Exploring the Potential of 3D Printing Construction to Address the Housing Crisis for South Sudanese Refugees

Quinn, Kyle O.'Brien

08 November 2021

South Sudan currently has the third largest refugee crisis around the globe, with over 3.7 million people being displaced from their homes due to ethnic and political civil war. Over 2 million of these refugees have been displaced from their home country, seeking asylum in refugee settlements that neighbor South Sudan. One of the most important needs within these settlements is adequate housing. Through polling and census data, it has been found that more than half of the refugees are living in dilapidated housing conditions, without any resources to make repairs. The average amount of time spent within these settlements is over a decade and is increasingly getting worse as more refugees enter these settlements. Due to the exponential technological advancements in 3D printing technology, using this form of construction could potentially address a situation within a refugee settlement. 3D printing technology could provide benefits due to its ability to produce housing units at a high rate, its ability to use clay aggregate soil as construction material, mimicking adobe brick housing found in Africa, and the ability to lower the need for labor within these settlements. This thesis will explore the idea of employing this technology within a refugee settlement, to test if it can appropriately balance the implementation of a high tech 21st century technology with the historic and cultural vernacular architecture found regionally throughout Africa. / Master of Architecture / The country of South Sudan currently is experiencing the third largest refugee crisis around the globe. Over 2.5 million refugees have fled their home country of South Sudan and are entering refugee settlements from neighboring countries. Due to the exponential increasing rate of refugees within these settlements, issues such as overcrowding and inadequate housing are afflicting the lives of everyone here. Typical houses in South Sudan consist of mud and adobe brick material known as "tukul huts". While these huts have remained the leading housing type for the past 2,000 years, these houses where not intended for addressing the common refugee crisis we are experience today. These huts require the period of months to construct and extensive physical labor. Given that the refugees are entering these settlements at an exponential rate, it is ineffective to approach housing construction in a traditional manner due to the time and effort it requires to keep up with the high demand. A possible way to address this concern, is by looking at other construction practices that could potentially supplement the traditional forms of erecting houses. Construction technology has advanced to the point where 3D printers can create life size structures that provide housing to individuals. This thesis will explore the idea of employing 3D printers into a South Sudanese refugee settlement, to see if it can adequately produce houses that provide shelter for the incoming refugees.

South Sudanese

Refugees

Crisis

3D Printing

Additive Construction

Clay Aggregate Construction

South Sudan

Uganda

Resettlement Camp

Refugee Settlements

Vernacular Architecture

Tukul Hut

« L'illusion de l'amour n'est pas l'amour trouvé » : Camp and queer desire in Jacques Demy's Les Parapluies de Cherbourg, Les Demoiselles de Rochefort, and Peau d'âne

Finch, Frank Frederick

03 November 2020

Jacques Demy's Les Parapluies de Cherbourg (1964), Les Demoiselles de Rochefort (1967), and Peau d'âne (1970), though quite popular with the public at their time of release and continuing to leave an aesthetic stamp on contemporary cinema, have been received by some critics and viewers in general as pure contrivance with little edification. This thesis puts forward, however, that such interpretations of these Demy musicals as primarily saccharine, superficial, and light miss the elemental melancholy belied by the charming varnish. Here, the three are unified as a triptych that thematizes and aestheticizes lack and desire in ways that can speak directly to the queer viewer. This thesis first situates the films among criticism from the 1960s to the present, opening a discourse on the potential for diverse political and aesthetic readings of Demy's work that continues to the present queer reading. Through a method of narratological close reading, I unify the three films as a triptych, each a variation on themes of isolation, absence, and amorous lack. Jean-Pierre Berthomé's Jacques Demy et les raciness du rêve (1982) is a rich resource in presenting these three seemingly distinct films as a totality. Once justified for study as a triptych, my thesis presents a queer reading of the films' ostensibly heterosexual narrative structures. With the buttressing of the queer theory of Harold Beaver, Andrew Ross, and Michael Koresky, among others, this chapter demonstrates how the narratives of longing Demy crafts can speak to the queer viewer and transcend a heterosexual framework. Finally, my thesis moves beyond narrative to another continuity, the aesthetic of camp present throughout the triptych. Through an exploration of the interconnectivity of camp, gender performance, and seduction, drawing on scholars Susan Sontag, Judith Butler, and Jean Baudrillard, respectively, the aesthetic of Demy's triptych is situated in a queer sensibility. Catherine Deneuve, Demy's "princesse idéale," is read as the reification of this sensibility in her potent performance of gender at the confluence of masculine and feminine qualities, as well as the ideal tabula rasa onto which the queer viewer's desire and longing can be projected. Ultimately, the triptych's reconciliation of the visually confectionary and the narratively somber is celebrated, as it points to a victory over tragedy through affective agency. / Master of Arts / Jacques Demy's Les Parapluies de Cherbourg (1964), Les Demoiselles de Rochefort (1967), and Peau d'âne (1970), French musicals from a masterful director of the New Wave movement in cinema, have been generally received positively by the public, and especially by gay viewers. Yet, these Demy films have been met with a range of skepticism to derision by some critics and even by a number of Demy's contemporaries. The three films' narratives concern a nascent romance thwarted by the Algerian War and economic demands, potential amorous encounters prevented by missed connections and arbitrary social barriers, and a flight from incestuous demands and its consequences of isolation and ridicule, respectively. Though these narratives are fundamentally melancholic, they are aestheticized through kaleidoscopic colors, virtuosic dancing, and the beautiful music scores of Michel Legrand. This thesis reexamines these films as a triptych that, considered together, thematizes lack and desire in a way that can speak directly to the queer viewer. Areas of overlap between the filmic narratives and the queer experience in the West are excavated and explored to demonstrate how the films can carry intimate signification to sexual minorities, as well as other marginalized identities. Finally, the particular and continuous aesthetic of the three films is studied as a queer sensibility embodied by the star of all three, Catherine Deneuve. The ability of this triptych to transcend a singular heterosexual interpretation and to heighten its effects on the viewer through a tension of form and content is celebrated.

Jacques Demy

Les Parapluies de Cherbourg

Les Demoiselles de Rochefort

Peau d'âne

Catherine Deneuve

camp

queer

desire

lack

seduction

gender performativity

Nouvelle Vague

affect theory

Transcriptional Insights for Spinal Cord Injury and Neural Precursor Cell Therapy: Toward a Novel Optogenetics-Based Treatment for cAMP Neuronal Induction

Martínez Rojas, Beatriz

08 March 2024

[ES] La lesión medular traumática (LM) se refiere a una condición neurológica en la que un insulto mecánico interrumpe la adecuada comunicación de impulsos nerviosos a través del sistema nervioso central (SNC), resultando en la pérdida de función locomotora por debajo del área lesionada. Lamentablemente, en la actualidad aún no existe cura efectiva para restaurar la funcionalidad después de una LM. La búsqueda de un tratamiento eficiente sigue siendo un gran desafío debido a nuestra aún incompleta comprensión de la multitud de procesos biológicos desencadenados por la lesión. La terapia celular destaca como la aproximación más recurrente para el tratamiento de la LM. En las últimas décadas, se han explorado varias estrategias celulares, siendo una de las más prometedoras el trasplante de células progenitoras neurales (CPN). Muchos estudios preclínicos demostrado el potencial del trasplante de CPN para proporcionar una recuperación motora en modelos animales, sin embargo, las mejoras funcionales en ensayos clinicos humanos son limitadas. Por lo tanto, aún se deben realizar esfuerzos para descubrir la cascada precisa de procesos moleculares a lo largo de la fisiopatología de LM, así como el mecanismo subyacente de los CPN. En ese contexto, el Capítulo 1 del presente trabajo tuvo como objetivo proporcionar una caracterización de los cambios en el perfil transcripcional medular a lo largo de las diferentes etapas temporales de una lesión severa contusiva. Además, hemos descrito el impacto transcripcional del trasplante de CPN en ratas lesionadas. Hemos demostrado que mientras la LM conllevó una fuerte desregulación de varios componentes de señalización de AMPc (entre ellos EPAC2), el trasplante de CPN pudo restaurar estas alteraciones transcripcionales. Para explorar el papel de EPAC2 en el mecanismo terapéutico mediado por CPN, realizamos un experimento de inhibición sostenida de EPAC2 mediante la administración de ESI-05. En comparación con los animales solo trasplantados, los animales CPN +ESI-05 mostraron un aumento en el área de cicatriz, una exacerbación de la polarización de la microglía hacia un perfil inflamatorio y una ampliación de la brecha de neuronas preservadas a lo largo de la lesión, sugiriendo que el trnasplante de CPN en el contexto de LM implican un mecanismo dependiente de EPAC2, reduciendo la neuroinflamación y proporcionando un entorno neuro-permisivo. El Capítulo 2 explora el potencial del AMPc para la regeneración de la LM. Hemos diseñado una estrategia innovadora para inducir AMPc en las neuronas corticoespinales a través de la activación optogenética de un adenilato ciclasa foto-inducible (bPAC). La estimulación optogenética en ratas con una hemisección dorsal torácica promovió una recuperación locomotora en comparación con el grupo control. Además, la estimulación de bPAC aumentó el número de neuronas marcadas retrógradamente desde el segmento lumbar tanto en la corteza motora como en la formación rafe-reticular, pero no en el núcleo rojo.La inmunotinción del tracto rafespinal mostró que la estimulación de bPAC aumenta el ratio de axones serotonérgicos caudales a la lesión correlacionando con una mejora funcional. Por último, la depleción del sistema serotoninérgico mediante la administración de 5,7-Dihydroxytryptamina suprimió la abolió la mejora mediada por bPAC, confirmando la implicación de la vía serotoninérgica en la recuperación de los animales estimulados. En resumen, se han proporcionado nuevos conocimientos sobre los cambios transcripcionales que ocurren a lo largo de la progresión de la LM y tras el trasplante de CPN, con énfasis en la señalización de AMPc. La manipulación optogenética de AMPc en las neuronas corticoespinales después de la LM ha demostrado ser efectiva para la recuperación funcional y permitido descubrir una ruta cortical alternativa a través del tracto descendente serotoninérgico / [CA] Lesió medul·lar traumàtica (LM) es una condició neurològica en la qual un traumatisme interromp la comunicació adequada dels impulsos a través del sistema nerviós central (SNC), amb el resultat de la pèrdua de la funció locomotora per baix de la zona lesionada. Lamentablement, en l'actualitat encara no hi ha una cura efectiva per a restaurar completament la funcionalitat de la medul·la espinal després de la lesió. La recerca d'un tractament eficient per a la LM roman un repte complex a causa de la nostra comprensió encara incompleta de la gran quantitat de processos biològics desencadenats per la lesió primària. La teràpia cel·lular destaca com l'aproximació més recurrent per al tractament de la LM. En les dècades passades, s'ha explorat diverses estratègies basades en cèl·lules i una de les més prometedores és el trasplantament de cèl·lules progenitores neurals (CPN). Molts estudis preclínics han demostrat el potencial del trasplantament de CPN per proporcionar una recuperació motora en models animals, no obstant això, les millores funcionals en pacients humans tractats són limitades. Per tant, encara s'han de fer esforços per a descobrir la cascada precisa de processos moleculars al llarg de la fisiopatologia de la LM, així com el mecanisme subjacent dels CPN. El Capítol 1 del present treball va tindre com a objectiu proporcionar una caracterització dels canvis en el perfil transcripcional espinal al la llarga de les diferents etapes temporals de una lesió contusiva. A més, s'ha descrit l'impacte transcripcional del trasplantament d'CPN en animals lesionats. S'ha demostrat que mentre la LM va causar una forta desregulació de diversos components de senyalització de AMPc (sent EPAC2 el gen més regulat a la baixa), el transplantament de CPN van ser capaç de restaurar les alteracions derivades de la LM. Per a explorar el paper d'EPAC2 en el mecanisme terapèutic mediat per CPN, es va realitzar un experiment de inhibició sostinguda d'EPAC2 degut a l'administració d'ESI en animals lesionats. En comparació amb els animals només trasplantats, els animals CPN+ESI-05 van mostrar un augment de l'àrea de cicatriu, una exacerbació de la polarització de les micròglies cap a un perfil inflamatori i una ampliació de la bretxa de neurones preservades a través de la lesió.Aquests resultats suggereixen que el trasplantament de CPN en el context de la LM involucren un mecanisme depenent d'EPAC2, reduint la neuroinflamació i proporcionant un entorn més neuropermissiu. El Capítol 2 va tindre com objectiu explotar el potencial de regeneració de AMPc dissenyant una nova estratègia per a les induccions artificials de AMPc en les neurones corticoespinals mitjançant l'activació optogenètica d'una adenilat ciclasa fotoinduïble (bPAC). L'estimulació diària de AMPc en rates que pateixen una hemisècció dorsal toràcica va promoure una recuperació en comparació amb els control. L'estimulació de bPAC va augmentar el nombre de neurones marcades retrògradament des del segment lumbar, tant a l'escorça motora com a la formació rafe-reticular, però no al nucli roig. A més, la immunotinció del tracte rafespinal va mostrar que l'estimulació de bPAC va augmentar la ràtio d'axons serotoninèrgic cabals a la lesió, cosa que es va correlacionar significativament amb una millora dels paràmetres funcionals. Finalment, la depleció del sistema serotoninèrgic mitjançant l'administració de 5,7-Dihydroxytryptamina va abolir la millora mediada per bPAC, confirmant la implicació de la via serotoninèrgica en la recuperació. En resum, la investigació ha proporcionat coneixements sobre els canvis transcripcionals que tenen lloc a la llarga de la progressió de la LM i després del trasplantament de CPN, amb un èmfasi especial en la senyalització d'AMPc. La manipulació optogenètica d'AMPc a les neurones corticoespinals després de la LM ha demostrat ser efectiva per a la recuperació funcional i ha permès descobrir una ruta cortical alternativa a través del tracte descendent serotoninèrg / [EN] Traumatic spinal cord injury (SCI) refers to a neurological condition in which a mechanic insult disrupts the proper communication of the impulses through the central nervous system (CNS), resulting on the loss of locomotor function below the injured area. Unfortunately, nowadays there is still no effective cure to completely restore the functionality of the spinal cord after the injury. Cell therapy is the most recurring approach for SCI treatment. In the past decades several cell-based strategies have been explored, being one of the most promising the transplantation of neural progenitor cells (NPCs). Many pre-clinical studies evidenced the potential of the NPCs transplantation to provide a substantial motor recovery in animal models, yet functional improvements in clinical trials have been limited. Therefore, efforts still need to be made in disclosing the precise cascade of molecular processes along SCI pathophysiology as well as the NPCs underlying mechanism. In that context, Chapter 1 of the present work aimed to provide a comprehensive characterization of the spinal transcriptional changes along the different temporal stages of rats suffering a severe contusive injury. Additionally, we have described the transcriptional impact of acute and subacute NPCs transplantation in injured animals. Interestingly we have shown that while SCI caused a strong dysregulation of several cAMP-signaling components (being EPAC2 the most downregulated gene), NPCs was able to restore SCI-derived alterations over this pathway with EPAC2 significant upregulation. In order to further explore EPAC2 role in NPCs-mediated therapeutical mechanism we performed a loss-of-function experiment by sustained EPAC2 inhibition via ESI-05 administration along with NPCs transplantation after SCI. Compared with only transplanted animals, NPCs+ESI-05 animals showed increased scar area, exacerbated microglia polarization into an inflammatory profile and widened gaps of preserved neurons across the lesion. Overall, these results suggest that NPC therapeutic mechanisms in the context of SCI involve an EPAC2-dependent mechanism, reducing neuroinflammation and providing a neuro-permissive environment. Chapter 2 aimed to further explore cAMP potential for SCI regeneration. We designed a novel strategy for artificial cAMP inductions in corticospinal neurons via optogenetic activation of a photoinducible adenylyl cyclase (bPAC). Daily optogenetic cAMP stimulation in rats suffering a thoracic dorsal hemisection, which completely disrupt the dorsal aspect of the corticospinal tract (CST), promoted and early and sustained locomotor recovery compared to non-treated control animals. We have shown that bPAC stimulation increased the number of retrograde traced neurons from the lumbar segment both in the motor cortex and the raphe-reticular formation, but not in the red nuclei. Moreover, immunolabelling of the raphespinal tract by 5-HT showed that bPAC stimulation increased the ratio of descending serotoninergic axons caudal to the injury which significantly correlated with improved functional parameters. Our results from corticobulbar projection study, WGA trans-synaptic tracing, and P-CREB analysis suggest that bPAC modulation of cortico-serotonergic pathway might occurs at the brainstem level. Lastly, the serotonergic system depletion by 5,7-Dihydroxytryptamine administration suppressed bPAC-mediated recovery, confirming the implication of the serotonergic tract in the recovery of stimulated animals. In summary, our research has provided new insights into the transcriptional changes that occur along SCI progression and after NPCs transplantation with a special emphasis on cAMP signaling. Optogenetic cAMP manipulation in corticospinal neurons after SCI has proven to be effective for functional recovery and allowed to unveil a cortical rerouting pathway through the serotonergic descending tract. / This research was funded by FEDER/Ministerio de Ciencia e Innovación – Agencia Estatal de Investigación [RTI2018-095872-BC21/ERDF]. Part of the equipment employed in this work was funded by Generalitat Valenciana and cofinanced with ERDF funds (OP ERDF of Comunitat Valenciana 2014– 2020) and the UE; Fondo Europeo de Desarrollo Regional (FEDER) incluido en el Programa Operativo FEDER de la Comunidad Valenciana 2014-2020. B. MartinezRojas was supported by a grant from the Conselleria de Educación, Investigación, Cultura y Deporte de la Generalitat Valenciana and the European Social Fundation ACIF/2019/120. / Martínez Rojas, B. (2024). Transcriptional Insights for Spinal Cord Injury and Neural Precursor Cell Therapy: Toward a Novel Optogenetics-Based Treatment for cAMP Neuronal Induction [Tesis doctoral]. Universitat Politècnica de València. https://doi.org/10.4995/Thesis/10251/202972

Movilidad

Locomotion

Neural Progenitor Cell Transplantation

Regeneración

Regeneration

cAMP

Optogenética

Optogenetics

Lesión medular

Spinal Cord Injury

BIOLOGIA CELULAR

Konstruktion und Charakterisierung einer lichtaktivierten Phosphodiesterase

Gasser, Carlos Fernando

03 December 2015

Genetisch kodierte Photorezeptoren in Modellorganismen begründen die Optogenetik. Sie ermöglicht die nicht-invasive, reversible und räumlich-zeitlich präzise Perturbation von zellulären und physiologischen Signalprozessen durch Licht. Natürliche photoaktivierte Adenylylzyklasen (PACs) steigern die intrazelluläre Konzentration des Botenstoffs zyklischen Adenosinmonophosphats (cAMP) durch Blaulicht. Damit erlauben sie die optogenetische Analyse von cAMP-abhängigen Signalwegen. Diese Arbeit komplementiert PACs durch die synthetische rotlichtaktivierte Phosphodiesterase LAPD zur Degradation von cAMP und zyklischem Guanosinmonophosphat (cGMP). LAPD ist eine Chimäre aus dem photosensorischen Modul von Deinococcus radiodurans Bakteriophytochrom (DrBPhy) und der Effektordomäne der cAMP/cGMP-spezifischen H. sapiens Phosphodiesterase 2A (HsPDE2A). Die Fusionsstelle wurde von den helikalen Linkern zwischen Sensor- und Effektormodulen durch strukturelle Überlagerung abgeleitet. LAPD inkorporierte den Chromophor Biliverdin (BV) nach Expression in E. coli und Reinigung vollständig und entsprach spektral und photochemisch dem Wildtyp-DrBPhy. Durch Bestrahlung mit Rot- und Fernrotlicht (R bzw. FR) wurde LAPD in die metastabilen photochemischen Zustände Pfr (fernrot) bzw. Pr (rot) umgewandelt. Vollständig aktivierte LAPD katalysierte die Hydrolyse von cGMP und cAMP in derselben Größenordnung wie Wildtyp-HsPDE2A. LAPD degradierte cGMP und cAMP bei 6- bzw. 4-facher Steigerung von vmax unter R im Vergleich zu dunkeladaptiertem Enzym. Die Aktivität von R-adaptierter LAPD wurde durch FR reduziert. Die enzymatische Aktivität und Lichtregulation von LAPD-Linkervarianten waren abhängig von der Linkerlänge. LAPD degradierte lichtabhängig cGMP in einer PDE-Reporterzelle. Dabei genügte die endogene BV-Konzentration der Säugerzelle zur Sättigung des Lichteffekts. / Genetically encoded photoreceptors in model organisms establish optogenetics. It enables non-invasive, reversible, and spatio-temporally precise perturbation of cellular and physiological signalling by light. Natural photoactivated adenylate cyclases (PACs) increase the intracellular concentration of the second messenger cyclic adenosine monophosphate (cAMP) under blue light. Hence, PACs allow the optogenetic analysis of cAMP-dependent signalling. This work complements PACs with the synthetic red-light-activated phosphodiesterase LAPD for degradation of cAMP and cyclic guanosine monophosphate (cGMP). LAPD is a chimera made up of the photosensory module of Deinococcus radiodurans bacteriophytochrome (DrBPhy) and the effector domain of cAMP/cGMP-specific H. sapiens Phosphodiesterase 2A (HsPDE2A). The fusion site was derived from the helical linkers between sensor and effector modules via structural superposition. LAPD incorporated the chromophor biliverdin (BV) after expression in E. coli and purification quantitatively, and spectrally and photochemically resembled the wildtype DrBPhy. Upon irradiation with red and far-red light (R and FR, resp.), LAPD was converted to the metastable photochemical states Pfr (far-red) and Pr (red), respectively. Fully activated LAPD catalized the hydrolysis of cGMP and cAMP with rates similar to wildtype HsPDE2A. LAPD degraded cGMP and cAMP with 6- and 4-fold increase of vmax under R, respectively, as compared to the dark state. The activity of R-adapted LAPD was reduced upon irradiation with FR. Enzymatic activity and light regulation of LAPD linker variants depended on the linker length. LAPD light-dependently degraded cGMP in a PDE reporter cell line. Endogenous BV concentrations were sufficient to saturate the light effect in the mammalian cell, which enables a true optogenetic approach.

cGMP

cAMP

Optogenetik

Bakteriophytochrom

Phosphodiesterase

zyklische Nukleotide

synthetische Photorezeptoren

optogenetics

bacteriophytochrome

phosphodiesterase

cyclic nucleotide

synthetic photoreceptor

570 Biologie

32 Biologie

WE 5320

ddc:570

Les ombres du monde : Anders et le refus du nihilisme / The shadows of the world : Anders and the refusal of nihilism

Jolly, Édouard

10 December 2013

Ancien élève de Husserl et Heidegger, Günther Anders (1902-1992) composa une oeuvre philosophique dont la particularité est d'interroger la situation de l'homme face aux événements les plus sombres du 20e siècle. Ce travail, élaboré à partir d'une lecture de l'oeuvre éditée à ce jour, complétée par celle du Nachlass, vise à ressaisir l'unité, la cohérence et la singularité de sa pensée autour d'une question majeure : comment un monde technicisé, un monde sans hommes, est-Il compatible avec une éthique pour des hommes sans monde ? Décrire les ombres du monde, celles d'abord laissées par un monde humain technicisé, c'est déceler les idéalités de la technique qui recouvrent chaque chose d'une évidence artificielle. Observer le monde fabriqué par des hommes devenus des ombres, c'est aussi percevoir qu'ils peuplent un environnement dont ils sont les produits. Ce monde artificiel, à défaut de ne faire que soulager l'hostilité naturelle, ajoute d'autres souffrances au poids de la nécessité, que les arts parviennent à peine à déjouer. Théoriser les ombres du monde, c'est relever la négativité d'un nihilisme réalisé par la technique, à refuser. L'hypothèse philosophique ici défendue est celle d'un nihilisme métaphysique conçu comme préalable nécessaire au refus de toute autre pratique nihiliste. A cet effet, à partir de l'oeuvre d'Anders se conçoit une philosophie occassionnelle comme pratique théorique d'une sobriété tragique. Si briser toute idée métaphysique aboutit à désenchanter les victimes de trop naïves généralités, cette théorie n'impose cependant en rien de s'interdire de faire de la métaphysique. / As a former student of Husserl and Heidegger, Günther Anders (1902-1992) wrote a philosophical work which characteristic is to examine the situation of man facing the darkest events of the 20th century. Our thesis developed with a reading of the edited work supplemented by the Nachlass, aims to synthesize the unity consistency and uniqueness of his thoughts by asking a specific question : how a technical world, a world without men, could be compatible with any ethic for men without world ? To describe the shadows of the world left by a technical one, is meant to identify idealities which cover everything with an artificial obviousness. To observe the world made by men, who themselves became shadows, is like to perceive thet they are living in a environment whose they are the products. This artificail world, instead of relieving man about the nature hostility, adds other difficulties, which the technology is only sometimes able to cope with. To theorize the shadows of the world is meant to seek the specific negativity of nihilism, which is produced by technology. Our task is to show that we can refuse the nihilism as an attitude. The philosophical hypothesis defended here is metaphysical nihilism designed as prerequisite for the refusal of any other nihilistic praxis. The philosophical work of Anders allows us to conceive an occasional philosophy as a theoretical practice, pointed out as a tragic sobriety. If to break any metaphysical idea leads to disenchant the naïve victims of generalities, this theory however does not refrain us from doing metaphysics.

Günther Anders

Nihilisme

Technique

Désuétude

Prométhée

Herméneutique

Métaphysique

Monde

Mort

Situation

Présence

Tonalité affective

Liberté

Culture

Machine

Camp

Nucléaire

Hégémonie

Menace

Günther Anders

Nihilism

Technology

Outdatedness

Prometheus

Hermeneutics

Metaphysic

World

Death

Situation

Presencing

Mood

Freedom

Culture

Machine

Camp

Nuclear

Hegemony

Threat

Atraktivita letního tábora YMCA / Attractiveness of the summer camp with a spiritual program

ROH, Zdeněk

January 2019

The diploma thesis concentrates on and deals with the attractiveness of YMCA summer camp. The aim is to find out what factors are able to influence the decisions of children and parents if they take part in this camp. The work has been bringing in the different possibilities of activities. It is expected from these activities to have the ability in infuencing the attractiveness of this characteristic the summer camp. These activities have been proved by evidence and realized on the specific cases in the practice in this diploma thesis. The answers have been looked for in the context of the basic research question and the diploma thesis has been drawing conclusions on the basic of the research result of the sample of respondents.

Deoli Camp: An Oral History of the Chinese Indians from 1962 to 1966

Li, Kwai

11 August 2011

China and India claimed two territories along their borders on the Himalayas: Aksai Chin in the west and the North-East Frontier Agency in the east. The border dispute escalated and, on October 20, 1962, the Chinese People’s Liberation Army (PLA) opened fire on the two fronts and advanced into the disputed territories. One month later, on November 21, China declared a unilateral ceasefire and withdrew behind its disputed line of control. In response, the Indian government arrested over 2,000 Chinese living in India and interned them in Deoli, Rajasthan. When the Chinese were released between 1964 and 1966, they found their properties sold off by the Indian government. Many left India and immigrated to Canada. I interviewed four Indian-born Chinese who were interned and who now live in the Greater Toronto Area. I recorded their accounts of life in Deoli Detention Camp in Rajasthan.

Oral history

Interview method

translation

transcription

1962 Sino-Indian Incident

Chinese-Indians

China-India border war

Hakka Chinese

Aksai Chin

North-East Frontier agency (NEFA)

McMahon Line

Johnson and Macartney-McDonald Lines

Chou En-Lai

Jawaharlal Nehru

Indian Enemy Property Law of 1968

1962 Defence of India Rule

Tibet

China

India

British India

Deoli detention Camp, Rajasthan

Deoli Concentration Camp

Calcutta Chinatown

Chinese Diaspora in India

0332

0279

Deoli Camp: An Oral History of the Chinese Indians from 1962 to 1966

Li, Kwai

11 August 2011

China and India claimed two territories along their borders on the Himalayas: Aksai Chin in the west and the North-East Frontier Agency in the east. The border dispute escalated and, on October 20, 1962, the Chinese People’s Liberation Army (PLA) opened fire on the two fronts and advanced into the disputed territories. One month later, on November 21, China declared a unilateral ceasefire and withdrew behind its disputed line of control. In response, the Indian government arrested over 2,000 Chinese living in India and interned them in Deoli, Rajasthan. When the Chinese were released between 1964 and 1966, they found their properties sold off by the Indian government. Many left India and immigrated to Canada. I interviewed four Indian-born Chinese who were interned and who now live in the Greater Toronto Area. I recorded their accounts of life in Deoli Detention Camp in Rajasthan.

Oral history

Interview method

translation

transcription

1962 Sino-Indian Incident

Chinese-Indians

China-India border war

Hakka Chinese

Aksai Chin

North-East Frontier agency (NEFA)

McMahon Line

Johnson and Macartney-McDonald Lines

Chou En-Lai

Jawaharlal Nehru

Indian Enemy Property Law of 1968

1962 Defence of India Rule

Tibet

China

India

British India

Deoli detention Camp, Rajasthan

Deoli Concentration Camp

Calcutta Chinatown

Chinese Diaspora in India

0332

0279

Die funktionelle Modifikation der proinflammatorischen M-DC8+ dendritischen Zellen durch zyklisches Adenosin-Monophosphat / Functional modification of the proinflammatory M-DC8+ dendritic cells by cyclic adenosine monophosphate

Ebling, Annette

23 June 2005

In this work, the influence of the second messenger cAMP on the functional plasticity of M-DC8+ dendritic cells (DC) was examined. The marker M-DC8 defines a population of native DC first described in blood. After their isolation, M-DC8+ DC acquire a mature CD83+ phenotype during a short culture ex vivo. After a challenge with LPS and IFN-g, M-DC8+ DC secrete large amounts of the proinflammatory cytokines IL-12(p70) and TNF-a surpassing by far other DC populations and monocytes. Due to their preferential induction of TH1-dominated T cell responses, M-DC8+ DC might play a role in the pathogenesis of inflammatory diseases. Different cAMP-elevating agents suppressed the proinflammatory cytokine production and enhanced the secretion of anti-inflammatory IL-10. Activity of phosphodiesterase (PDE) 4, the most important cAMP-hydrolysing enzyme in immune cells, was detected and RT-PCR revealed the expression of PDE4 subtypes 4A, 4B and 4D in M-DC8+ DC, whereas 4C was not detectable. The PDE4-specific inhibitors AWD12-281 and Roflumilast were then used to elevate cAMP concentrations. These substances have been proven to be efficient in anti-inflammatory therapies. In the presence of PDE4 inhibitors, the LPS/IFN-g-induced production of IL-12 and TNF-a was decreased by 90 % and 60 %, respectively, whereas the IL-10-release was doubled. These effects were only observed, if the PDE4 inhibitors where present from the beginning of the culture. The inhibition of the IL-12 secretion was reverted using an a-IL-10-receptor antibody. PDE4 inhibitor-treated M-DC8+ DC showed a reduced capacity to polarize TH1-cells, which was demonstrated analysing culture supernatants by ELISA and by single-cell analysis detecting intracellular IFN-g und IL-4. These results suggest that PDE4 inhibitors may not only be useful in the therapy of TH2-mediated diseases but also in TH1-dominated indications such as multiple sclerosis and Crohn´s disease. Despite the shift of the cytokine profile, the in vitro maturation of M-DC8+ DC was not affected by PDE4 inhibitors. The expression of CD83, CD80, CD86, MHC-molecules as well as CD54 and CD58, was assessed by FACS analysis. Correspondingly, in the presence of AWD12-281, M-DC8+ DC efficiently stimulated the proliferation of allogeneic CD4+CD45RA+ T-cells. In the second part of this study, the effects of an inhibition of cAMP-synthesis in M-DC8+ DC were analyzed. Two adenylyl cyclase (AC) inhibitors, 2,5-Dideoxyadenosine and SQ22536, clearly hampered the in vitro maturation of M-DC8+ DC. The expression of the DC maturation marker CD83 could be reconstituted using the stable cAMP-analogon 8-Br-cAMP. Measuring the intracellular cAMP concentration in M-DC8+ DC, initially low cAMP-levels were observed, but within 30 min the concentration raised and returned to original levels within 2 hrs. Blocking the cAMP synthesis by AC inhibitors, the LPS/IFN-g-induced production of IL-12, TNF-a and IL-10 was strongly reduced. Furthermore, it was demonstrated that M-DC8+ DC can only release IL-12 after a transient elevation of cAMP, i.e. they acquire a "license". Such a regulation of the IL-12 production has not been described before. Protein kinase A is an important effector molecule of cAMP. Inhibiting its activity resulted in a reduced expression of the DC maturation marker CD83 and a lower cytokine production underlining the importance of cAMP-signalling for the activation of M-DC8+ DC. In conclusion, this study provides evidence for a new concept of the immune-regulatory function of cAMP. Here, cAMP is essentially involved in the initial activation and maturation of DC and enables them to secrete large amounts of IL-12 and TNF-a upon stimulation with a TLR ligand. Conversely, a long-term elevation of cAMP-concentrations inhibits the proinflammatory effector functions of M-DC8+ DC and can induce anti-inflammatory responses by enhancing the secretion of IL-10. / In dieser Arbeit wurde der Einfluss des second messengers cAMP auf die funktionelle Plastizität von M-DC8+ dendritischen Zellen (DC) untersucht. Der Oberflächenmarker M-DC8 definiert eine zunächst im Blut beschriebene Population nativer DC. Nach ihrer Isolation erlangen M-DC8+ DC während einer kurzen Kultur einen maturen CD83+ Phänotyp. Nach Stimulation mit LPS und IFN-g produzieren native M-DC8+ DC deutlich höhere Mengen der proinflammatorischen Zytokine IL-12(p70) und TNF-a als andere DC-Populationen oder Monozyten. Dies resultiert in einer Programmierung TH1-dominierter T-Zellantworten. M-DC8+ DC könnten daher an der Pathogenese entzündlicher Krankheiten beteiligt sein. Unterschiedliche cAMP-erhöhende Substanzen supprimierten die proinflammatorische Zytokinproduktion und verstärkten gleichzeitig die Sekretion des anti-inflammatorischen IL-10. In M-DC8+ DC konnte die Aktivität von Phosphodiesterase (PDE) 4, dem wichtigsten cAMP-hydrolysierenden Enzym in Immunzellen, nachgewiesen werden. Durch RT-PCR wurde die Expression der PDE4-Subtypen 4A, 4B und 4D gezeigt, nicht aber 4C. Zur Erhöhung der cAMP-Konzentration wurden dann die PDE4-spezifischen Inhibitoren AWD12-281 und Roflumilast eingesetzt, deren klinische Effizienz bei anti-inflammatorischen Therapien belegt ist. Auch diese Substanzen verringerten die LPS/IFN-g-induzierte Produktion von IL-12 und TNF-a durch M-DC8+ DC um 90 % bzw. 60 %, während die IL-10-Freisetzung etwa verdoppelt wurde. Diese starken Effekte konnten nur erzielt werden, wenn die PDE4-Inhibitoren von Beginn der Kultur an eingesetzt wurden. Die Hemmung der IL-12-Sekretion wurde in Gegenwart eines a-IL-10-Rezeptor-Antikörpers aufgehoben. Unter dem Einfluss von PDE4-Inhibitoren war die TH1-Programmierung durch M-DC8+ DC deutlich reduziert, was sowohl durch die Analyse der Zellüberstände mittels ELISA als auch auf Einzelzell-Ebene durch intrazelluläre Detektion von IFN-g und IL-4 nachgewiesen wurde. Diese Ergebnisse legen nahe, dass PDE4-Inhibitoren nicht nur für TH2-vermittelte Erkrankungen sondern auch für TH1-dominierte Indikationen wie Multiple Sklerose oder Morbus Crohn von Nutzen sein könnten. Trotz der starken Modulation des Zytokinprofils blieb die in vitro-Ausreifung M-DC8+ DC unbeeinflusst von PDE4-Inhibitoren. Untersucht wurde die Expression von CD83, CD80, CD86, MHC-Molekülen, CD54 und CD58 mittels FACS-Analyse. Entsprechend induzierten M-DC8+ DC auch in Anwesenheit von AWD12-281 die Proliferation allogener CD4+CD45RA+ T-Zellen. Im zweiten Teil der Arbeit wurde untersucht, wie sich die Blockade der cAMP-Synthese auf M-DC8+ DC auswirkt. Zwei Adenylatcyclase-Inhibitoren, 2,5-Dideoxyadenosine und SQ22536, hemmten die in vitro-Maturation von M-DC8+ DC deutlich. Die CD83-Expression wurde mit 8-Br-cAMP rekonstituiert. Messungen der intrazellulären cAMP-Konzentration in unbehandelten M-DC8+ DC zeigten initial niedrige cAMP-Spiegel, die innerhalb von 30 min anstiegen und nach 2 h wieder auf das Ausgangsniveau abfielen. Die LPS/IFN-g-induzierte Produktion von IL-12, TNF-a und IL-10 wurde durch AC-Inhibitoren deutlich vermindert. M-DC8+ DC erhalten nur nach einer transienten cAMP-Erhöhung die "Lizenz" IL-12 freizusetzen. Eine derartige Regulation der IL-12-Sekretion ist bisher nicht beschrieben. Eine Hemmung des cAMP-Effektormoleküls Proteinkinase A resultierte in der reduzierten Expression des DC-Maturationsmarkers CD83 und einer verringerten Zytokinproduktion. Dies unterstreicht die Bedeutung von cAMP für die Aktivierung M-DC8+ DC. Zusammenfassend gibt diese Arbeit am Beispiel nativer humaner DC Anhalt für ein neues Konzept der immunregulatorischen Funktion von cAMP. Hierbei ist cAMP wesentlich an der Ausreifung von M-DC8+ DC beteiligt, woraufhin diese große Mengen IL-12 und TNF-a sekretieren können. Dagegen wirkt eine langfristige cAMP-Erhöhung durch die Induktion von IL-10 anti-inflammatorisch.

Adenylatcyclase

IL-10

IL-12

Immunregulation

Phosphodiesterase (PDE) 4

T-Zellen

TNF-a

anti-inflammatorisch

cAMP

dendritische Zellen (DC)

IL-10

IL-12

T cells

TNF-a

adenylyl cyclase

anti-inflammatory

cAMP

dendritic cells (DC)

immune regulation

phosphodiesterase (PDE) 4

ddc:171

rvk:WF 9890

Adenylatcyclase

Cyclo-AMP

Cytokine

Entzündung

Immunsystem

Phosphodiesterasen

Regulation

T-Lymphozyt

dendritische Zelle

Das Maximilian-Kolbe-Werk : Wegbereiter der deutsch-polnischen Aussöhnung 1960 - 1989 /

Stempin, Arkadiusz.

January 2006

Univ., Diss.--Freiburg, 2002.