The development of models for computer simulation with detailed application to a CDC 6400 system

Beaumont, William Paul.

January 1975

No description available.

Computer simulation

Control date 6400 computer

Scalability Modeling for Optimal Provisioning of Data Centers in Telenor : A better balance between under- and over-provisioning

Rygg, Knut Helge

January 2012

The scalability of an information system describes the relationship between system ca-pacity and system size. This report studies the scalability of Microsoft Lync Server 2010 in order to provide guidelines for provisioning hardware resources. Optimal pro-visioning is required to reduce both deployment and operational costs, while keeping an acceptable service quality.All Lync servers in the test setup are virtualizedusingVMware ESXi 5.0 and the system runs on a Cisco Unified Computing System (UCS) platform. The scenario is a typical hosted Lync deployment with external users only and telephone integration. While several companies offer hosted virtual Lync deployments and the Cisco UCS platform has a rich market share, Microsoft’s capacity planning guides don’t provide help for such a deployment scenario or hardware platform. This report consequently fill an information gap.The scalability is determined by using empirical measurements with different work-loads and system sizes. The workload is determined by the number of Lync end-users and the system size varies from 1/4 to 4/4 Cisco UCS blade server. The results show a linear scaling in the range of 1/4 to 4/4 blade servers. The processor is found to be the main bottleneck resource in this deployment. Themean opinion score (MOS) aswell as the front end server utilization are the best metrics formonitoring service quality.

ntnudaim:6400

MTDT datateknikk

Komplekse datasystemer

The development of models for computer simulation with detailed application to a CDC 6400 system

Beaumont, William Paul

January 1975

xiii, 270 leaves : ill. ; 26 cm. / Title page, contents and abstract only. The complete thesis in print form is available from the University Library. / Thesis (Ph.D.)--University of Adelaide, Dept. of Computing Science, 1976

Computer simulation.

Control date 6400 computer.

The development of models for computer simulation with detailed application to a CDC 6400 system.

Beaumont, William Paul.

January 1975

Thesis (Ph.D.) -- University of Adelaide, Dept. of Computing Science, 1976.

Analysis of Account Dayfiles for the CDC 6400 Computer Under NOS

Ng, Hok-Nam

09 1900

<p> System performance evaluation is an on-going task for computer system management personnel in order to fine-tune the system operations. One of the evaluation aids that is readily available for the CDC 6400 computers is the job accounting dayfile maintained by the operating system NOS. A set of three programs in FORTRAN has been developed to analyze the dayfile with a view to evaluating the system performance. Program PHASEl prepares the dayfile for analysis. Program PHASE2 creates a job summary file with information on system resources utilization by each job. Program PHASE3 analyzes the job summary file by evaluating various parameters characterizing the system workload and performance at regular time intervals. The results are displayed in tabular and graphical forms. Test results from the analysis of a limited number of dayfiles are discussed. </p> / Thesis / Master of Science (MSc)

CDC 6400

Account Dayfiles

NOS

Computer

Vliv minerálního hnojení na fotosyntetické charakteristiky ostřice štíhlé (Carex acuta) / Effect of mineral fertilization on photosynthetic characteristics of Carex acuta

LESKOVCOVÁ, Martina

January 2009

The MSc. thesis "Effect of mineral fertilization on photosynthetic characteristics of Carex acuta" deals with photosynthetic characteristics of plants subjected to different nutrient regimes. Stands dominated with Carex acuta were studied din two localities: Záblatské louky with organic soil and Hamr with mineral soil. The experimental treament was subjected to high fertilization, while the control treatment received no nutrient addition. The net assimilation was measured using Licor 6400. The aim was to find out whether the net assimilation was higher in fertilized plants as compared with non-fertilized plants. In spring the fertilized plants did not have higher photosynthetic rates at either locality, probably because of water limitation. The positive effect of fertilization was proved only at Hamerské louky after the second cut.

The role of Histone H3 Lysine 4 trimethylation in zebrafish embryonic development

Krause, Maximilian

06 April 2017

Cells within multicellular organisms share the same genetic information, yet their shape and function can differ dramatically. This diversity of form and function is established by differential use of the genetic information. Early embryonic development describes the processes that lead to a fully differentiated embryo starting from a single fertilized cell - the zygote. Interestingly, in metazoan species this early development is governed by maternally provided factors (nutrients, RNA, protein), while the zygotic genome is transcriptionally inactive. Only at a specific developmental stage, the zygotic genome becomes transcriptionally active, and zygotic transcripts drive further embryonic development. This major change is called zygotic genome activation (ZGA). While major regulators of activation of early zygotic genes could be identified recently, the molecular mechanisms that contribute to robust global genome activation during embryonic development is not fully understood. In this study, I investigated whether the establishment of histone H3 lysine 4 trimethylation (H3K4me3) is involved in zebrafish zygotic transcription activation and early embryonic development. H3K4me3 is a chromatin modification that is implicated in transcription regulation. H3K4me3 has been shown to be enriched at Transcription Start Sites (TSS) of genes prior to their activation, and is postulated facilitate transcription activation of developmentally important genes. To interfere with H3K4me3 establishment, I generated histone methyltransferase mutants. I further inhibited H3K4me3 establishment by introduction of histones with lysine 4-to-methionine (K4-to-M) substitution, which act as dominant-negative inhibitors of H3K4me3 establishment. Upon H3K4me3 reduction, I studied the resulting effect on early transcription activation. I found that H3K4me3 is not involved in transcription activation during early zebrafish embryogenesis. Finally I analyzed possible cues in DNA sequence and chromatin environment that might favor early H3K4me3 establishment. These studies show that H3K4me3 is established during ZGA, yet it is not involved in transcription activation during early zebrafish development. Establishment of H3K4me3 might be a consequence of histone methyltransferase recruitment during a permissive chromatin state, and might be targeted to CpG-rich promoter elements that are enriched for the histone variant H2A.z. / Jede Zelle eines multizellulären Organismus enthält dieselbe Erbinformation, und doch können Form und Funktion von Zellen untereinander sehr unterschiedlich sein. Diese Diversität wird durch unterschiedliches Auslesen - Transkribieren - der Erbinformation erreicht. Embryogenese beschreibt den Prozess, der aus einer einzelnen Zelle - der Zygote - einen multizellulären Embryo entstehen lässt. Interessanterweise laufen frühe Stadien der Embryogenese ohne Transkription der embryonalen Erbinformation ab, sondern werden durch maternal bereitgestellte Faktoren ermöglicht. Erst nach einer spezies-spezifischen Entwicklungsphase wird das Erbgut der Zygote aktiv transkribiert und ermöglicht die weitere Embryonalentwicklung. Obwohl bereits wichtige Regulatoren dieser globalen Genomaktivierung identifiziert werden konnten, sind viele molekulare Mechanismen, die zur Aktivierung des zygotischen Genoms beitragen, bisher unbekannt. In der hier vorliegenden Doktorarbeit habe ich die Rolle von Histon H3 Lysin 4 Trimethylierung (H3K4me3) während der frühen Embryogenese des Zebrafischs untersucht. H3K4me3 ist eine Chromatinmodifikation, die mit aktiver Transkription in Verbindung gebracht wird. H3K4me3 ist an Transkriptions-Start-Stellen von aktiv ausgelesenen Genen angereichert und es wird vermutet, dass diese Modifikation das Binden von Transkriptionsfaktoren und der Transkriptionsmaschinerie erleichtert. Während meiner Arbeit habe ich durch Mutation verschiedener Histon-Methyltransferasen beziehungsweise die Überexpression eines dominant-negativen Histonsubstrats versucht, die Etablierung von H3K4me3 in frühen Entwicklungsstadien des Zebrafischs zu verhindern. Anschliessend habe untersucht, welchen Effekt H3K4me3-Reduktion auf Tranksriptionsaktivität entsprechender Gene hat. Allerdings konnte ich keinen Zusammenhang zwischen H3K4me3-Reduktion und Transkriptionsaktivität beobachten. Um herauszufinden, weshalb H3K4me3 dennoch während früher Embryonalstadien etabliert wird, habe ich nachfolgend untersucht, ob möglicherweise bestimmte DNASequenzen oder Chromatin-Modifikationen zur Etablierung von H3K4me3 wahrend der Embryogenese des Zebrafischs beitragen. Aus der hier vorliegenden Arbeit lässt sich schlussfolgern, dass H3K4me3 in Tranksriptionsaktivierung während früher Embryonalstadien des Zebrafischs nicht involviert ist. Möglicherweise wird H3K4me3 in diesen Stadien in einer permissiven Chromatinumgebung etabliert, bevorzugt an Promotoren mit starker H2A.z-Anreicherung und CpG-reichen DNA-Elementen.

Embryonalentwicklung

Chromatin

H3K4me3

Transkriptions-Aktivierung

embryonic development

H3K4me3

transcription activation

chromatin

ddc:570

rvk:WX 6400

Diabetes in Primary Care: Prospective Associations between Depression, Nonadherence and Glycemic Control

Dirmaier, Jörg, Watzke, Birgit, Koch, Uwe, Schulz, Holger, Lehnert, Hendrik, Pieper, Lars, Wittchen, Hans-Ulrich

29 November 2012

Background: Findings are inconsistent regarding the degree to which depression may exert a negative impact on glycemic control in patients with type 2 diabetes. We therefore aimed to examine the longitudinal relationship between depression, behavioral factors, and glycemic control. Methods: In a prospective component of a nationally representative sample, 866 patients with type 2 diabetes aged ≧18 years completed a standardized assessment including a laboratory screening, questionnaires, and diagnostic measures. Subsequent to baseline (t0), patients were tracked over a period of 12 months (t1). Depression was assessed according to DSM-IV and ICD-10 criteria. Glycemic control was determined by levels of glycosylated hemoglobin (HbA1c); a level of ≧7% was judged as unsatisfactory. Regression analyses were performed to analyze the prospective relationship between depression, medication adherence, diabetes-related health behavior, and HbA1c. Results: Patients with depression at t0 revealed increased rates of medication nonadherence (adjusted OR: 2.67; CI: 1.38–5.15) at t1. Depression (adjusted regression coefficient: β = 0.96; p = 0.001) and subthreshold depression (β = 1.01; p < 0.001) at t0 also predicted increased problems with diabetes-related health behavior at t1. Adjusted ORs for poor glycemic control (HbA1c ≧7%) at t1 were also increased for patients with baseline depression (2.01; CI: 1.10–3.69). However, problems with medication adherence as well as problems with diabetes-related health behavior at t0 did not predict poor glycemic control at t1. Conclusions: In a prospective representative study of patients with type 2 diabetes, baseline depression predicted problems with medication adherence, problems with health-related behaviors, and unsatisfactory glycemic control at follow-up.

Diabetes

Blutzuckerspiegel

Nichtbeachtung

Glykämische Index

Blutzuckermessung

diabetes

nonadherence

glycemic control

ddc:616

rvk:YC 6400

rvk:CU 3200

Omalizumab versus ‘Usual Care’: Results from a Naturalistic Longitudinal Study in Routine Care

Wittchen, Hans-Ulrich, Mühlig, Stephan, Klotsche, Jens, Kardos, P., Ritz, T., Riedel, Oliver

10 July 2013

Background: It is unclear how far the superior efficacy of omalizumab, established in randomized controlled clinical trials of patients with severe allergic asthma (SAA), translates into routine practice and when compared to matched controls. Methods: New-onset omalizumab-treated (OT) patients with SAA (n = 53) were compared to a matched control group of usual-care (UC) patients (n = 53). Treatment and procedures were naturalistic. Subsequent to a baseline assessment, patients were followed up over at least 6 months with at least two follow-up assessments. Primary clinical outcomes were the number of asthma attacks, persistence of asthma symptoms and degree of control [asthma control test (ACT), Global Initiative for Asthma]. Secondary outcome criteria were quality of life (Euro-Qol 5D) and number of medications. For each outcome we compared within-group effects from baseline to 6-month follow-up as well as between-group effects. Results: OT patients showed significant improvements in number [effect size (ES) = 0.03] and frequency (ES = 0.04) of asthma attacks as well as asthma control (ES = 0.09), whereas controls revealed no significant improvements in these measures. Further improvements in the OT group were found for ‘perceived control always’ (ACT, p = 0.006), no impairment (ACT, p = 0.02), reduction of sickness days (p = 0.002) and number of medications needed (p = 0.001). Conclusions: Substantial beneficial effects of omalizumab, similar to those observed in controlled trials and after marketing studies, were confirmed, particularly with regard to the reduction of asthma attacks, persistence of symptoms, asthma control and reduction of concomitant asthma medications. This study provides a tougher test and generalizable evidence for the effectiveness of omalizumab in routine care.

Omalizumab

allergisches Asthma

Atemwegserkrankungen

Allergic asthma

Omalizumab

Pulmonary diseases

ddc:616.238

rvk:YB 6400

Identification of proteins controlling gastrulation movements by a proteomic approach in zebrafish

Link, Vinzenz

20 March 2006

During vertebrate gastrulation, a well-orchestrated series of cell movements leads to the formation of the three germ layers: ectoderm, mesoderm and endoderm. In zebrafish, a model organism for vertebrate development, the mesendodermal progenitor cells separate from the ectodermal cells and migrate towards the animal pole. To identify proteins controlling these processes, I used a comparative proteomic approach following two alternative strategies: (1) Based on the notion that Wnt11 regulates cell movement and morphology during gastrulation independent of transcriptional regulation, I performed a screen aimed at the identification of proteins phosphorylated upon Wnt11 signalling. To regulate Wnt11 expression tightly, I engineered a transgenic slb/wnt11-/- fish line expressing wnt11 under the control of a heat shock promoter. Using this line, I performed a quantitative comparison of protein phosphorylation with or without Wnt11 pathway activation by analysing 32P-labelled embryo extracts on 2D gels. (2) Since these experiments did not reveal any Wnt11 targets, I addressed, in the second approach, proteomic differences causal for the changes in cell adhesion and motility observed in mesendodermal cells upon involution. Quantitative 2D gel analysis comparing ectodermal and mesendodermal cells revealed 37 significantly regulated spots, 36 of which I identified by mass spectrometry. Interestingly, the majority of these proteins were not regulated on a transcriptional level as determined by an accompanying microarray analysis confirming the complementary nature of proteomics and transcriptomics. Among the identified targets, several proteins, including Ezrin2, had previously been assigned a cytoskeleton-related function. I characterised Ezrin2 in more detail showing that Ezrin2 is specifically activated by phosphorylation in mesendodermal cells and that it is required for proper gastrulation movements. In the course of this study, I developed techniques for proteomic analysis of early zebrafish embryos, including a protocol to remove the yolk. I identified several cytoskeleton-related proteins in a comparative proteomic screen for regulators of gastrulation movements. The subsequent characterisation of Ezrin2 confirmed the power of proteomics for the analysis of developmental processes. In conclusion, this work provides a foundation to study developmental and cell biological questions in early zebrafish embryos using proteomics.

Gastrulation

Zebrafish

ezrin

gastrulation

proteomics

zebrafish

ddc:570

rvk:WX 6400

rvk:WC 4150

Gastrulation

Proteomanalyse

Zebrabärbling