic apparatus at the cell middle but also caused the redistribution of the cytoskeletal elements like actin to the cell ends that led to bipolar cell elongation similar to cells in interphase (Mishra et al., 2004). These results suggested that SIN signaling inhibits interphase bipolar growth, but it was not clear if the SIN had a direct role in inhibition of interphase growth during mitosis and this question was the major focus of this thesis. The results presented in Chapter II show a novel cross-pathway interaction between the SIN and the MOR in the fission yeast. Our results in Chapter III suggest that some of the MOR pathway components might be important for coordination between nuclear and cytoplasmic divisions in mitosis, revealing novel roles of the pathway. In a separate study (Chapter IV) we sought to identify additional regulators of the SIN and cytokinesis through a suppressor screen and found that the nucleolar rDNA transcription machinery inhibits cytokinesis in fission yeast.
122

Identification and Characterization of Agv1, a Pre-Metazoan Arf GAP: A Dissertation

Long, Kimberly Renee 20 June 2007 (has links)
Human immunodeficiency virus type 1 (HIV-1) is a member of the lentivirus subfamily of retroviruses. HIV-1 expresses multiple genes from a single provirus by alternative splicing. Early in viral expression, fully spliced 2-kb viral RNA is exported from the nucleus and encodes the viral regulatory protein, Rev, which is essential for nuclear transport of partially spliced and unspliced genomic-length RNA. Rev binds to an RNA structural element called the Rev response element (RRE) and mediates nuclear export through the leucine-rich nuclear export signal (NES) pathway. The human Rev Interacting Protein (hRIP) interacts specifically with the Rev NES. Rev NES mutants that are unable to export Rev-dependent RNAs are also unable to bind to hRIP. The hRIP cDNA encodes a 562 amino acid protein containing an N-terminal zinc finger with homology to Arf GAP domains, a central serine and threonine rich region, and C-terminal phenylalanine-glycine (FG) repeats characteristic of nucleoporins. To identify an hRIP ortholog in a genetically tractable organism, we performed database searches using the N-terminal zinc finger of hRIP. Using this approach, we identified a novel gene in Schizosaccharomyces pombe. Alignment of the entire reading frame of the putative ortholog with hRIP indicates similarity with the serine/threonine rich region and with the FG repeats, suggesting that S. pombecould be a good model system to study the cellular function of hRIP. We find that the S. pombe ORF is an essential gene, which encodes a 483 amino acid protein that is also able to interact with the NES of HIV-1 Rev. Based on being an essential gene, and the presence of a putative Arf GAP domain, the ORF was named an Arf GAP essential for viability, agv1+. We show that Agv1 is not directly involved in the nuclear export of poly(A+) RNA or 5S rRNA, nuclear export of leucine-rich NES-containing proteins, or nuclear import of nuclear localization signal (NLS)-containing proteins. However, Agv1 does appear to play a role in the cytoplasmic localization of 5S rRNA. We demonstrate that loss of Agv1 alters the localization of endoplasmic reticulum (ER) membrane and Golgi membrane resident proteins, accumulates intracellular membrane, and blocks processing of carboxypeptidase Y. Furthermore, the S. cerevisiae ADP-ribosylation factor (Arf) GTPase activating protein (GAP) Glo3, but not a catalytically inactive Glo3 mutant [R59K], is able to partially compensate for the loss of Agv1 function in temperature sensitive strains, indicating that Agv1 is an S. pombe Arf GAP with some functional features similar to S. cerevisiae Glo3.
123

Replication Stress Induced by the Ribonucleotide Reductase Inhibitors Guanazole, Triapine, and Gemcitabine in Fission Yeast

Alyahya, Mashael Yahya A 04 May 2022 (has links)
No description available.
124

Coordinating Cytokinesis with Mitosis by a Conserved Signal Transduction Network in the Fission Yeast Schizosaccharomyces Pombe: a Dissertation

Guertin, David A. 08 November 2002 (has links)
Cytokinesis is the final event of the cell division cycle and results in physical and irreversible separation of a mother cell into two daughter cells. Cytokinesis must only occur after chromosomes have segregated during mitosis to ensure each daughter cell receives the proper complement of genetic material. Failure to execute normal cytokinesis can result in aneuploidy and/or polyploidy, a hallmark of many cancers. Cytokinesis occurs mechanically through constriction of an actin-myosin based contractile ring, while initiation of ring constriction is temporally and spatially mediated by complex signaling networks. It is absolutely crucial that cytokinesis is tightly coordinated with the cell cycle in order to preserve the fidelity of cell division. We hypothesized that to achieve such tight control of cytokinesis, cells may utilize both promotional and inhibitory signals, however how cells maintained this control was poorly understood. The goal of this thesis was to characterize how cells regulate signaling of cytokinesis, both positively and negatively, during cell division using the fission yeast Schizosaccharomyces pombe as a model organism. Two approaches were employed. (1) We first sought to characterize the positive timing mechanism that signals cytokinesis though a detailed investigation of Sid1p, a protein kinase essential for activation of ring constriction. (2) Secondly, we sought to define how cells negatively regulate cytokinesis through investigation of Dma1p, a spindle checkpoint protein implicated in inhibition of cytokinesis. Our results reveal a conserved signaling network, termed the Septation Initiation Network (SIN), of which Sid1p is an intermediate component, that controls temporal and spatial regulation of cytokinesis. We found Sid1p is additionally controlled by Cyclin Dependent Kinase activity, uncovering an important link between mitotic events and initiation of cytokinesis. Furthermore, we found that aberrant SIN activation can override a microtubule-damage-induced spindle checkpoint arrest. This effect is counteracted by Dma1p, which normally inhibits the SIN during checkpoint activation to preserve cell viability until damage is repaired. We conclude that signaling cytokinesis is tightly coordinated with mitosis in S. pombe by positive signals acting through Sid1p and the SIN, and under certain conditions, negative signals acting through Dma1p. Considering the conservation of cell cycle regulators in the eukaryotic kingdom, it is likely that similar mechanisms to control cytokinesis exist in humans.
125

Understanding Regulation of the Cytoskeleton during Cell Cycle Transitions through Examination of Crosstalk between Homologous Fission Yeast Pathways, Septation Initiation Network and Morphogenesis ORB6 Network: A Dissertation

Gupta, Sneha 10 December 2013 (has links)
The fission yeast Schizosaccharomyces pombe has become a powerful model system for studying cytokinesis, a process of cytoplasmic division by which one cell divides into two identical daughter cells. Like mammalian cells, S. pombe divides through the use of an actomyosin contractile ring, which is composed of a set of highly conserved cytoskeletal proteins. Cytokinesis in S. pombe is primarily regulated by the SIN pathway, which is activated in late mitosis and is required for actomyosin contractile ring and septum assembly, and also plays a role in spindle checkpoint inactivation, and telophase nuclear positioning. The various functions of the SIN are carried out by the terminal kinase in the pathway called Sid2. The lack of information in the downstream targets of Sid2 has limited our understanding of the different functions of the SIN. We recently showed that, in addition to its other functions, the SIN promotes cytokinesis through inhibition the MOR signaling pathway, which normally drives cell separation and initiation of polarized growth following completion of cytokinesis (Ray et al, 2010). The molecular details of this inhibition and the physiological significance of inhibiting MOR during cytokinesis was unclear. The results presented in Chapter II describe our approach to identify Sid2 substrates, particularly focusing on Nak1 and Sog2 that function in the MOR signaling cascade. We identified and characterized Sid2 phosphorylation sites on the Nak1 and Sog2 proteins. Chapter III explores how post translational modification of MOR proteins by Sid2 regulates polarized growth during cytokinesis. This includes delineating the effect of Sid2 mediated phosphorylation of Nak1 and Sog2 on protein-protein interactions in the MOR pathway as well as on the regulation of their localization during late mitosis. Finally, results in Chapter IV demonstrate that failure to inhibit MOR signaling is lethal because cells initiate septum degradation/cell separation before completing cytokinesis thereby emphasizing the importance of cross-regulation between the two pathways to prevent initiation of the interphase polarity program during cytokinesis.
126

Untersuchungen zur Regulation des TSC - Komplexes in Schizosaccharomyces pombe

Schaubitzer, Kerstin 07 September 2009 (has links)
Die Anpassung des Zellwachstums eukaryotischer und prokaryotischer Zellen an sich ändernde intra- und extrazelluläre Signale wie Nährstoffverfügbarkeit, Wachstumsfaktoren und dem zellulären Energielevel bedarf eines effektiven Regulationssystems. In Säugern übernimmt der TSC-Komplex als negativer Regulator des TOR-Signalweges eine wichtige Rolle bei der Regulation des Zellwachstums. In S. pombe ist der TSC-Komplex konserviert. Zudem existieren Homologe der Untereinheiten der AMPK, welche in Säugern den TSC-Komplex positiv regulieren. In der vorliegenden Arbeit konnte die Existenz von zwei funktionell getrennten AMPK-Komplexen nachgewiesen werden: AMPK I, bestehend aus Ssp2, SPCC1919.03c und Cbs2 und AMPK II, bestehend aus Ppk9, SPCC1919.03c und Cbs2. Genetische Daten lassen eine Beteiligung von AMPK I an der Regulation der sexuellen Differenzierung, der Adaption an osmotischen Stress und der Verwertung nicht-fermentierbarer Kohlenstoffquellen vermuten. AMPK II scheint für die Adaption an Cadmiumstress wichtig zu sein.In der vorliegenden Arbeit wurde weiterhin die Beteiligung der beiden AMPK alpha-Isoformen am TSC/Rhb1/TOR-Signalweg in S. pombe näher untersucht. Dabei deutete sich an, dass Ppk9 und der TSC-Komplex weder synergistische noch antagonistische Funktionen in der Zelle ausüben. Im Gegensatz dazu scheinen Ssp2 und die TSC-Proteine antagonistische Funktionen auszuüben. Einige Wachstumsdefekte der ssp2 -Deletionsmutanten können durch eine Hyperaktivierung des TSC/Rhb1/TOR-Signalweges supprimiert werden. Die Deletion von ssp2 führt zu einer Suppression des Wachstumsdefektes von Leucin-auxotrophen tsc-Mutanten. Diese Beobachtung erlaubt die Einordnung von Ssp2 in einem zum TSC/Rhb1/TOR-Weg parallelen Signalweg. Im Gegensatz zu Säugern scheinen in S. pombe TSC/Rhb1/TORC1 und Ssp2 einen gemeinsamen Effektor unabhängig voneinander zu regulieren, um verschiedene Wachstumsbedingungen miteinander zu integrieren und das Zellwachstum entsprechend anzupassen.
127

Genetic studies of genes involved in the initiation of DNA replication in the fission yeast Schizosaccharomyces pombe

Wang, Zhuo 28 October 2010 (has links)
No description available.
128

Histone H4 Acetylation in the DNA Damage Response and Telomere Formation of <i>Schizosaccharomyces pombe</i>

Eisenstatt, Jessica R. 27 January 2016 (has links)
No description available.
129

Fission Yeast as a Model Organism for FUS-Dependent Cytotoxicity in Amyotrophic Lateral Sclerosis

Cone, Alan J. 06 September 2016 (has links)
No description available.
130

Telomere Regulation and Heterochromatin Formation in Yeasts

Wang, Jinyu 08 February 2017 (has links)
No description available.

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