1,721,030 research outputs found
Systems-level analysis of the mitotic entry switch
Full text linkEntry into mitosis in eukaryotes depends on the activation of the Cyclin-dependent kinase 1 (Cdk1), which phosphorylates many mitotic protein substrates. Activation of Cdk1 requires formation of a complex with Cyclin B (CycB), which gradually rises in concentration during interphase. However, in most organisms Cdk1 activation is not gradual but switch-like, because phosphorylation of the Cdk1-CycB complex by the Wee1 kinase normally keeps Cdk1-CycB inactive during interphase. Mitotic entry is induced when rapid dephosphorylation of Cdk1-CycB by the Cdc25 phosphatase causes abrupt activation of Cdk1-CycB. Cdk1-CycB in turn phosphorylates both Wee1 and Cdc25 leading to Cdc25 activation and Wee1 inhibition. This regulation creates both a positive and a double-negative feedback loop in the system, which are thought to generate a sharp, bistable switch that controls mitotic entry. Bistability is known to require positive feedback and ultrasensitivity, however, how ultrasensitivity arises in the mitotic switch is subject to extensive research efforts both experimentally and theoretically. In this thesis I explore several possible sources of ultrasensitivity in the mitotic switch through mathematical modelling. Based on theoretical considerations and experimental evidence, I show that the existence of multiple positive feedback loops, multisite phosphorylation, and Cdk1-CycB-dependent regulation of Cdk1-counteracting phosphatase activity can all contribute to ultrasensitivity and bistability in the mitotic switch. I analyse models of the mitotic switch including these bistability-generating mechanisms, to simulate and explain experimental data and make testable predictions. I argue that it is unlikely that a single mechanism is responsible for ultrasensitivity in this system, and that bistability requires a combination of different sources, including the ones studied here and others such as enzyme saturation and sequestration effects. I also highlight the importance of network architecture and coherent regulation of opposing reactions in generating efficient biochemical switches. Finally, I draw on recent experimental evidence and ideas derived from this analysis to propose a revised network of the mitotic switch
Going Beyond Counting First Authors in Author Co-citation Analysis
Full text linkThe present study examines one of the fundamental aspects of author co-citation analysis (ACA) - the way co-citation
counts are defined. Co-citation counting provides the data on which all subsequent statistical analyses and mappings
are based, and we compare ACA results based on two different types of co-citation counting - the traditional type that
only counts the first one among a cited work's authors on the one hand and a non-traditional type that takes into
account the first 5 authors of a cited work on the other hand. Results indicate that the picture produced through this non-traditional author co-citation counting contains more coherent author groups and is therefore considerably clearer. However, this picture represents fewer specialties in the research field being studied than that produced through the traditional first-author co-citation counting when the same number of top-ranked authors is selected and analyzed. Reasons for these effects are discussed
Variations on the Author
Full text link“Variations on the Author” discusses two of Eduardo Coutinho’s recent films (Um Dia na Vida, from 2010, and Últimas Conversas, posthumously released in 2015) and their contribution to the general question of documentary authorship. The director’s filmography is characterized by a consistent yet self-effacing form of authorial self-inscription: Coutinho often features as an interviewer that rather than express opinions propels discourses; an interviewer that is good at listening. This mode of self-inscription characterizes him as an author who is not expressive but who is nonetheless markedly present on the screen. In Um Dia na Vida, however, Coutinho is completely absent form the image, while Últimas Conversas, on the contrary, includes a confessional prologue that moves the director from the margins to the center of his films. This article examines the ways in which these works stand out in the filmography of a director who offers new insights into the notion of cinematic authorship
Appropriate Similarity Measures for Author Cocitation Analysis
Full text linkWe provide a number of new insights into the methodological discussion about author cocitation analysis. We first argue that the use of the Pearson correlation for measuring the similarity between authors’ cocitation profiles is not very satisfactory. We then discuss what kind of similarity measures may be used as an alternative to the Pearson correlation. We consider three similarity measures in particular. One is the well-known cosine. The other two similarity measures have not been used before in the bibliometric literature. Finally, we show by means of an example that our findings have a high practical relevance.information science;Pearson correlation;cosine;similarity measure;author cocitation analysis
Mathematical modelling of mitotic exit control in budding yeast cell cycle
Full text linkThe operating principles of complex regulatory networks are more easily understood with mathematical modelling than by intuitive reasoning. In this thesis, I study the dynamics of the mitotic exit control system in budding yeast. I present a comprehensive mathematical model, which provides a system’s-level understanding of the mitotic exit process. This model captures the dynamics of classic experimental situations reported in the literature, and overcomes a number of limitations present in previous models.Analysis of the model led to a number of breakthroughs in the understanding of mitotic exit control. Firstly, numerical analysis of the model quantified the dependence of mitotic exit on the proteolytic and non-proteolytic functions of separase. It was shown that the requirement for the non-proteolytic function of separase depends on cyclin-dependent kinase activity. Secondly, APC/Cdc20 is a critical node that controls the phosphatase (Cdc14) branch and both cyclin (Clb2 and Clb5) branches of the cell cycle regulatory network. Thirdly, the model proved to be a useful tool for the systematic analysis of the recently discovered phenomenon of Cdc14 endocycles.Most proteins belonging to the cell cycle control network are regulated at the level of synthesis, degradation and activity. Presumably, these multiple layers of regulation facilitate robust cell cycle behaviour in the face of genetic and environmental perturbations. To falsify this hypothesis, I subjected the model to global parameter perturbations and tested viability against pre-defined criteria. According to these analyses, the regulated transcription and degradation of proteins make different contributions to cell cycle control. Regulated degradation confers cell cycle oscillations with robustness against perturbations, while regulated transcription plays a major role in controlling the period of these oscillations. Both regulated transcription and degradation are part of important feedback loops, that combined promote robust behaviour in the face of parametric variations
Mathematical modelling of cell cycle network motifs controlling M-Phase progression
Full text linkEukaryotic cells must coordinate growth, replication of their genetic material, and cell division in order to generate two progeny cells from a single progenitor. M-phase is a critical phase of this process during which newly replicated DNA is precisely segregated into two distinct fractions, followed by cell division to produce two new daughter cells. M-phase is a component of both the mitotic cell cycle, during which each daughter cell should inherit an exact copy of the genetic material from the parent cell, and of meiosis, during which each daughter should receive only half of the genetic material from the parent cell to generate a haploid gamete. Despite these differences, both mitotic and
meiotic M-phases share many of the same regulatory components.
In this thesis we present work from four different studies in which mathematical modelling is used to analyse the behaviour of the biochemical reaction networks controlling M-phase progression in mitosis and meiosis. We firstly present a theoretical analysis of
a conserved network motif (termed here the Feedback-amplified Domineering Substrate or FADS motif), which is responsible for creating bistable switches controlling cell cycle progression at multiple points, including progression through and exit from mitotic M-phase.
We then present three sets of work using mathematical models in combination with data provided by experimental collaborators to examine the regulation of M-phase progression in mitosis and meiosis. We present evidence for how variations on common
regulatory themes can generate the distinct outcomes required in each case.</p
The dynamical properties of the cell cycle control network
Full text linkThe eukaryotic cell cycle is the physiological process by which cells divide and proliferate. Normally, it consists of four phases (G1, S, G2 and M) necessary for carrying out DNA replication, chromosome segregation and division. Under special circumstances, cells bypass some of the canonical phases, giving rise to endocycles, which drive a diversity of developmental processes, such as growth, multi-nucleation, or germ cell generation. Despite ample characterisation of cell cycle biochemistry, the mechanistic requirements for endocycle emergence remain poorly understood. To address this knowledge gap, the work presented here proposes a mechanistic model of the mammalian cell cycle control network which predicts the emergence of endoreplication and mitotic endocycles (Cdc20 endocycles) following molecular perturbations. These predictions are verified experimentally.
Using a control systems approach and analytical tools from the field of nonlinear dynamics, I show that the cell cycle can be framed as a complex oscillatory system, analogous to mechanical devices, such as “Newton’s cradle” or a “Wheel of fortune”, to explain endocycles. Such minimal models explain the organisational principles of the cell cycle in terms of hierarchies of dynamical control motifs. This approach provides general, broadly applicable frameworks, which can guide the experimental dissection of cell cycle regulation, regardless of the model organism choice. Further, the frameworks presented herein provide a scaffold for building tailored mechanistic models for specific organisms and cell types
Mathematical modelling of mitotic controls
Full text linkThe mitotic cell cycle is fundamental to eukaryotic life. In mitosis, replicated chromosomes are segregated to form two new nuclei. This is essential to ensure the maintenance of chromosome number between parent and daughter cells. In higher eukaryotes, numerous cytological changes occur to facilitate the separation of the genetic material: the nuclear envelope breaks down, the mitotic spindle assembles, and the cell rounds-up. There is a well-conserved control network that regulates these processes to bring about the entry into mitosis, the separation of the genetic material, and the reversal of these processes during mitotic exit. To build a coherent model of these regulatory networks requires us to write the biochemical reactions in mathematical form.
The work in this Thesis pertains to three fundamental switches: entry into mitosis, the metaphase-to-anaphase transition, and exit from mitosis. I present three studies from a systems-level perspective. The first investigates a novel bistable mechanism controlling mitotic entry/exit in vitro using purified proteins. Dephosphorylation of Greatwall kinase by the phosphatase PP2A-B55 creates a double negative feedback loop that gives a bistable system response with respect to cyclin-dependent kinase 1 (Cdk1) activity. The second looks at hysteresis between mitotic entry and mitotic exit in HeLa cells. Hysteresis persists when either of the regulatory loops of Cdk1 or its counter-acting phosphatase PP2A-B55 is removed, but is diminished when they are both removed. Finally, the regulation of separase in the metaphase-to-anaphase transition is analysed. Separase that is liberated from securin inhibition is isomerised by Pin1 into a conformation that can bind to cyclin B1. This binding peaks after separase has cleaved cohesin and initiated anaphase.</p
Dispelling the Myths Behind First-author Citation Counts
Full text linkWe conducted a full-scale evaluative citation analysis study of scholars in the XML research field to explore just how different from each other author rankings resulting from different citation counting methods actually are, and to demonstrate the capability of emerging data and tools on the Web in supporting more realistic citation counting methods. Our results contest some common arguments for the continued
use of first-author citation counts in the evaluation of scholars, such as high correlations between author rankings by first-author citation counts and other citation
counting methods, and high costs of using more realistic citation counting methods that are not well-supported by the ISI databases. It is argued that increasingly available digital full text research papers make it possible for citation analysis studies to go beyond what the ISI databases have directly supported and to employ more
sophisticated methods
- …
