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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.
31

Social Capital, Non-governmental Organisations and Development: A Study of the Impact of Intermediary Actors on Household Wellbeing.

Gemechu, Shambel. January 2007 (has links)
<p><font face="Times New Roman" size="3"><font face="Times New Roman" size="3"> <p align="left">The Social Capital approach to development is based on the premise that both cognitive and structural aspects of a given society determine the level of development performance. It is argued that norms of trust and reciprocity, networks, and mutual aid govern interaction among people, hold them together, facilitate opportunities to manage common property and pursue common goals, and ultimately contribute to development by facilitating their cooperation and collective action. In this thesis I explore the relationship between social capital and development by analysing the performance of household wellbeing in a given community. Two dominant views on social capital and the outcomes of development performance are currently in prominence in the development discourse. This debate centres on whether social capital is a sufficient cause on its own or whether it needs intermediary actors.</p> </font></font></p>
32

Social capital, non-governmental organisations and development: a study of the impact of intermediary actors on household wellbeing.

Gemechu, Shambel. January 2007 (has links)
<p><font face="Times New Roman" size="3"><font face="Times New Roman" size="3"> <p align="left">The Social Capital approach to development is based on the premise that both cognitive and structural aspects of a given society determine the level of development performance. It is argued that norms of trust and reciprocity, networks, and mutual aid govern interaction among people, hold them together, facilitate opportunities to manage common property and pursue common goals, and ultimately contribute to development by facilitating their cooperation and collective action. In this thesis I explore the relationship between social capital and development by analysing the performance of household wellbeing in a given community. Two dominant views on social capital and the outcomes of development performance are currently in prominence in the development discourse. This debate centres on whether social capital is a sufficient cause on its own or whether it needs intermediary actors. The social capital theory argues that the development performance of a particular community can be explained directly by the prevailing level of social capital, and that the underlying levels of trust, social norms and networks are sufficient to explain development. On the other hand, the school of thought that supports the need for intermediary actors argues that social capital is unable to influence development performance at higher levels. If a larger impact and a more precise outcome are expected, intermediary actors who facilitate interest formation, aggregation and representation are necessary. Without them, social capital remains largely inactive and dormant. In exploring the possible link between the two variables, this thesis supports the second premises, introducing the notion of intermediary actors that might activate the stock of social capital and its performance on household wellbeing. The need to explore the relationship between the two variables demanded empirical research. The research was conducted in the rural villages of Oromia regional State of Ethiopia. Based on the empirical evidence, the relationship between the stock of social capital and performance in household wellbeing is generally positive. A large stock of social capital is generally accompanied by a higher level of performance in household wellbeing. However, I argue that social capital is only truly social when activated by an intermediary development actor. Failing this, though it contributes significantly to village solidarity and unity, social capital remains inactive and dormant. Therefore, the general conclusion of this thesis is that social capital matters, but its utilisation by intermediary agencies matters more.</p> </font></font></p>
33

Impulsive Differential Equations with Applications to Infectious Diseases

Miron, Rachelle 17 April 2014 (has links)
Impulsive differential equations are useful for modelling certain biological events. We present three biological applications showing the use of impulsive differential equations in real-world problems. We also look at the effects of stability on a reduced two-dimensional impulsive HIV system. The first application is a system describing HIV induction-maintenance therapy, which shows how the solution to an impulsive system is used in order to find biological results (adherence, etc). A second application is an HIV system describing the interaction between T-cells, virus and drugs. Stability of the system is determined for a fixed drug level in three specific regions: low, intermediate and high drug levels. Numerical simulations show the effects of varying drug levels on the stability of a system by including an impulse. We reduce these two models to a two-dimensional impulsive model. We show analytically the existence and uniqueness of T-periodic solutions, and show how stability changes when varying the immune response rate, the impulses and a certain nonlinear infection term. The third application shows how seasonal changes can be incorporated into an impulsive differential system of Rift Valley Fever, and looks at how stability may differ when impulses are included. The analysis of impulsive differential systems is crucial in developing more realistic mathematical models for infectious diseases.
34

Petrochemistry and geochronology of Ngorongoro Volcanic Highland Complex (NVHC) and its relationship to Laetoli and Olduvai Gorge, Tanzania

Mollel, Godwin F. January 2007 (has links)
Thesis (Ph. D.)--Rutgers University, 2007. / "Graduate Program in Geological Sciences." Includes bibliographical references (p. 219-232).
35

Diagnostics for Rift Valley fever virus

Upreti, Deepa January 1900 (has links)
Master of Science / Department of Diagnostic Medicine/Pathobiology / A. Sally Davis / Rift Valley fever virus (RVFV) is a mosquito-borne, zoonotic Phlebovirus that is a significant threat to ruminants and humans. RVFV is categorized as an overlap Select Agent by the Department of Health and Human Services and US Department of Agriculture. Therefore, the study of RVFV’s pathogenesis and the development of novel diagnostic tools for the prevention and control of outbreaks and virus spread is crucial. RVF is endemic to sub-Saharan Africa but has spread beyond the continent to the Arabian Peninsula indicating the competence of the virus to emerge in new areas. Thus, the high likelihood of RVF’s spread to other non- endemic countries also spurs the need for development and implementation of rapid diagnostic tests and surveillance programs. In the US, RVFV is a Select Agent, requiring BSL-3 enhanced containment practices for research work. First, we developed a method for the detection of RVFV RNA by reverse transcriptase real-time PCR (RT-qPCR) using non-infectious, formalin- fixed, paraffin-embedded tissues (FFPET). The results from FFPET RT-qPCR were compared to prior results for fresh-frozen tissues (FFT) RT-qPCR, as well as immunohistochemistry and histopathology completed on the same FFPET blocks. We developed a novel technique using a rapid and low cost magnetic bead extraction method for recovery of amplifiable RVFV RNA from FFPET. FFPET RT-qPCR can serve as an alternative tissue-based diagnostic test, which does not require a BSL-3 research facility. Second, we assessed the diagnostic accuracy and precision of a recombinant RVFV nucleoprotein based competitive ELISA (cELISA) assay to detect RVFV antibodies. The cELISA results were compared to the virus neutralization test, the gold standard serological assay for RVFV. This prototype cELISA is easy to implement, sensitive, specific, and safe test for the detection of antibodies to RVFV in diagnostic and surveillance applications. RVF is an important transboundary disease that should be monitored on a regular basis. The diagnostic tests developed and validated in this thesis could be used in endemic or non-endemic countries for the early detection of RVF and assist with the implementation of countermeasures against RVFV.
36

The development of novel diagnostic countermeasures for Rift Valley fever virus

Ragan, Izabela January 1900 (has links)
Doctor of Philosophy / Department of Diagnostic Medicine/Pathobiology / A. Sally Davis / William Wilson / Rift Valley fever virus (RVFV) is a zoonotic arbovirus that is a significant threat to livestock and humans. It is listed as #3 for most dangerous animal threats and is in the top 10 pathogens needing urgent research in preventative and control measures. Although RVFV has never been reported in the US or Europe, outbreaks outside the African continent have sparked renewed interest in developing diagnostics and vaccines to protect both agriculture and public health. Having specific and versatile diagnostics is critical for vaccine development and application. For example, diagnostic tools that aid in identifying key immunogens and understanding the virus-host interaction directly contribute to developing protective vaccines. Additionally, vaccines that are used prophylactically or in response to an outbreak require diagnostic tests to differentiate infected from vaccinated animals (DIVA). This is critical for assessing the return to ‘disease free’ status after an outbreak. Unfortunately, there are limited RVFV diagnostic tests that are versatile and DIVA compatible with the newest RVFV vaccines. We describe the development of several diagnostic tools that are DIVA compatible for detecting RVFV nucleic acid, antibodies, and antigens. First, we evaluate a fluorescence microsphere immunoassay (FMIA) for the detection of antibodies against a RVFV surface glycoprotein and the nucleocapsid protein. The targets developed in this assay provide the basis for a DIVA-compatible serological assay with a candidate RVFV Gn/Gc subunit vaccine, as well as, offer a multiplexing platform that can simultaneously screen for several ruminant diseases. Second, we describe a novel chromogenic in situ hybridization (ISH) assay to detect RVFV in formalin-fixed, paraffin-embedded (FFPE) tissues. This molecular assay offers a highly sensitive, multiplexing platform that detects RVFV RNA on the cellular level of diagnostic tissue samples. Moreover, we demonstrate the first application of ISH as a DIVA-compatible assay for candidate RVFV gene-deletion vaccines. Third, we provide working protocols for western blot (WB), immunohistochemistry (IHC), and immunofluorescence (IF) that use monoclonal or polyclonal antibodies against key RVFV antigens. These tools can be applied to pathogenesis research and used in the development of vaccine and therapeutic countermeasures against RVFV. The RVFV diagnostic methods developed and evaluated in this dissertation can serve as a model for developing diagnostic strategies for other transboundary animal diseases.
37

Génétique de la résistance à la fièvre de la vallée du Rift : Rvfs2 confére une tolérance à l'hépatite / Genetics of the resistance to Rift valley fever : Rvfs2 confers tolerance to hepatitis

De Araujo Paredes Batista, Ruben Leandro 25 September 2015 (has links)
La fièvre de la Vallée du Rift (FVR) est une zoonose émergente provoquée par un virus. La FVR affecte principalement le bétail. Chez l'Homme, la maladie peut évoluer sous deux formes mortelles: une fièvre hémorragique et une encéphalite. Malgré l'importance du fonds génétique dans l'issue de la FVR, l'identité des gènes responsables reste inconnue. Nous avons étudié les facteurs génétiques qui déterminent la sensibilité de la lignée de souris MBT/Pas et la résistance de la lignée BALB/c à la FVR. Nous avons identifié trois QTLs sur les chromosomes 2, 5 et 11, nommés, respectivement, Rvfs1, Rvfs3 et Rvfs2. Une infection des lignées congéniques correspondantes, C.MBT Rvfs1, -2 et -3, a confirmé le rôle de la région Rvfs2 dans la sensibilité à la FVR. Une analyse pathophysiologique a montré que les souris C.MBT Rvfs2 et BALB/c développent précocement une hépatite. Les souris C.MBT Rvfs2 meurent de cette hépatite aiguë. En revanche, les souris BALB/c régénèrent leur foie, ce qui leur permet de mieux tolérer l'atteinte du foie. La majorité des souris BALB/c sont décédées plus tard d'une encéphalite. Ces observations montrent que les modèles étudiés reproduisent chacune des deux formes de la maladie observées chez l'Homme. Nous avons produit des lignées sous-congéniques pour la région Rvfs2 et avons testé leur sensibilité à la FVR. Les résultats ont été croisés avec une analyse des variants de structure et de régulation présents dans l'intervalle. Cette stratégie a permis d'identifier 3 gènes candidats : Rnf213, Cd7 et Fasn. La fonction du gène Fasn suggère qu'il puisse jouer un rôle lors de la régénération du foie et ainsi être le facteur génétique que nous recherchons. / Rift Valley fever (RVF) is an emerging zoonosis caused by an arbovirus. The disease affects mainly livestock, but it can have a severe impact on human health. In humans, RVF may progress into fatal outcomes due to acute hepatitis or encephalitis. Despite the influence of the host genetic background on the outcome of the disease, the identity of causative genes remains unknown. We studied the genetic factors determining the susceptibility of MBT/Pas and the resistance of BALB/c mouse strains to RVF. We identified 3 QTLs linked to survival on chromosomes 2, 5 and 11 and named them, respectively, Rvfs1, Rvfs3 and Rvfs2. The infection of the corresponding congenic strains, C.MBT Rvfs1, 2 and 3, confirmed the role of Rvfs2 on the susceptibility to RVF. A pathophysiological investigation showed that both C.MBT Rvfs2 and BALB/c mice exhibit early onset severe hepatitis. However, while C.MBT Rvfs2 died rapidly from liver failure, BALB/c mice tolerated the liver disease and regenerated the hepatic tissue. These mice eventually died at a later stage from encephalitis. These observations indicate that each of the studied mouse models recapitulates one form of the human disease. We generated subcongenic strains harboring the Rvfs2 region and tested their susceptibility to RVF. The results were combined with high-throughput analyses of the structural and regulatory variants found in the region. Our combined approach allowed the identification of three candidate genes: Rnf213, Cd7 and Fasn. The function of the Fasn gene suggests that it could play a role in the mechanism of liver regeneration and, thus, Fasn is our best candidate gene to account for the susceptibility phenotype.
38

Seroprevalence of Rift Valley fever and lumpy skin disease in African buffalo (Syncerus caffer) in the Kruger National and Hluhluwe-iMfolozi Parks, South Africa

Fagbo, Shamsudeen 09 October 2012 (has links)
Lumpy skin disease (LSD) and Rift Valley fever (RVF) are transboundary viral diseases occurring in Africa and the Middle East (e.g. Israel, Saudi Arabia and Yemen) with increasing potential for global spread. Although the role of wildlife in the epidemiology of these diseases is still not clearly understood, the African buffalo (Syncerus caffer) is thought to play a role in the epidemiology of these diseases. This study sought to expand our understanding of the role of buffalo in the maintenance of RVF and LSD by determining seroprevalence to these viral diseases in buffalo during the inter-epidemic period. Lumpy skin disease is endemic in Africa, and has spread to the Middle East (e.g. Israel); consequently there is a high risk of lumpy skin disease virus (LSDV) expanding its geographical distribution to other areas and due to its economic importance it is included in the list of Notifiable Diseases of the World Organization of Animal Health (OIE). The African buffalo is also suspected to play a role in the epidemiology of RVF. Like LSD, RVF was, until recently, only endemic in Africa. However, it spread to the Arabian Peninsula (Saudi Arabia and Yemen) in 2000 exacerbating concerns that it will extend to other regions of the world. Studies have already established that competent mosquito vectors for RVFV exist in North America and other parts of the world. A total of 248 buffalo sera was tested for antibodies to capripoxviruses and neutralising antibodies against LSDV and RVFV using an indirect enzyme-linked immunosorbent assay (I-ELISA) as well as the serum neutralisation test (SNT). The samples were obtained from the Kruger National Park (KNP) and Hluhluwe-iMfolozi Park (HiP) in South Africa. The prevalence of antibodies to LSDV and RVFV in the sera tested was 70/248 (28.2%) and 15/248 (6.1%), respectively using an I-ELISA. The LSDV I-ELISA, using a sheeppox virus as antigen, has not been validated for use in African buffalo. The high percentage of LSDV positive antibody results obtained in this study is however a concern. Results obtained is in contrast with other published results as well as results obtained with the SNT for antibodies against LSDV. The SNT is currently the gold standard for LSDV antibody testing. Using this test for LSDV in this study, 5/66 (7.6 %) samples tested positive. The results of the RVF I-ELISA, which had previously been validated for use in the African buffalo, correlated with the SNT results. From 12 SNT RVFV-positive sera, 3 (25%) had very high SNT titres of 1:640. Neutralising antibody titres of more than 1:80 were found in 80% of the positive sera tested. Eleven buffaloes (4.4% of the total samples) also showed evidence of antibodies to both LSDV and RVFV. The results obtained in this study complement other reports indicating the role of African buffalo in the epidemiology of these diseases during inter-epidemic periods. / Dissertation (MSc)--University of Pretoria, 2012. / Veterinary Tropical Diseases / unrestricted
39

Impulsive Differential Equations with Applications to Infectious Diseases

Miron, Rachelle January 2014 (has links)
Impulsive differential equations are useful for modelling certain biological events. We present three biological applications showing the use of impulsive differential equations in real-world problems. We also look at the effects of stability on a reduced two-dimensional impulsive HIV system. The first application is a system describing HIV induction-maintenance therapy, which shows how the solution to an impulsive system is used in order to find biological results (adherence, etc). A second application is an HIV system describing the interaction between T-cells, virus and drugs. Stability of the system is determined for a fixed drug level in three specific regions: low, intermediate and high drug levels. Numerical simulations show the effects of varying drug levels on the stability of a system by including an impulse. We reduce these two models to a two-dimensional impulsive model. We show analytically the existence and uniqueness of T-periodic solutions, and show how stability changes when varying the immune response rate, the impulses and a certain nonlinear infection term. The third application shows how seasonal changes can be incorporated into an impulsive differential system of Rift Valley Fever, and looks at how stability may differ when impulses are included. The analysis of impulsive differential systems is crucial in developing more realistic mathematical models for infectious diseases.
40

Actinobacterial diversity of the Ethiopian Rift Valley lakes

Du Plessis, Gerda January 2011 (has links)
>Magister Scientiae - MSc / The class Actinobacteria consists of a heterogeneous group of filamentous, Gram-positive bacteria that colonise most terrestrial and aquatic environments. The industrial and biotechnological importance of the secondary metabolites produced by members of this class has propelled it into the forefront of metagenomics studies. The Ethiopian Rift Valley lakes are characterized by several physical extremes, making it a polyextremophilic environment and a possible untapped source of novel actinobacterial species. The aims of the current study were to identify and compare the eubacterial diversity between three geographically divided soda lakes within the ERV focusing on the actinobacterial subpopulation. This was done by means of a culture-dependent (classical culturing) and culture-independent (DGGE and ARDRA) approach. The results indicate that the eubacterial 16S rRNA gene libraries were similar in composition with a predominance of α-Proteobacteria and Firmicutes in all three lakes. Conversely, the actinobacterial 16S rRNA gene libraries were significantly different and could be used to distinguish between sites. The actinobacterial OTUs detected belonged to both the Rubrobacterales and Actinomycetales orders with members of the genus Arthrobacter being found in all three lakes. Geochemical properties were significantly different between the lakes, although more than one property attributed to the variance between community compositions. The diversity detected in the culture-based study differed significantly and all isolates belonged to the genus Streptomyces. Two novel strains were characterized by means of phylogenetic (16S rRNA gene sequence), physiological, morphological and biochemical analyses. Both novel isolates were capable of growing under "extreme" conditions- pH 12, 10% NaCl and 45°C. Partial enzyme characterization revealed that both strains produced xylanase enzymes that were active at pH 6.5 and 8.5 with an increase in activity up to 45°C. The results obtained revealed a previously undetected diversity of actinobacteria in the Ethiopian Rift Valley with a potentially novel subpopulation adapted to haloalkaline conditions. The low 16S rRNA sequence similarity of a substantial proportion of the libraries suggests that culture-based isolation may play a vital role in deciphering the community fingerprint. / The National Research Foundation and the Norwegian Research Council

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