Global ETD Search

61	Giardia CWP2 : determining its immunogenic[i]ty and its potential as a candidate for vaccine against giardiasis Larocque, Renée, 1975- January 2000 (has links) No description available. Protozoan Proteins. Giardiasis -- Immunological aspects. Immunogenetics.
62	Human genetic susceptibility to tuberculosis : the investigation of candidate genes influencing interferon gamma levels and other candidate genes affecting immunological pathways Moller, Marlo 12 1900 (has links) Thesis (PhD (Biomedical Sciences. Molecular Biology and Human Genetics))--University of Stellenbosch, 2007. / The infectious disease tuberculosis (TB) is one of the leading causes of death worldwide. The idea that infectious diseases are the most important driving force in natural selection and that they sustain frequent polymorphisms in the human genome was formally suggested by Haldane in 1949. This hypothesis implicated the human genetic component in the response to infectious disease. Today the involvement of host genetics in TB has been proven unequivocally and, together with environmental factors (e.g. nutrition and crowding) and the causative bacterium, Mycobacterium tuberculosis (M.tuberculosis), may influence the outcome of disease. As is evident, TB is a complex disease and the implication for studying genetic susceptibility is that a number of genes will be involved. Interferon gamma (IFN-7) is the major macrophage-activating cytokine during infection with M.tuberculosis and its role has been well established in animal models and in humans. This cytokine is produced by activated T helper 1 (Th1) cells. These Th1 responses can best deal with intracellular pathogens such as M.tuberculosis. We selected twelve candidate genes based on the hypothesis that genes which regulate the production of IFN-7 may influence TB susceptibility. We also selected polymorphisms from 27 other candidate genes, which may affect immunological pathways involved in TB, to investigate as susceptibility factors based on the following hypotheses: 1) granulomatous diseases can share susceptibility genes; 2) gene expression studies done by DNA-array analysis experiments may reveal TB susceptibility genes; 3) genomewide linkage studies in TB can determine susceptibility loci and genes in this region are possibly susceptibility factors; and 4) functional susceptibility polymorphisms in genes involved in immune-mediated diseases other than TB may contribute to susceptibility to TB. This research tested the association of 136 genetic polymorphisms in 39 potentially important genes with TB in the South African Coloured population. Well-designed case-control association studies were used and we attempted to replicate these findings in an independent sample set using family-based case-control designs (transmission disequilibrium tests (TDTs)). In addition, haplotypes and linkage disequilibrium (LD) in the candidate genes were also investigated. During the case-control analyses we found significant associations for 6 single nucleotide polymorphisms (SNPs) in the following genes: SH2 domain protein 1A, tolllike receptor 2, class II major histocompatibility complex transactivator, interleukin 1 receptor antagonist, runt-related transcription factor 1 and tumour necrosis factor superfamily, member 1B. Discrepant results were obtained during the TDT analyses. The number of families available was small and for this reason we cannot conclude that the case-control results were spurious. We also tested the association of haplotypes with TB. Haplotypes in the interleukin 12, beta (IL12B) and toll-like receptor 4 genes were nominally associated with TB in both the case-control and TDT analyses. We observed strong LD for the genes in the South African Coloured population. In total 17 novel SNPs were identified and one novel allele was found for a microsatellite in IL12B. This research contributes to the increasing amount of information available on genes involved in TB susceptibility, which in the future may help to predict high risk individuals. Tuberculosis Immunogenetics Genetic aspects of Tuberculosis Immunogenetics
63	Mutagenized HLA DNA Constructs: Tools for Validating Molecular HLA Typing Methodologies Schulte, Kathleen Q. 05 1900 (has links) This study describes the development and validation of mutagenized cloned DNA constructs, which correspond to the polymorphic regions of the class II region of the HLA complex. The constructs were used to verify the allelic specificity of primers and probes in polymerase chain reaction (PCR)-based HLA typing assays such as Sequence Specific Primers (SSP) and Sequence Specific Oligonucleotide Probes (SSOP). The constructs consisted of the entire polymorphic region of exon 2 of class II HLA allele sequences that included primer annealing sites or probe hybridization sites. An HLA allele sequence was inserted into a plasmid, cloned, then mutagenized to match a specific HLA allele, and finally, the correct clone was verified by bidirectional sequencing of the insert. Thus, the construct created a cloned reference DNA sample for any specific allele, and can be used to validate the accuracy of various molecular methodologies. DNA analysis HLA allele sequences immunogenetics alleles HLA histocompatibility antigens. DNA -- Analysis. Immunogenetics.
64	Immune regulation in response to mycobacterial infection Cheung, Ka-wa, Benny, 張嘉華 January 2007 (has links) published_or_final_version / abstract / Paediatrics and Adolescent Medicine / Doctoral / Doctor of Philosophy HIV (Viruses) Immunogenetics. Tuberculosis.
65	Defeitos genético-moleculares e aspectos clínicos de pacientes com síndrome de hiper IgM autossômica. / Molecular-genetic defects and clinical spectrum of autosomal hyper IgM syndrome in Brazilian patients. Klaver, Stefanie Gomes 09 September 2011 (has links) A síndrome de HIGM é uma imunodeficiência, caracterizada por níveis séricos normais ou elevados de IgM associados com baixos níveis de IgG, IgA e IgE. Neste estudo investigamos pacientes com HIGM autossômico recessivo. Selecionamos 15 pacientes com diagnóstico clínico sugestivo de AR-HIGM, 10 do sexo feminino, 05 do sexo masculino, onde onze são brasileiros, um é francês e três são turcos, com idades que variam de 2 a 40 anos. Todos os pacientes apresentam infecções recorrentes: 100% pneumonias, 80% otites médias agudas, 53% sinusites, 46% amigdalites, 40% diarréias 26% infecções urinárias, uma apresentou micobacteriose cutânea. Encontramos as seguintes mutações no gene AICDA: Pacientes EJ e GF, mutação missense na base 260 do cDNA (c.260G>C; p. Cys87Ser). Pacientes DA e RC apresentam defeito de splice, acarretando na deleção total do exon 4 do gene AICDA. Os pacientes estrangeiros foram previamente estudados para os genes AICDA, UNG e CD40, e nenhuma alteração foi encontrada. Neste caso, estudamos o gene INO80, e encontramos nos exons 04 (g.24012 G>A) e 26 (g.99976 G>T) do gene INO80, duas mutações missense em heterozigose no DNAg do paciente OD. O estudo molecular e genético é importante para a realização do diagnóstico diferencial, estratégia terapêutica e prognóstico dos casos. / HIGM syndrome is a rare immunodeficiency characterized by high or normal levels of serum IgM associated with low levels of IgG, IgA and IgE. We selected 15 patients with clinical diagnosis suggestive of AR-HIGM, 10 females, 05 males, where 11 are Brazilian, one is French and three are Turkish, with ages ranging from 2 to 40 years. All patients had recurrent infections: 100% pneumonia, 80% acute otitis media, 53% sinusitis, 46% tonsillitis, 40% recurrent diarrhea, 26% urinary tract infections, 20% stomatitis, and one patient presented a cutaneous mycobacteriosis. 20% of the patients had opportunistic infections: Mycobacterium marinum, Toxoplasma gondii, varicella-zoster virus, Pseudomonas aeruginosa, fungus, and Mycobacterium tuberculosis. As a result, we found two types of mutations in 4 diferent patients with no consanguinity. We found in AICDA gene the following mutations: Patients EJ and GF missense mutation in base 260 in cDNA, which results in a change of aminoacid (c.260G> C; Cys87Ser p.). Patients DA and RC showed a splice defect, resulting in a complete deletion of exon 4 in AICDA gene. All other patients were sequenced for AICDA, UNG and CD40 genes, and no changes were found. In this case, we studied the INO80 gene, and we found in exons 04 (g.24012 G> A) and 26 (g.99976 G> T) INO80 gene, two heterozygous missense mutations in DNAg of patient OD. Since these molecular genetic defects result in similar clinical features, molecular and genetic studies are important for the differential diagnosis, therapeutic strategy and prognosis of the cases. Genetic mutation Genética molecular Immunogenetics Imunogenética Molecular genetics Mutação genética
66	Papel da Arg127 na conformação estrutural e secreção de Fator H, importante proteína reguladora da via alternativa do sistema complemento / Role of Arg127 for complement regulatory Factor H structural conformation and secretion. Albuquerque, José Antonio Tavares de 13 September 2011 (has links) A Via Alternativa é a principal via de ativação do sistema complemento (SC), sendo o Fator H (FH) um de seus principais reguladores. No presente estudo, nós investigamos os mecanismos moleculares pelo qual o paciente com a mutação Arg127His no FH possui deficiência do SC. Para isto, utilizamos fibroblastos de paciente e individuo normal estimulados com IFN-<font face=\"Symbol\">g e verificamos que as células do paciente eram capazes de produzir FH, contudo a maior parte das proteínas estava retida no retículo endoplasmático (RE). Em paralelo, transfectamos células Cos-7 com plasmídeos contendo a mutação CG453T<font face=\"Symbol\">® CA453T e observamos que a mutação foi responsável pelo retardo na secreção de FH. Apesar da mutação reduzir a secreção de FH, observamos que a capacidade de FH atuar como co-factor não foi afetada. Assim, avaliamos se o uso de chaperonas químicas poderia induzir a secreção da proteína e observamos que houve aumento na secreção de FH nos fibroblastos. Desta forma, propomos o uso desses fármacos como alternativa de tratamento para melhorar a sobrevida do paciente. / Factor H (FH) is one of the most important regulatory proteins of the alternative pathway of the complement system (CS). In this study, we investigated the consequences of FH Arg127His mutation to the secretion ratio of this protein by skin fibroblasts in vitro. We stimulated the FH synthesis from patient and normal control with IFN<font face=\"Symbol\">g when we observed that the patient cells were able to synthetize FH, however this mutant protein was mainly retained at the endoplasmic reticulum. In parallel, we transfected Cos-7 cells with plasmids containing CG453T<font face=\"Symbol\">® CA453T mutation and observed that the mutation was responsible for the delay in the FH secretion. Although the mutation reduced the FH secretion, we observed that the FH function was not affected. Thus, we evaluated whether the treatment with chemical chaperones could release FH to the culture supernant. We observed that patients fibroblasts treated increased the secretion of FH. In conclusion, we suggest the use of these chemical chaperones as a potential alternative therapeutic to improve the patients survival. Cell immunology Immunogenetics Imunogenética Imunologia celular Imunologia médica Medical immunology
67	Characterization of the MHC II B of the bald eagle Unknown Date (has links) The Major Histocompatibility Complex class II B (MHC II B) gene encodes a protein that is part of the adaptive immune system and critical for the non-self recognition ability of immune cells. This gene has been characterized in the Bald Eagle, ten unique alleles were found in two subpopulations at the geographic extremes of the range margins. Geographic genetic variation is suggested by the presence of population specific alleles. The results showed considerable divergence of groups of Bald Eagle alleles when compared to alleles from other birds of prey. Particular codons within the exon II show signs of balancing selection driving the evolution of the MHC II B. Transcription data showed statistically significant differential expression of alleles. This can be interpreted as meaning a particular locus is being preferentially expressed in blood. The analysis of the polymorphism of this adaptive marker may aid managers of wildlife during this age of global climate change and the biodiversity crisis. / by Andrew Smith. / Thesis (M.S.)--Florida Atlantic University, 2010. / Includes bibliography. / Electronic reproduction. Boca Raton, Fla., 2010. Mode of access: World Wide Web. Major histocompatibility complex Cellular signal transduction Immunogenetics Genetic polymorphisms
68	Factors affecting the immunogenicity and protective efficacy of routine childhood immunisations Boros, Christina Ann. January 2001 (has links) (PDF) Includes list of publications arising from the thesis. Bibliography: leaves 327-341. Examines the effect of adverse storage on the immunogenicity of pertussis, diphtheria and tetanus vaccines, the protective efficacy of pertussis vaccines and the effect of premature birth on antibody response to routine childhood immunisations. Immunogenetics Vaccination of infants Evaluation Vaccines Storage Vaccines Effectiveness
69	Factors affecting the immunogenicity and protective efficacy of routine childhood immunisations / Christina Ann Boros. Boros, Christina Ann January 2001 (has links) Includes list of publications arising from the thesis. / Bibliography: leaves 327-341. / 341, [15] leaves : ill. (some col.) ; 30 cm. / Title page, contents and abstract only. The complete thesis in print form is available from the University Library. / Examines the effect of adverse storage on the immunogenicity of pertussis, diphtheria and tetanus vaccines, the protective efficacy of pertussis vaccines and the effect of premature birth on antibody response to routine childhood immunisations. / Thesis (Ph.D.)--University of Adelaide, Dept. of Paediatrics, 2002? Immunogenetics. Vaccination of infants Evaluation. Vaccines Storage. Vaccines Effectiveness.
70	Organization of the class I region of the bovine major histocompatibility complex (BoLA) and the characterization of a class I frameshift deletion (BoLA-Adel) prevalent in feral bovids Ramlachan, Nicole 12 April 2006 (has links) The major histocompatibility complex (MHC) is a genomic region containing genes of immunomodulatory importance. MHC class I genes encode cell-surface glycoproteins that present peptides to circulating T cells, playing a key role in recognition of self and non-self. Studies of MHC loci in vertebrates have examined levels of polymorphism and molecular evolutionary processes generating diversity. The bovine MHC (BoLA) has been associated with disease susceptibility, resistance and progression. To delineate mechanisms by which MHC class I genes evolved to function optimally in a species like cattle, it is necessary to study genomic organization of BoLA to define gene content, and investigate characteristics of expressed class I molecules. This study describes development of a physical map of BoLA class I region derived from screening two BAC libraries, isolating positive clones and confirming gene content, order and chromosomal location through PCR, novel BAC end sequencing techniques, and selected BAC shotgun cloning and/or sequencing and FISH analysis. To date, this is the most complete ordered BAC array encompassing the BoLA class I region from the class III boundary to the extended class I region. Characterization of a frameshift allele exhibiting trans-species polymorphism in Bos and Bison by flow cytometry, real-time RT-PCR, 1D and 2D gel analysis is also described. This frameshift allele encodes an early termination signal within the antigen recognition site (ARS) of exon 3 of the BoLA BSA-Adel class I gene predicting a truncated class I protein that is soluble. An ability to assess MHC diversity in populations and provision of animals with defined MHC haplotypes and genetic content for experimental research is necessary in developing a basis upon which to build functional studies to elucidate associations between haplotype and disease in bovids. The BoLA class I region is immunologically important for disease association studies in an economically important species. This study provides knowledge of gene content and organization within the class I MHC region in cattle, providing a template for more detailed analysis and elucidation of complex disease associations through functional genomics and comparative analysis, as well as evolution of the MHC in bovids to optimize a populationÂs immune response. MHC BoLA class I immunogenetics comparative genomics bovine

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