ENTERPRISE RESOURCE PLANNING SYSTEMS, BUSINESS PERFORMANCE AND USERS COMPLAINTS

Restemis, Andreas, Okpor, Lovelyn

January 2013

Introduction: Enterprise recourse planning (ERP) is a system that combines software, hardwareand people to manage information The aim of this study is to investigate ERP systems effect onbusiness performance (advertised vs. realized benefits) and user’s complaints. It also aims toidentify the most important issue a company faces after implementing an ERP system and if thisstops potential benefits from happening. This will be viewed from a user’s perspective. Approach/Methodology: This research includes qualitative and quantitative primary data withsecondary data to answer the research questions posed. It is based on a number of semistructuredinterviews of people well versed in ERP systems presented in case study form.Alongside, it also utilizes a series of questionnaires presented in tabular form. The data wasanalyzed and linked with theory to provide answers and test assumptions. Findings: ERP systems provide their advertised benefits to a large extent. The most importantorganizational issue after implementing an ERP system is resistance to change and this issueaffects the benefits realization of the system. Finally, user’s complaints about ERP systems arevaried and include the speed of the system, support in error situations and general complexity. Conclusions: Even though it provides many benefits in business performance, an ERP system,selection and implementation in a company is a critical step. The whole process is complicated,resource consuming, takes a long time and can encounter problems. Mistakes in theimplementation cost a company more resources to fix after they happen. In this case preventionis better than cure and the best medicine.Implications and Value of research: ERP system implementation and use should bemethodically planned from the beginning to get maximum benefits realization. This is especiallyimportant in effectively managing change in an organization. In this issue, top level managersshould be aware and committed to. Suggestion for future studies: A possible research that could correlate user complaintcategories already established with age group of respondents under a global perspective.

ERP

user perspective

advertised versus realized benefits

user complaints

Optimize the generation and depletion of alloreactive T cells for cellular therapy

Shao, Mei.

January 2005

Thesis (Ph. D.)--Ohio State University, 2005. / Available online via OhioLINK's ETD Center; full text release delayed at author's request until 2006 Dec 22

Chronic graft-versus-host disease, autoimmunity and microvascular pathology an experimental approach to scleroderma /

Bos, Gerardus Marinus Josef.

January 1989

Proefschrift Maastricht. / Met lit. opg. - Met samenvatting in het Nederlands.

Naše/moje cesta k BodyVoiceBandu / Our/my journey to BodyVoiceBand

Holubová, Iva

January 2015

The subject of this thesis is the analysis of studies of the graduates of drama2013/2014 at the Theatre Faculty of the Academy of Performing Arts in Pragueunder the guidance of teachers MgA. Jaroslava Šiktancová Ph.D., MgA. LukášHlavica and doc. Marie Málková. I am describing the methods of our dramatictraining, which formed the basis for further joint work leading to the creation ofthe company BodyVoiceBand. My thesis describes the process chronologicallyfrom the very beginning of the study to the birth of the performance Vojna (TheWar), which we already prepared under the heading of BodyVoiceBand.I divided the thesis into three parts. In the first one I deal with the workshops ofFarma v jeskyni (Farm in a Cave), which were decisive for all our future work, forboth the ensemble, and the individuals. I described what kind of training wewent through during the workshops and the way it prepared us for furtherstudies. The second part deals with the study at the faculty. It is divided intosubheads according to the phenomena we were dealing with and which are thestarting point for a certain kind of work, thanks to which the bodyBodyVloiceBand started to shape. The third part is devoted to the production ofVojna /War, which is the result of our efforts, and which is the starting point ofthe formation of BodyVoiceBand. I focused on the way and course of preparingthe production.

Comparison of Poractant Versus Beractant in the Treatment of Respiratory Distress Syndrome in Premature Neonates in a Tertiary Academic Medical Center

Jorgensen, Ashley, Phan, Hanna

January 2012

Class of 2012 Abstract / Specific Aims: The objective of this study is to evaluate and compare clinical outcomes and economic impact involved with the use of beractant (B) compared to poractant (P) for the treatment of respiratory distress syndrome (RDS) in premature neonates admitted to a neonatal intensive care unit. Methods: Patients were included if they were less than 35 weeks gestational age at birth, survived at least 48 hours, and admitted to the neonatal intensive care unit and treated with P or B for RDS. The primary outcome of this study is the change in the fraction of inspired oxygen (FiO2) over the first 48 hours after surfactant administration. Secondary outcomes were the change in oxygen saturation, time spent on mechanical ventilation and continuous positive airway pressure (CPAP), complication occurrence and mortality of the neonates. Main Results: There were a total of 40 neonates whose charts were reviewed (n= 13 and n=27 in the P and B groups respectively). The mean gestational age of the neonates were 29.2+/-2.9 and 28.8+/-2.9 weeks in the P and B groups respectively. The FiO2 was found to not be lower between the P and B groups (35.5+/-22.2 and 42.4+/-24.2, respectively; p=0.379), as well as the O2 saturation (94.6+/-4.6 and 92.3+/-6.1; p=0.194). Significance was also not found for the other clinical or economic outcomes assessed in this study. Conclusions: There was not a significant difference between poractant and beractant in FiO2, O2 saturation, or in the other clinical outcomes evaluated in this study.

versus

treatment

respiratory distress syndrome (RDS)

poractant

beractant

neonates

Identification of genes regulated in target organs of acute graft versus host disease in different organs in different species

Shah, Pranali Nitin

19 August 2016

No description available.

610

Graft-versus-host-disease

Gene expression

Medizin (PPN619874732)

Evaluating Treatment Options for NAP1 Versus Non-NAP1 Strains of Clostridium Difficile Infection Among Pediatric Patients at an Academic Hospital.

Smith, Amelia, Matthias, Kathyrn, Phan, Hanna

January 2014

Class of 2014 Abstract / Specific Aims: The incidence of Clostridium difficile (C. Diff) infections in pediatric patients has continually risen, which could be caused by the emergence of a hyper virulent strain, specifically NAP1/B1/027. The objectives of the study were to evaluate the incidence of strain type, compare treatment(s) prescribed, treatment duration, rate of infection recurrence based on strain and severity, rates of re-infection or recurrence, and treatment failures for patients less than 6 months and up to 18 years of age. Methods: A retrospective study of patients admitted to an academic medical center with detection of C. diff toxin was performed. Data analyses included descriptive and inferential statistics to examine demographics, strain type, infection severity, and treatment failure. Main Results: Fourty-five patients with C. Diff toxin detection were included in study analyses and the median age was 6.2 [0.31- 17.9 years]. Oral or intravenous metronidazole was prescribed as initial therapy in 89% of the patients. Strain type was available in 77% of patients, with NAP1/B1/027 detected in 31% of stool samples tested. Within 21 days after initial toxin detection, there was a 13% rate of clinical failure or death, although none directly associated with C. Diff. Within days 22 - 65 after initial toxin detection, there was a 16% rate of recurrence or reinfection. Initial therapy selection, therapy duration, and rate of recurrence or reinfection were not significantly associated with NAP1/B1/027 strain type. Conclusion: Despite variability in severity of infection, the majority of pediatric patients with C. Diff were treated with metronidazole and were infected with a non-B1/NAP1/027 strain.

treatment

NAP1 versus

non-NAP1

Clostridium difficile (C. Diff)

pediatric

An analysis of the perceptions on corruption – residents of Brooklyn in cape town

Gonya, Prince Zukile

January 2020

Masters in Public Administration - MPA / The subject matter of corruption is a topical one in South Africa, where many institutions in the socio-political economy, both private and public, are subject to corruption allegations which emerge from time to time in the media. A number of studies have been undertaken on this topic globally, mainly in Latin America, but there remains a dearth of published academic work on the phenomenon in South Africa. Inevitably what transpires in the socio-political economy has a bearing on the lives of the general public. Of interest in this study is public perceptions of corrupt practices in the country and how these affect ordinary people. The objective of this study is to explore how people perceive corruption in the City of Cape Town, using the residents of Brooklyn as a case study.

Public perception

Perception versus reality

Corruption

Forms of corruption

Social class

Induktion von GvHD-artigen Gewebeschäden an humanen artifiziellen Hautmodellen / Induction of GvHD-like tissue damage in human artificial skin models

Wallstabe, Julia

January 2020

Graft-versus-Host Disease (GvHD) stellt einen häufigen, den Gesamterfolg einer allogenen hämatopoetischen Stammzelltransplantation limitierenden Faktor dar. Bei dieser Komplikation attackieren vor allem alloreaktive T-Lymphozyten des Stammzellspenders gesunde Körperzellen des Patienten. Infolgedessen kommt es zu Gewebeschäden in den Zielorganen Haut, Leber und Darm. Die Behandlung der GvHD erfordert eine effektive Immunsuppression, was wiederum Graft-versusTumor-Effekte kompromittiert und den Rückfall der malignen Grunderkrankung bedingen kann. Viele Patienten sprechen aus bisher ungeklärten Gründen nicht auf die klassische immunsuppressive Therapie mit Steroiden oder second-line Therapien an. Neue zelluläre Therapien zur Behandlung der refraktären GvHD sind auf dem Vormarsch, bedürfen aber einer weiterführenden klinischen Testung, auch um die exakten Wirkungsmechanismen zu verstehen. Idealerweise könnten neue Testsysteme das GvHD-Potential von allogenen Stammzellpräparaten oder aber das immunsuppressive Potential von neuen GvHD-Therapien vorhersagen, bevor diese in klinischen Studien eingesetzt werden. Ziel der vorliegenden Arbeit war es, ein erstes, in multiplen Replikaten einsetzbares, humanes organotypisches Gewebemodell zur Simulation einer GvHD-Reaktion am Beispiel der Haut zu etablieren. Zu diesem Zweck wurden artifizielle humane Hautmodelle unter statischen (KollagenHautmodelle) und dynamischen Kulturbedingungen (vaskularisierte Hautmodelle) generiert. Die Injektion unstimulierter PBMCs (engl. peripheral blood mononuclear cells) führte zu keinen histomorphologischen Veränderungen in den KollagenHautmodellen. Im Gegensatz dazu hatte die Injektion vorstimulierter allogener PBMCs eine Zerstörung der epidermalen Strukturen der Kollagen-Hautmodelle zur Folge, welche vergleichbar waren mit Gewebeschäden bei einer akuten GvHD der Haut. Dieselben Schädigungen der Epidermis wurden durch die Injektion von Mediumüberständen vorstimulierter PBMCs in die Kollagen-Hautmodelle erreicht. Im Kulturmedium der Kollagen-Hautmodelle wurden hohe Konzentrationen von Interleukin 2 und 17, Interferon gamma sowie Tumornekrosefaktor alpha gemessen, wodurch auf die Beteiligung von Zytokinen an der inflammatorischen Reaktion geschlossen werden konnte. Auch im komplexeren vaskularisierten Hautmodell verursachte die Injektion vorstimulierter PBMCs histomorphologische Veränderungen entsprechend einer akuten Haut-GvHD sowie einen zeitabhängigen Anstieg proinflammatorischer Zytokine. Zusammenfassend zeigen die Resultate dieser Arbeit, dass die Induktion einer starken Inflammations- und Immunreaktion in artifiziellen humanen Hautmodellen, welche histomorphologisch eine GvHD imitiert, möglich ist. Dieses Modell könnte als Grundlage für die Entwicklung eines klinisch relevanten Testsystems zur Bestimmung des GvHD-Restpotentials oder zur Festlegung der immunsuppressiven Kapazität innovativer Zellpräparate dienen. Somit könnten humane artifizielle GvHDModelle in klinischen Studien eingesetzt werden und die Erfahrungen aus Tiermodellen ergänzen sowie erste in vitro Ergebnisse im humanen System liefern, welche dann mit dem tatsächlichen klinischen Resultat verglichen werden könnten. / Graft-versus-Host Disease (GvHD) remains the most important limiting factor for the success of allogeneic hematopoietic stem cell transplantation. This major complication is caused by alloreactive donor T-lymphocytes that attack healthy tissues of the recipient leading to severe tissue damage within the target organs skin, liver and gut. Treatment of GvHD requires effective immunosuppression, which in turn impairs Graft-versus-Tumor activity and enhances the risk for relapse of the malignant disease. However, for still unknown reasons many patients do not respond to standard immunosuppressive therapy with steroids or to second-line therapies. Development of novel cellular therapies that gain more and more clinical relevance due to their high anti-tumor potency lead to a strong demand for advanced test platforms to further investigate their underlying functional mechanisms and exclude off-tumor effects against healthy tissues. Ideally, new test systems could be used for the prediction of the GvHD potential of allogeneic stem cell products or for prediction of an immunosuppressive potential of novel GvHD therapies before entering clinical studies. The aim of this study was to establish a GvHD test system based on human organotypic skin models allowing the simulation of GvHD reactions in the skin in multiple replicates. To this end, artificial human skin models were generated under static (collagen skin model) and dynamic culture conditions (vascularized skin model). Injection of unstimulated peripheral blood mononuclear cells (PBMCs) did not cause histomorphological changes in collagen skin models. In contrast, injection of prestimulated PBMCs resulted in disruption of the epidermis of collagen skin models mimicking acute skin GvHD. The same disruption of the epidermal layer was observed using cell culture supernatants of prestimulated PBMCs, suggesting the involvement of proinflammatory cytokines. Indeed, measurement of cytokine levels in culture supernatants revealed an increase of interleukin 2 and 17, interferon gamma and tumor necrosis factor alpha. In addition, injection of prestimulated PBMCs into more complex vascularized skin models also caused disruption of the epidermal layer and an increase of proinflammatory cytokine levels in a time dependent manner. Taken together, these findings demonstrate that it is possible to induce a strong immune reaction and inflammatory tissue damage in artificial human skin models mimicking histomorphological patterns of acute skin GvHD. Therefore, this model could contribute to the development of a clinically relevant GvHD test platform for prediction of the GvHD potential or immunosuppressive capacity of innovative cell products. Thus, artificial human GvHD models may be employed in clinical studies in order to gain first in vitro results in a human system and to extend information from animal models, which can then be compared to the actual clinical outcome.

Graft-versus-host-disease

Tissue Engineering

ddc:570

Migration of allogenic T cells in intestinal lymphoid structures during acute Graft-versus-Host Disease / Migration allogener T-Zellen in intestinalen lymphoiden Strukturen während der akuten Graft-versus-Host Reaktion

Jarick [née Ottmüller], Katja Julika

January 2020

T cell infiltration into the intestine occurs after priming and activation in the mesenteric lymph nodes and Peyer’s patches and subsequent trafficking via the blood circulation. We hypothesized that additionally to the vascular trafficking route, a fraction of T cells in the Peyer’s patches directly migrate into the adjacent lamina propria of the small intestine. To test this hypothesis, we employed a mouse model of acute Graft-versus-Host Disease to study the direct T cell migration from the Peyer’s patches to the adjacent lamina propria. First, we analyzed the border of Peyer’s patches on histological sections and found that the Peyer’s patch is not enclosed by a capsule or basement membrane. Thus, the tissue architecture allows for direct access to the surrounding tissue. With whole-mount light sheet fluorescence microscopy we quantified a three-dimensional gradient of T cells around Peyer’s patches on day 2.5 and day 3 after transplantation. This gradient evened out at day 4 and day 6 when high numbers of T cells started to evenly infiltrate the intestine from the blood circulation. We confirmed that gradient-forming T cells around Peyer’s patches resided within the tissue parenchyma of the lamina propria and not inside lymphatic vessels. To positively prove that the recently activated donor T cells around Peyer’s patches have egressed directly from that patch, we established a protocol for intravital photoconversion of T cells inside Peyer’s patches. 12 h after photoconversion inside a single Peyer’s patch, photoconverted T cells resided only around this particular Peyer’s patch and not elsewhere in the small intestine. This indicated that the T cells did not infiltrate via the blood but migrated to the adjacent lamina propria of the small intestine. Dynamic intravital two-photon microscopy revealed that these T cells next to the Peyer’s patch migrated in a random pattern. This suggested that these cells did not follow a positive chemoattractive gradient once they had reached the lamina propria. Laser-capture microdissection combined with RNA sequencing of the mucosa near the Peyer’s patch identified a wide range of migration-promoting factors. These included chemokines, co-stimulatory receptors and migration-associated intracellular molecules, which are candidates to promote this direct migration from Peyer’s patches. Altogether, we demonstrate for the first time that additionally to the vascular trafficking route, a fraction of T cells migrates directly from the Peyer’s patch to the surrounding mucosa. This mechanism implies so far unrecognized regional specification of Peyer’s-patch-primed T cells. Our findings may impact treatment strategies to avoid intestinal inflammation or foster immunity after oral vaccination. / T-Zell Infiltration in den Darm erfolgt nach Primen und Aktivierung in den mesenterialen Lymphknoten und Peyerschen Plaques durch Rezirkulation über die Blutbahn. Wir stellten die Hypothese auf, dass zusätzlich zur vaskulären Route ein Teil der T-Zellen im Peyerschen Plaque direkt in die angrenzende Lamina propria des Dünndarms wandert. Um diese Hypothese zu testen, setzten wir ein Mausmodell für eine akute Graft-versus-Host Reaktion ein, um die direkte Migration von T Zellen aus den Peyerschen Plaques in die angrenzende Lamina propria zu untersuchen. Zuerst analysierten wir die Randzonen um die Peyerschen Plaques mit histologischen Schnitten und konnten bestätigen, dass der Peyersche Plaque von keiner Kapsel oder Basalmembran umschlossen ist, sodass die Gewebearchitektur den direkten Zugang des umliegenden Gewebes zulässt. Mithilfe der Lichtblatt-Fluoreszenzmikroskopie von Dünndarm-Komplettpräparaten quantifizierten wir einen dreidimensionalen T-Zell Gradienten um Peyersche Plaques an den Tagen 2,5 und 3 nach allogener Stammzelltransplantation. Dieser Gradient verschwand zwischen an Tag 4 und Tag 6, als eine hohe Anzahl an T-Zellen begann, den Darm gleichmäßig über die Blutbahn zu infiltrieren. Wir bestätigten, dass die Gradienten-bildenden T-Zellen im Gewebe der Lamina propria und nicht in lymphatischen Gefäßen saßen, um zirkulierende Zellen von der Gradientenbildung auszuschließen. Um direkt zu beweisen, dass die T-Zellen um dem Peyerschen Plaque unmittelbar aus diesem Plaque ausgewandert sind, haben wir ein Protokoll für intravitale Photokonversion von T-Zellen im Peyerschen Plaque etabliert. 12 h nach der Photokonversion in einem einzelnen Peyerschen Plaque befanden sich die T-Zellen nur um diesen bestimmten Plaque herum. Dies zeigt, dass die T-Zellen das Gewebe nicht über die Blutbahn infiltrierten, sondern direkt in die angrenzende Lamina propria des Dünndarms gewandert waren. Dynamische intravitale Zweiphotonenmikrokopie offenbarte, dass diese T-Zellen um den Peyerschen Plaque nach zufälligem Schema wanderten. Dies legte nahe, dass diese T-Zellen keinem positiven Chemokingradienten folgten, sobald sie die Lamina propria erreicht hatten. Laser-Mikrodissektion kombiniert mit RNA-Sequenzierung der Mukosa nahe des Peyerschen Plaques identifizierte eine große Auswahl an migrationsfördernden Faktoren. Hierunter waren Chemokine, kostimulatorische Rezeptoren und intrazelluläre migrationsassoziierte Moleküle, welche Kandidaten sind, diese direkte Migration aus den Peyerschen Plaques zu fördern. In dieser Arbeit zeigen wir erstmalig, dass zusätzlich zur vaskulären Route ein Teil der T Zellen direkt vom Peyerschen Plaque in die umliegende Mukosa wandert. Dieser Mechanismus impliziert bislang unerkannte regionale Spezialisierung von T Zellen, welche in Peyerschen Plaques aktiviert wurden. Diese neuen Befunde können zukünftige Behandlungsstrategien gegen intestinale Entzündungserkrankungen oder für Immunreaktionen nach oraler Impfung beeinflussen.

T-Lymphozyt

Graft-versus-host-disease

Darm

Zellmigration

ddc:570