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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.
71

Disorderly and Inhumane: the United States and the Expulsion of Germans after World War II

Brewer, Bradley J 09 May 2015 (has links)
This dissertation examines the role of the United States in the mass expulsion of Germans from East-Central Europe from spring 1945 through 1947. By agreeing to allow Czechoslovakia and Poland to expel their German minority populations in 1943, and again in 1945 under Article XIII of the Potsdam Agreement, the United States permitted approximately 14 million to 16 million Germans to be forcibly relocated into a truncated, war-torn Germany, an incident that is the largest example of ethnic cleansing in world history. Although these expulsions threatened the postwar stability of Europe and were of great concern they were of marginal interest to most people in the United States. Informed discussion of these expulsions occurred among a fairly narrow group of military officials, diplomats, politicians, intellectuals, and immigrants or exiles. In fact there was a dearth of contemporary debate and analysis on all aspects of the United States role in the expulsion of Germans, both within government and in society more generally. Newspaper reports, magazine articles, diplomatic documents, government documents and the personal papers of diplomats and politicians reveal that the expulsion of Germans was a secondary issue to the United States government. Despite considerable media coverage, it seems that most Americans lacked both awareness of and compassion for the plight of the German expellees. These expulsions however, changed the politics and the demographics of Europe forever and made the ethnic cleansing of the minority populations of nations an international legal precedent. Today, the expulsions remain a controversial subject within the region of East-Central Europe where the people of Czechoslovakia, Germany and Poland still debate the expulsions as if they occurred yesterday. In the United States, however, the expulsions have been long forgotten. This dissertation is unique in that examines the involvement of the United States in the planning of the expulsions and the reaction of the American press, intellectuals and policymakers whereas previous literature has focused very sparingly on this aspect of the expulsions.
72

Einfluss des Transkriptionsfaktors B-cell lymphoma 6 (BCL6) auf die Expression renaler Transportproteine / The effect of the transcription factor B-cell lymphoma 6 (BCL6) on the expression of renal transport proteins

Millé, Aline Noel 07 November 2016 (has links)
No description available.
73

Investigations of in vitro test systems for the detection of Glucocorticoid-induced skin atrophy as a tool in drug discovery

Schoepe, Stefanie 12 August 2009 (has links)
Topische Glukokortikoide (GCs) sind wirksam bei Therapie von entzündlichen Hauterkrankungen. Durch ihr Nebenwirkungspotential (z.B. Induktion von Hautatrophie) ist ihr Einsatz jedoch begrenzt. Für die Medikamentenentwicklung ist die Bestimmung des atrophogenen Potenzials neuer Verbindungen daher von großer Bedeutung. Derzeit stehen dafür keine prädiktiven in vitro Modelle zur Verfügung. Ziel dieser Arbeit war daher die Etablierung solcher Modelle. Es wurden kutane Zelltypen (3T3-Zellen, Rattenfibroblasten, HaCaT-Zellen, humane Keratinozyten [NHEK] und Fibroblasten) und Vollhautmodelle (CellSystems AST-2000 und Phenions FTSM) untersucht. Atrophie-Marker, die Proliferation, Kollagen-Metabolismus und Epidermisdicke betreffend, wurden auf mRNA-, Protein- bzw. zellulärer Ebene gemessen. Außerdem wurden mittels Genexpressionsanalysen von GC-behandelter Nagerhaut neue potenzielle Marker identifiziert, deren Regulation in vitro jedoch nicht bestätigt werden konnte. Nach Pilotexperimenten wurden 3 Modelle ausgewählt und für Evaluierungsexperimente mit Referenz-GCs behandelt: 1). MMP1, -2, -3 und -9 mRNA-Expression in NHEK, 2). COL1A1 und COL3A1 mRNA-Expression in 3T3-Zellen, 3.) Epidermisdicke, Kollagen- und MMP-Synthese in FTSM. Die Messparameter der 3 Modelle erwiesen sich als dosisabhängig reguliert und korrelierten mit dem atrophogenen Potenzial der GCs. Schließlich wurde die Prädiktabilität der 3 in vitro Modelle für die in vivo Situation im Nager analysiert. In allen 3 in vitro Systemen induzierte die Behandlung mit einem selektiven GC-Rezeptor-Agonisten weniger atrophogene Effekte als das Referenz-GC. Ähnliche Ergebnisse wurden auch in vivo im Rattenhautatrophie-Modell gefunden. Zusammenfassend wird eine Kaskade von 3 in vitro Modellen empfohlen, um das atrophogene Potential von GC-Rezeptor-Liganden zu bestimmen. Der tatsächliche prädiktive Wert für die klinische Situation sollte in weiteren Studien untersucht werden. / Topical glucocorticoids (GCs) are effective for the therapy of inflammatory skin diseases. However, their use is limited by their side effect potential, with skin atrophy being the most prominent one. Thus, determining the atrophogenic potential of novel compounds is of importance for drug development. Currently, there are no according predictive in vitro models available. The aim of this study was to establish such atrophy models. Rodent and human cutaneous cell types (3T3 cells, rat fibroblasts, HaCaT cells, human keratinocytes [NHEK] and fibroblasts) and human full-thickness skin equivalents (CellSystems AST-2000 and Phenions FTSM) were investigated. Atrophy markers related to proliferation, collagen metabolism and epidermal thickness were measured on mRNA, protein and cellular level, respectively. Additionally, by gene expression profiling of GC-treated rodent skin novel potential markers were identified, but subsequently not confirmed in vitro. After pilot studies 3 models were selected and treated with reference GCs for evaluation experiments: 1.) MMP1, -2, -3 and -9 mRNA expression in NHEK, 2.) COL1A1 and COL3A1 mRNA expression in 3T3 cells, 3.) epidermal thickness, collagen and MMP synthesis in FTSM. The read out parameters of all 3 test systems turned out to be regulated dose-dependently and correlated with the atrophogenic potential of the GCs. Finally, the predictability of the 3 recommended in vitro test system for the rodent in vivo situation was analyzed. In all 3 in vitro test systems, the treatment with a novel selective GC receptor agonist induced less atrophogenic effects than the reference GC clobetasol. Indeed, similar results were found in the hr/hr rat skin atrophy model. In summary, a cascade of 3 in vitro models is recommended to be applied for the characterization of the atrophogenicity of GC receptor ligands. Further experiments are necessary to eventually demonstrate the true predictability of these models for the clinical situation.
74

Differentielle Expression von HLA-DRB-Genen

Heldt, Christian 31 July 2002 (has links)
In den humanen Leukozyten-Antigenen (HLA) wird die wichtigste genetische Ursache von rheumatoider Arthritis gesehen. Es wurden bisher mehrere Mechanismen beschrieben, wie diese HLA-Moleküle die Entstehung und den Verlauf der Erkrankung beeinflussen. Im Rahmen dieser Arbeit wurde die differentielle Expression von HLA-DRB-Genen in unterschiedlichen Antigen-präsentierenden Zellen als möglicher Mechanismus untersucht. Dabei wurden strukturelle Unterschiede zwischen den Promotoren des krankheitsassoziierten HLA-DR4-Haplotyps und den neutralen Haplotypen DR7 und DR9 eingehender betrachtet. Allen drei Haplotypen ist gemein, daß sie das DRB4-Gen als zweites funktionelles DRB-Gen tragen, wobei das DRB4-Gen entweder den DRB4A oder den -B-Promotor besitzt. Um den Einfluß einzelner Promotorelemente auf die mit dem Luziferase-Assay bestimmten Transkriptionsaktivitäten näher zu untersuchen, wurde mit Hilfe der surface plasmon resonance die Bindung der Transkriptionsfaktoren aus den Zellkernlysaten von der humanen Monozytenzellinie THP-1 und von der humanen B-Lymphom-Zellinie BJAB an die unterschiedlichen S-, X-, Y-, CCAAT- und TATA-Boxen analysiert. Es konnte gezeigt werden, daß die unterschiedliche Expression von DRB4A und DRB4B durch die ubiquitäre TATA-Box vermittelt wird. Dagegen wurde die INF-gamma-Stimulation der HLA-DR-Expression von THP-1- aber auch von BJAB-Zellen durch die für die HLA-DR-Promotoren spezifische X-Box vermittelt. Bei der Analyse von DR4-, DR7- und DR9-positiven Patienten einer bereits gut charakterisierten RA-Kohorte stellte sich heraus, daß der DRB4B-Promotor, welcher im Vergleich zu DRB4A eine höhere transkriptionelle Aktivität besitzt, mit einem schweren Krankheitsverlauf assoziiert ist, so daß eine erhöhte HLA-DR-Expression den Krankheitsverlauf negativ zu beeinflussen scheint. / Disease associated human leukocyte antigen (HLA) genes have been identified in humans where they are assumed to promote the susceptibility and/or progression of rheumatoid arthritis. Several mechanisms have been described how these HLA haplotypes impact on the disease. Among them the differential expression of HLA-DRB molecules in different types of antigen-presenting cells, which was investigated here in detail. The promoters of the disease associated HLA-DR4 to the neutral DR7 and DR9 haplotypes were analyzed for sequence polymorphisms resulting in functional differences. All three haplotypes carry as a second functional DRB gene the DRB4 gene, which is regulated by the DRB4A or -B promoter. To determine the impact of the promoter elements on the transcriptional activities measured by luciferase assay the surface plasmon resonance technology was employed. To this end, nuclear extracts from the monocytic cell line THP-1 and from the B lymphoma cell line BJAB were used to analyze their binding to the various S-, X-, Y-, CCAAT-, and TATA boxes. It could be demonstrated that the differential expression of DRB4A and -B was regulated via the ubiquitous TATA box. By contrast, the INF-gamma stimulation of HLA expression in THP-1 and BJAB was mediated via the unique X box. Analyzing the DR4, DR7 and DR9 positive patients of an RA cohort, the DRB4B promoter, which has a higher transcriptional activity than the DRB4A promoter, is associated with radiographic progression of RA. This data is thus indicative of an impact of elevated HLA-DR expression on the progression of the disease.
75

Auswirkungen der Bestrahlung mit UVB, UVA-1 und PUVA-1 auf das Funktionsverhalten humaner dermaler Mastzellen nach Stimulation mit anti-IgE und Substanz P

Strathmann, Marc 16 September 2004 (has links)
Die in dieser Arbeit isolierten und hochaufgereinigten, humanen dermalen Mastzellen wurden mit UVB, UVA-1 und PUVA-1 bestrahlt und anschließend entweder mit Substanz P oder anti-IgE stimuliert. Dadurch sollten Einblicke in die unterschiedlichen Wirkmechanismen der bei zahlreichen mastzellassoziierten Erkrankungen eingesetzten UV Licht Therapie gewonnen werden. Ein Schwerpunkt dieser Arbeit lag in der Erforschung der Histamin-, Tryptase- und Zytokinfreisetzung von menschlichen Mastzellen. Zusätzlich wurde die Expression von Lysosomen-assoziierten Membran Proteinen (LAMPs) auf der Oberfläche dieser Zellen untersucht. Im Gegensatz zu der durch UV Licht induzierbaren spontanen Histaminfreisetzung zeigte sich die anti-IgE stimulierte Histaminausschüttung durch UVB, UVA-1 und PUVA-1 signifikant und dosisabhängig inhibierbar. Auch die durch Substanz P stimulierten Mastzellen gaben nach UVA-1 Bestrahlung deutlich weniger Histamin ab. Demgegenüber blieb die sezernierte Menge des Mediators nach UVB und PUVA-1 konstant. Analog zu den erhobenen Histaminergebnissen konnte eine signifikante Inhibition der anti-IgE induzierten Tryptasefreisetzung nachgewiesen werden. Ebenso zeigte sich eine signifikante Verringerung, der innerhalb von vierundzwanzig Stunden basal freigesetzten Menge an Interleukin-6 und Interleukin-8, nach UV Bestrahlung. Die spontane Ausschüttung vom Tumornekrosefaktor-a verblieb in dem Untersuchungszeitraum auf sehr geringem Niveau, so dass eine relevante Beeinflussung durch UV Licht nicht stattfand. Des weiteren konnte eine vermehrte basale Expression von CD107a und CD63 auf der Mastzellmembran durch UV Bestrahlung demonstriert werden. Auch die anti-IgE induzierte Mehrexpression der LAMPs konnte bei den drei Bestrahlungsarten nachweisbar supprimiert werden. Die in dieser Arbeit gewonnenen Erkenntnisse zeigen, dass die Auswirkungen der UV Licht Therapie auf Mastzellen sehr komplex sind. Zu beachten ist, dass unter physiologischen Bedingungen nicht nur isolierte Mastzellen, sondern auch weitere bestrahlte Zellverbände eine Veränderung erfahren. Erst durch das Zusammenspiel aller Zellen lassen sich Rückschlüsse auf Krankheitsbilder und die anzuwendende Therapien ziehen. Letztendlich soll diese Arbeit dazu beitragen, dass das Verständnis der unterschiedlichen Wirkungen von UV Licht begriffen und so ein sinnvolles und gezieltes Einsetzen im klinischen Alltag ermöglicht wird. / For all experiments highly purified dermal mast cells were used. The aim of the current study was to systematically investigate the effects of UVB, UVA-1 and PUVA-1 on skin derived human mast cells. Baseline and stimulated release of histamine, tryptase and of the proinflammatory cytokines IL-6, IL-8 and TNF-a were examined. Furthermore, the CD 107a and CD 63 surface levels in UV treated cells were investigated representing two members of lysosome associated membrane proteins which were found to appear on mast cell surface during degranulation. Prior treatment with UV resulted in a striking suppression of the anti-IgE induced release of preformed mediators such as histamine and tryptase in a dose dependent manner. This inhibition was accompanied by a diminished, anti-IgE mediated increase in CD 107a and CD 63 surface expression. In sharp contrast, UV-light slightly preactivates mast cells as indicated by a marginal but statistically significant direct UV-caused histamine release. Theses findings matched the observation of slightly enhanced CD 107a and CD 63 surface levels in UV treated but unstimulated cells. After UVA-1 treatment the histamine release of substance P stimulated mast cells is statistically significant reduced which contrasts to the unchanged liberation of this preformed marker after UVB and PUVA-1 irradiation. Furthermore the release of mediators that are not or only partially preformed was examined. In the present study all types of UV-irradiation inhibits baseline IL-6 and IL-8 secretion from mast cells. The very low baseline level of TNF-a remained unaffected. Taken together, the present findings identify cutaneous human mast cells as important targets of UV-induced immunomodulation. They help explain both the dose-dependent adverse effects of UV-light and the beneficial and desired antiinflammatory effects during therapy.
76

Das Renin-Angiotensin-System in menschlicher Haut

Wollschläger, Tanja 04 May 2006 (has links)
In der vorliegenden Arbeit wurde die Expression von Angiotensinogen, Renin, Angiotensin-Converting-Enzym (ACE) und von den Agiotensin-Rezeptoren AT1 und AT2 in humaner Haut untersucht, um zu sehen, ob humane Haut ein lokales Gewebe Renin-Angiotensin-System (RAS) besitzt und fähig ist, Angiotensin II (Ang II) zu synthetisieren sowie welche physiologische Rolle Ang II in humaner Haut haben könnte. Außerdem wurde das Expressionsmuster von Angiotensinogen, Renin und ACE in gesunder humaner Haut mit dem in Psoriasis, Basaliom und Spinaliom (SCC) verglichen, um einen Einblick in pathophysiologische Funktionen des RAS zu gewinnen. Mit Hilfe von RT-PCR konnten alle Komponenten des RAS in vitro auf mRNA Ebene in kultivierten primären Keratinozyten, Melanozyten, dermalen Fibroblasten und dermalen mikrovaskulären Endothelzellen (MVEC´s) nachgewiesen werden, mit einer Ausnahme: Melanozyten scheinen keine AT2-Rezeptoren zu exprimieren. Immunhistochemische Untersuchungen zeigten die Expression aller Komponenten auf Proteinebene in Epidermis und dermalen Gefäßwänden in Gewebeschnitten humaner Haut. Zusätzlich erfolgte der Nachweis von Ang II in kultivierten Keratinozyten mittels enzymatischen immunometrischen Assays. Während Angiotensinogen, Renin und ACE bei immunhistochemischen Untersuchungen an Gewebeschnitten gesunder menschlicher Haut in allen Epidermalschichten gleichmäßig verteilt waren, zeigte sich bei der Psoriasis eine deutliche Betonung der unteren Epidermalschichten. Immunhistochemische Untersuchungen von Basaliomen erbrachten eine verminderte Expression von Angiotensinogen und Renin innerhalb der Tumornester. ACE wurde in den Tumorzellen noch weniger exprimiert. In immunhistochemischen Untersuchungen von Spinaliomen färbten sich die Tumorzellen deutlich homogen an. Die Experimente haben gezeigt, dass alle Komponenten des RAS in enger Lokalisation in menschlicher Haut vorkommen und dass folglich ein lokales Gewebe RAS in humaner Haut existiert sowie dass humane Haut fähig ist, Ang II ohne Zufuhr weiterer Komponenten und ohne regulatorische Einflüsse aus der Zirkulation zu synthetisieren. Eine mögliche physiologische Rolle von Ang II könnte die Regulation von Keratinozyten-Proliferation und –Differenzierung über seine Rezeptoren sein. Bezüglich der pathophysiologischen Rolle haben die Untersuchungen eine Fehlregulation des kutanen RAS in Epidermis psoriatisch veränderter Haut gezeigt, welches ein Hinweis auf eine pathogenetische Rolle des RAS bei der gestörten Keratinozyten-Proliferation und –Differenzierung sein könnte. Das Expressionsmuster in den untersuchten Tumoren war uneinheitlich, weshalb eine Interpretation der Rolle des RAS in kutanen Tumoren ohne weitere Untersuchungen kaum möglich erscheint. 1 / The present study was designed to elucidate whether a local tissue renin-angiotensin system (RAS) is expressed in human skin, whether cutaneous cells are able to autonomously synthesise angiotensin II (Ang II), and to get a first insight into a putative physiological role of Ang II in this location. For this purpose, the expression of angiotensinogen, renin, angiotensin-converting enzyme (ACE) and of the angiotensin receptors AT1 and AT2 was examined in human skin samples and in diverse cutaneous cells in primary culture on mRNA- and protein-level. Furthermore, the study compared the expression pattern of angiotensinogen, renin and ACE in healthy human skin with that in psoriasis, basal cell carcinoma (BCC) and squamous cell carcinoma (SCC) to look for possible differences between healthy and diseased skin. Using mRNA derived from cultured primary keratinocytes, melanocytes, dermal fibroblasts and dermal microvascular endothelial cells (MVECs), all components of the RAS could be demonstrated by RT-PCR except for AT2 receptors in melanocytes. Immunohistochemical stainings of cryostat sections of human skin revealed the expression of all components at protein level within the epidermis and in dermal vessel walls. In addition, the presence of Ang II in cultured keratinocytes and their supernatants could be proven by enzyme immunometric assay giving strong evidence for the ability of keratinocytes to autonomously synthesise Ang II. Regarding the comparison of RAS expression in healthy versus diseased skin, expression of angiotensinogen, renin and ACE was altered in all dermatoses examined. While in normal skin, RAS components were distributed equally and homogenously throughout all layers of the epidermis, in psoriatic skin their expression was more intense in the basal epidermal layers and less intense in the upper layers. In BCC sections, expression of angiotensinogen and renin was down-regulated, and tumour cells stained negatively for ACE. In SCC cryostat sections, tumour cells stained positively for all RAS components with an intensity comparable to normal skin. Taken together, the experiments revealed that a local tissue RAS exists in human skin, and that human skin is able to autonomously synthesise Ang II without any supply of components from the circulation. The physiological role of Ang II in normal skin may comprise the regulation of keratinocyte proliferation and differentiation. Concerning a putative pathophysiological role of Ang II in skin, this study provides evidence for a deregulation of the RAS in psoriatic skin and in BCC pointing to an involvement of the RAS in the pathomechanisms of these dermatoses. 1
77

A garantia do direito ao meio ambiente saudável pela (re)construção da racionalidade ética social contemporânea fundada na alteridade

Giongo, Rafaela Luiza Pontalti 14 January 2010 (has links)
Submitted by CARLA MARIA GOULART DE MORAES (carlagm) on 2015-04-09T17:14:15Z No. of bitstreams: 1 RafaelaGiongoDireito.pdf: 1393721 bytes, checksum: e3c98423d409555d74661ce93c754798 (MD5) / Made available in DSpace on 2015-04-09T17:14:15Z (GMT). No. of bitstreams: 1 RafaelaGiongoDireito.pdf: 1393721 bytes, checksum: e3c98423d409555d74661ce93c754798 (MD5) Previous issue date: 2010-01-14 / Nenhuma / A presente dissertação vincula-se à linha de pesquisa Sociedade, Novos Direitos e Transnacionalização do Programa de Pós-Graduação em Direito da Universidade do Vale do Rio dos Sinos ? UNISINOS, apresentando a temática da garantia do meio ambiente saudável, como um direito fundamental, através da (re)construção da racionalidade ética social contemporânea, fundada na categoria da alteridade. Como objetivos específicos procurou-se caracterizar a sociedade contemporânea como sociedade de risco e a promoção dos direitos fundamentais nesse contexto; e identificar a possibilidade de garantia do meio ambiente saudável como um direito fundamental, através da (re)construção da racionalidade ética social na categoria da alteridade, permitindo uma sociedade humana e ecologicamente viável. A pesquisa estruturou-se através do método de abordagem hipotético-dedutivo, desenvolvendose a partir de dois aportes teóricos distintos que serviram a propósitos diferenciados: Teoria dos Sistemas Sociais, desenvolvida por Niklas Luhmann, para observar a sociedade contemporânea e ilustrá-la como produtora de riscos, e o meio ambiente saudável como direito fundamental nesse contexto; e Ética da Alteridade, criada por Emmanuel Levinas, para a proposta de (re)construção da racionalidade ética social contemporânea como fundamento de uma sociedade humana e ecologicamente viável e hipótese conciliadora ao problema apresentado. Aplicou-se a categoria da alteridade ao meio ambiente, uma vez que se pode interpretá-lo como débil (ou frágil) em relação ao homem. A presente interpretação torna-se cabível em decorrência das decisões humanas, que representam um espaço intersubjetivo assimétrico para com o meio ambiente, em razão da produção e distribuição de novas espécies de riscos, os quais, sem precedentes históricos, possibilitam a destruição de toda a vida no planeta. Pôde-se concluir que ao se considerar o meio ambiente degradado como sendo o Outro, somos chamados a dar uma ?resposta? ao atual questionamento inserido pela crise ambiental, possibilitando à sociedade a abertura de uma relação de responsabilidade, ou seja, a uma relação ética e equilibrada com o meio ambiental. / This work is linked to the research line Society, New Rights and Transnationalization of the Graduate Program in Law, of the University of Vale do Rio dos Sinos - UNISINOS,featuring the theme of ensuring a healthy environment as a fundamental right, through the (re) construction of contemporary social ethical rationality, founded on the category of otherness. As specific objectives tried to characterize contemporary society as risk society and the promotion of fundamental rights in this context; and identify the possibility of ensuring a healthy environment as a fundamental right, through the (re) construction of rationality in the category of social ethics otherness, allowing a human society and ecologically viable. The research was structured by the method of hypothetical-deductive approach, developing from two distinct theoretical contributions that have served for different purposes: Theory of Social Systems, developed by Niklas Luhmann, to observe the contemporary society and illustrate it as producer risk, and healthy environment as a fundamental right in this contex; and Ethics of Alterity, created by Emmanuel Levinas, for the proposed (re) construction of rationality contemporary social ethics as the foundation of human society and ecologically viable and conciliatory to the hypothesis problem presented. The category of otherness to the environment was applied, since it may interpret it as weak (or fragile) in relation to man. This interpretation becomes appropriate as a result of human decisions, which represent an intersubjective space asymmetrical with the environment, due to the production and distribution of new kinds of risks, which, without historical precedent, allow for the destruction of all life on the planet. It was concluded that when considering the degraded environment as the Other, we are called to give an answer to the current environmental crisis by questioning inserted, enabling the society to open a relationship of responsibility, in other words, a relationship ethics and balanced with the surrounding environment.
78

Happy Meat as a Passive Revolution: A Gramscian Analysis of Ethical Meat

Gagnon, Pierre-André 08 February 2019 (has links)
This thesis starts from the proposition that the ethical meat discourse that is, the discourse recognizing that factory farming is unacceptable while maintaining that it is possible to produce meat in an acceptable way — has not been thoroughly analyzed. Indeed, both the partisans of this idea and the animal rights literature provide oversimplified analyses of this relatively new phenomenon. Considering its explosion in popularity since Michael Pollan published the essay “An Animal's Place” in The New York Times Magazine in 2002, this lack of research is particularly problematic for the animal rights movement as this new discourse directly counters its objectives. As such, this thesis uses Gramsci’s concept of passive revolution to develop a richer analysis of the apparent marginalizing effect that this discourse has on the animal rights movement. More precisely, the thesis addresses the question: “If the emergence of the ethical meat discourse is understood as part of a passive revolution, what can the specific process of passive revolution tell us about the impacts of the ethical meat discourse on the animal rights movement?” It argues that the passive revolution operates on two levels: (1) it depoliticizes the issue of meat consumption by presenting it as irrelevant and reducing it to technical details and (2) it absorbs the moderate elements of the animal rights movement by proposing an attractive alternative. Both of these processes lead to the marginalization of the few animal advocacy organizations still criticizing ethical meat. The analysis is divided in three parts. The first and second analyze respectively the content of the discourse and internal dynamics of the coalition formed around it using Maarten Hajer’s concept of discourse-coalition. Building on this comprehensive understanding of the ethical meat discourse, the actual process of passive revolution is analyzed by looking at the way the meat industry, environmental organizations and animal advocacy organizations engage with it.
79

Using music therapy and visuals to facilitate language in exceptional preschoolers

Albert, Kimberly Joy 01 January 2007 (has links)
The purpose of this project is to explore the effectiveness of combining music and visual supports as a means of facilitating communication in exceptional preschoolers. The results indicate that music and visual supports have some merit for increasing verbal responses.
80

Using popular song lyrics to teach character and peace education

Corbett, Stacy Shayne 01 January 2007 (has links)
The purpose of this project is to develop an integrative unit for peace education that is based on analyzing song lyrics and developing critical literacy.

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