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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.
1

Assessment of the Functional Role of the NTR Domain of Complement Component C3 using a Homologous Dmain Exchange Approach

Rana, Amardeep 13 January 2011 (has links)
The complement system plays an important role in innate and adaptive immunity. Central to all complement activities is the function of complement component 3 (C3). C3 contains a C-terminal extension of ~150 residues known as the NTR (or C345C) domain. To address the role of the NTR domain in binding and functional activities of C3, a C3/C5 chimera was engineered, in which the NTR domain of C3 was replaced by the homologous domain of the closely related protein C5. Functionally, the C3(C5NTR) was devoid of classical pathway-dependent hemolytic activity and deficient in factor H- and CR1-dependent factor I cleavability. Direct binding SPR assays, using chip bound methylamine treated His6-tagged C3(C5NTR), showed a complete loss of C5 binding while retaining wild type binding with CR1, factor H and factor B. These results present the first evidence for a major C5 binding site within C3 NTR.
2

Assessment of the Functional Role of the NTR Domain of Complement Component C3 using a Homologous Dmain Exchange Approach

Rana, Amardeep 13 January 2011 (has links)
The complement system plays an important role in innate and adaptive immunity. Central to all complement activities is the function of complement component 3 (C3). C3 contains a C-terminal extension of ~150 residues known as the NTR (or C345C) domain. To address the role of the NTR domain in binding and functional activities of C3, a C3/C5 chimera was engineered, in which the NTR domain of C3 was replaced by the homologous domain of the closely related protein C5. Functionally, the C3(C5NTR) was devoid of classical pathway-dependent hemolytic activity and deficient in factor H- and CR1-dependent factor I cleavability. Direct binding SPR assays, using chip bound methylamine treated His6-tagged C3(C5NTR), showed a complete loss of C5 binding while retaining wild type binding with CR1, factor H and factor B. These results present the first evidence for a major C5 binding site within C3 NTR.
3

THE ANCIENT KEMETIC WORLDVIEW AND SELF-LIBERATION: MDW NTR AND SEEING WITH SIA

Tisdale, Stephanie Joy January 2013 (has links)
As the direct descendants of the first human beings, African people are the supreme witnesses of Creation itself, and senior authorities regarding the earthly Creations. African people bear supreme witness to humanity, and the most effective methods of being human: the biology and chemistry of life, the physiological and metaphysical aspects of earthly existence, and the science of the cosmic Creations--observing all that is above and what exists there, beyond the sky. By definition humanity is African: the first human beings were African and the first defining innovations of humanity were birthed in Africa. Since history is necessarily a study of the origins of humanity, and the first humans were African, history then must initiate at the emergence of humankind, which took place in Africa. The records left and maintained by the oldest humans on earth--written, memorized, or otherwise--provide amazing clues as to the initial Creation and subsequent development of humankind. As each successive generation works to strengthen the collective memory of their own people's past before conquer, the struggle to remember memories and to keep traditions intact becomes even more evident. As with every epic turn of events, the conquered are forced to decide if they will remain as such or not. This paper explores the ways in which the African worldview provides a critical and otherwise impossible analysis of human history, by exploring the oldest contributions of the first human beings--who were African. I argue that the ancient Kemetic worldview--Mdw Ntr--provides a prototypical blueprint for every African's self-liberation, creating a context through which contemporary freedom struggles can ultimately be assessed and achieved. In particular, this paper examines how the ancient Kemetic worldview has, since its inception, presented a working method of thinking and doing--seeing with Sia--which not only inspired successive African generations, but also the freedom struggles of contemporary African communities. Mdw Ntr is both a theory and a methodology: it encompasses a way of seeing reality, while also providing exact methods for how to go about this process. I propose that the notion of Sia--or "exceptional clarity"--is an actionable blueprint exemplified in the Shabaka Text and The Great Hymn to Aten. Both texts provide a methodology for achieving Sia; both texts speak to the fundamental processes of Mdw Ntr; and both texts exhibit a working model for self-liberation through the ancient Kemetic worldview. In order for human beings to manifest power--to be empowered--they must ultimately think with "exceptional clarity" and speak their intentions into existence. To be effective, one cannot speak without thinking, or do without first thinking and speaking. According to the ancient Kemites, thinking is the first step in speaking and also doing. Thinking initiates all actions: the more exceptional the clarity, the better. Hence, self-liberation emerges and subsequently, the collective liberation of African people. / African American Studies
4

Investigation into Catalytic Metallodrugs that Target Hepatitis C IRES RNA: Development, Characterization, and Mechanism

Ross, Martin James January 2015 (has links)
No description available.
5

Genes do metabolismo do nitrogênio e suas implicações na patogenicidade e virulência da Xanthomonas citri subsp. citri / Genes of nitrogen metabolism and its implications in the pathogenicity and virulence of Xanthomonas citri subsp. citri

Amorim, Julie Anne Espíndola 27 April 2018 (has links)
Submitted by JULIE ANNE ESPÍNDOLA AMORIM (julie__anne@hotmail.com) on 2018-06-05T18:33:56Z No. of bitstreams: 1 Tese_23-03-18-final_corrigida_05-06-2018_Juliecorrigidapdf.pdf: 3073465 bytes, checksum: 1673cd431dca7fe8472ab9ce8185182f (MD5) / Approved for entry into archive by Alexandra Maria Donadon Lusser Segali null (alexmar@fcav.unesp.br) on 2018-06-05T18:59:54Z (GMT) No. of bitstreams: 1 amorim_jae_dr_jabo.pdf: 3073465 bytes, checksum: 1673cd431dca7fe8472ab9ce8185182f (MD5) / Made available in DSpace on 2018-06-05T18:59:54Z (GMT). No. of bitstreams: 1 amorim_jae_dr_jabo.pdf: 3073465 bytes, checksum: 1673cd431dca7fe8472ab9ce8185182f (MD5) Previous issue date: 2018-04-27 / Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES) / O cancro cítrico tipo A, causado pela bactéria Xanthomonas citri subsp. citri (XccA), é uma das doenças de citros mais importantes, afetando todas as cultivares comerciais, para a qual não existem ainda estratégias de controle eficientes. Os genes ntrB e ntrC codificam, respectivamente, a histidina quinase (HK) e o regulador de respostas (RR), pertencentes a um sistema de dois componentes (TCSs), que atuam no sistema regulador de nitrogênio (NTR). Porém, o possível papel desses genes na virulência da XccA e de outros fitopatógenos ainda não foi elucidado. Este estudo teve como objetivo investigar os efeitos dos genes ntrB e ntrC no desenvolvimento do cancro cítrico em limão-cravo (Citrus limonia Osbeck), bem como a possível relação desses genes com a regulação da expressão de genes do sistema de secreção tipo 3 (SST3), considerado um dos principais fatores de virulência da XccA. Os mutantes ΔntrB e ΔntrC foram obtidos pela técnica de mutagênese sítio-dirigida por reação em cadeia da polimerase de extensão por sobreposição. A mutação dos genes causou redução na sintomatologia do cancro cítrico e diminuição da população bacteriana no espaço intercelular do tecido foliar da planta. A análise das curvas de crescimento in vitro revelou que a ausência do gene ntrB não alterou a viabilidade da bactéria, enquanto a mutação do gene ntrC afetou o “fitness” bacteriano em meio de cultura NB. Análises in vitro indicaram que o mutante ΔntrC formou duas vezes mais biofilme e produziu cinco vezes mais goma xantana do que a XccA 306 in vitro. A expressão dos genes (hpa1, hrpG, hrpX, hrpE, hrpW e hrpD6) do SST3 avaliados foi significativamente maior (p < 0,05) no mutante ΔntrC do que na XccA 306 e no ΔntrB, indicando que ntrC possa atuar na regulação do SST3. Porém, o nível de expressão desses genes no mutante ΔntrB não apresentou diferença significativa (p > 0,05) em relação à XccA 306. A modelagem molecular revelou semelhança estrutural entre as regiões receptoras de NtrC e HrpG, sugerindo que a fosforilação de HrpG por NtrB possa ocorrer in vivo. Em síntese, os resultados obtidos neste estudo indicam que a mutação dos genes ntrB e ntrC afeta o desenvolvimento do cancro cítrico em limão-cravo e que o gene ntrC pode atuar na regulação dos mecanismos de formação de biofilme, produção de goma xantana e expressão de genes do SST3 e/ou que a ausência desse gene ocasione um desequilíbrio celular na XccA 306, resultando na alteração desses mecanismos, enquanto NtrB pode apresentar papel na regulação de genes do SST3 por meio da fosforilação de HrpG. / The citrus canker type A, provoked by the bacterium Xanthomonas citri subsp. citri (XccA), is one of themost important citrus diseases, affecting all the commercial cultivars, for which there are no effective control strategies. The ntrB and ntrC genes encode a histidine kinase (HK) and the response regulator (RR), respectively, belong to a two-component system (TCSs), related to the nitrogen regulatory system (NTR). However, the possible role of ntrB and ntrC genes in the virulence of XccA and other phytopathogens has not yet been elucidated. Therefore, the aim of this study was to investigate the impact of the ntrB and ntrC genes on the development of citrus canker in rangpur lime (Citrus limonia Osbeck), as well as the possible relation of ntrB and ntrC genes with the regulation of the type 3 secretion system (T3SS) gene expression, which is considered one of the main virulence factors of XccA. The ΔntrB and ΔntrC were obtained by site-directed mutagenesis through overlap extension polymerase chain reaction. The mutation of the ntrB and ntrC genes caused a reduction of the citrus canker symptoms, and decrease of the bacterial population in the intracellular space of the foliar tissue of the plant. In vitro growth curves analysis revealed that the ΔntrB did not affect the viability of the bacterium, whereas the ΔntrC affected the bacterial fitness in NB culture medium. In vitro analysis indicated that the ΔntrC formed 2x more biofilm, and produced 5x xanthan gum compared to the XccA 306. The T3SS related genes (hpa1, hrpG, hrpX, hrpE, hrpW and hrpD6) expression was significantly higher (p <0.05) in the ΔntrC than in the XccA 306 and the ΔntrB, indicating that ntrC can modulate the regulation of T3SS. However, the level of expression of these genes in the ΔntrB did not differ (p> 0.05) in relation to the XccA 306. Molecular modeling revealed structural similarity between NtrC and HrpG receptors motifs, suggesting that phosphorylation of HrpG by NtrB may occur in vivo. Overall, the results obtained in this study strongly suggest that the mutation of the ntrB and ntrC genes affect the development of rangpur lime citrus canker and that ntrC gene may play an important role in the regulation of the mechanisms of biofilm formation, xanthan gum production and T3SS gene expression and/or that the absence of this gene causes a cellular imbalance in XccA 306 resulting in the alteration of these mechanism, whereas the NtrB may have a role with the regulation of T3SS genes by phosphorylation of HrpG. / 3385/2013
6

Usagères des nouvelles technologies de la reproduction dans un contexte de communauté virtuelle

Dupiech, Sophie January 2004 (has links)
Mémoire numérisé par la Direction des bibliothèques de l'Université de Montréal.
7

Nitroaromatic pro-drug activation and resistance in the African trypanosome

Sokolova, Antoaneta Y. January 2011 (has links)
Sleeping sickness, caused by Trypanosoma brucei, is a deadly disease that affects some of the poorest countries in sub-Saharan Africa. Although the disease prevalence is declining, strengthening of the current control efforts, including introduction of more adequate chemotherapeutic options, is needed to prevent the re-emergence of yet another epidemic. Nitroaromatic compounds, such as nifurtimox (in combination with eflornithine) and fexinidazole (in clinical trials), have been recently introduced for the treatment of the second stage of sleeping sickness. These compounds are believed to act as pro-drugs that require intracellular enzymatic activation for antimicrobial activity. Here, the role of the bacterial-like nitroreductase TbNTR as a nitrodrug activating enzyme is examined through overexpression and knock-out studies in T. brucei. Multiple attempts to purify soluble recombinant TbNTR from E. coli were unsuccessful, because the recombinant protein was found to be membrane associated. In keeping with the role of TbNTR in nitrodrug activation, loss of an NTR gene copy in T. brucei was found to be one, but not the only, mechanism that may lead to nitrodrug resistance. Furthermore, in the bloodstream form of T. brucei, resistance was relatively easy to select for nifurtimox, with no concurrent loss of virulence and at clinically relevant levels. More worryingly, nifurtimox resistance led to a decreased sensitivity of these parasites to other nitroaromatic compounds, including a high level of cross-resistance to fexinidazole. Conversely, generation of fexinidazole resistance resulted in cross-resistance to nifurtimox. Should these findings translate to the field, emerging nitrodrug resistance could reverse all recent advances in the treatment of sleeping sickness, made since the introduction of eflornithine 20 years ago. Therefore, all efforts should be made to ensure nitroaromatic drugs are used only in drug combination therapies against sleeping sickness, in order to protect them from emerging resistance.
8

Characterization of the thioredoxin system in Methanosarcina mazei

Loganathan, Usha R. 18 December 2014 (has links)
Thioredoxin (Trx) and thioredoxin reductase (TrxR) along with an electron donor form a thioredoxin system. Such systems are widely distributed among the organisms belonging to the three domains of life. It is one of the major disulfide reducing systems, which provides electrons to several enzymes, such as ribonucleotide reductase, methionine sulfoxide reductase and glutathione peroxidase to name a few. It also plays an important role in combating oxidative stress and redox regulation of metabolism. Trx is a small redox protein, about 12 kDa in size, with an active site motif of Cys-X-X-Cys. The reduction of the disulfide in Trx is catalyzed by TrxR. Two types of thioredoxin reductases are known, namely NADPH thioredoxin reductase (NTR) with NADPH as the electron donor and ferredoxin thioredxoin reductase (FTR) which depends on reduced ferredoxin as electron donor. Although NTR is widely distributed in the three domains of life, it is absent in some archaea, whereas FTRs are mostly found in plants, photosynthetic eukaryotes, cyanobacteria, and some archaea. The thioredoxin system has been well studied in plants, mammals, and a few bacteria, but not much is known about the archaeal thioredoxin system. Our laboratory has been studying the thioredoxin systems of methanogenic archaea, and a major focus has been on Methanocaldococcus jannaschii, a deeply rooted archaeon that has two Trxs and one TrxR. My thesis research concerns the thioredoxin system of the late evolving members of the group which are exposed to oxygen more frequently than the deeply rooted members of the group, and have several Trxs and TrxRs. Methanosarcina mazei is one such organism, whose thioredoxin system is composed of one NTR, two FTRs, and five Trx homologs. Characterization of the components of a thioredoxin system sets the basis to further explore its function. I have expressed in Escherichia coli and purified the five Trxs and three TrxRs of M. mazei. I have shown the disulfide reductase activities in MM_Trx1 and MM_Trx5 by their ability to reduce insulin with DTT as the electron donor, and that in MM_Trx3 through the reduction of DTNB by this protein with NADPH as the electron donor, and in the presence of NTR as the enzyme. MM_Trx3 was found to be the only M. mazei thioredoxin to accept electrons through the NTR, and to form a complete Trx - NTR system. The Trx - FTR systems are well studied in plants, and such a system is yet to be defined in archaea. I have proposed a mechanism of action for one of the FTRs. FTR2 harbors a rubredoxin domain, and this unit is the only rubredoxin in this organism. Superoxide reductase, an enzyme that reduces superoxide radical to hydrogen peroxide without forming oxygen, utilizes rubredoxin as the direct electron source and this enzyme is found in certain anaerobes, including Methanosarcina species. Thus, it is possible that FTR2 provides electrons via a Trx to the superoxide reductase of M. mazei. This activity will define FTR2 as a tool in combating oxidative stress in M. mazei. In my thesis research I have laid a foundation to understand a complex thioredoxin system of M. mazei, to find the role of each Trx and TrxR, and to explore their involvement in oxidative stress and redox regulation. / Master of Science
9

Die regulatorischen Funktionen des paralogen Phosphotransferase Systems (PTSNtr) in Escherichia coli. / The regulatory functions of the nitrogen-related phosphotransferase system, PTS(Ntr) in Escherichia coli

Lüttmann, Denise 25 January 2012 (has links)
No description available.

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