Loop-mediated isothermal amplification for the detection of HLA B*58:01 associated allopurinol hypersensitivity

Kwong, Ka-man., 鄺嘉敏.

January 2011

published_or_final_version / Pathology / Master / Master of Medical Sciences

Gene amplification.

Drug allergy - Genetic aspects.

The genetics of atopy and atopic asthma

Cookson, William Osmond Charles Michael

January 1994

No description available.

616.2

Identification of novel genes associated with allergen-driven T cell activation in human atopics

Bosco, Anthony

January 2007

[ Truncated abstract ] Atopic diseases such as asthma are thought to be driven to a significant extent by T helper memory cells which are programmed to respond in a harmful way to environmental allergens (e.g. house dust mite). Previous studies in humans and in animal models have established that activation of TH2 cytokine genes in T memory responses to allergens is central to the disease process. However, only a subset of atopics harbouring a TH2-memory response phenotype manifests clinical symptoms of disease. Moreover, clinical trials with TH2 antagonists in atopic patients have proven disappointing, suggesting underlying complexities in disease pathogenesis which escape regulation via these approaches. It was thus hypothesised that additional genes involved in the activation program of allergen-specific T memory cells which are central to disease pathogenesis remain unidentified. The aim of the current study was to identify such novel genes by applying microarray technology to survey genome-wide expression patterns in an in vitro model of allergen-driven human T cell activation. In contrast to previous human microarray studies in this area focusing on mitogen activated T cell lines and clones, the current study avoided the use of strong activation stimuli which have the potential to distort patterns of gene expression, and reports for the first time the findings of microarray analysis of house dust mite allergen-driven acute gene activation in recirculating T memory cells harvested from the peripheral blood of human atopics. ... Finally, methodology was established to investigate the function of the novel atopy-associated genes. In loss-of-function experiments, expression of DACT1 and CAMK2D was silenced in primary T cell responses driven by bacterial superantigens, a model system for studying T cell responses under conditions which mimic antigen-specific activation. Whilst silencing DACT1 and CAMK2D expression did not influence classical readouts of T cell function including proliferation and cytokine production, microarray profiling was employed to identify putative downstream transcriptional targets of each gene. The experimental strategy and optimised methodology presented herein can now be employed to investigate the molecular circuitry linking the novel atopy-associated genes to the T cell activation process. In conclusion, several novel genes associated with allergen-driven T memory responses in atopics have been first described in this thesis and represent logical candidates for more detailed immunological and genetic studies related to the pathogenesis of atopic diseases.

T cells

Asthma -- Genetic aspects

Allergy -- Genetic aspects

Microarray

Allergy

T cell

Asthma

The relationship between allergic diseases and vitamin D pathway genes and serum vitamin D levels in Chinese children. / 過敏性疾病與維生素D路徑的基因及血清維生素D水平之間的關係 / CUHK electronic theses & dissertations collection / Guo min xing ji bing yu wei sheng su D lu jing de ji yin ji xue qing wei sheng su D shui ping zhi jian de guan xi

January 2013

Wang, Shuxin. / Thesis (Ph.D.)--Chinese University of Hong Kong, 2013. / Includes bibliographical references (leaves 191-212). / Electronic reproduction. Hong Kong : Chinese University of Hong Kong, [2012] System requirements: Adobe Acrobat Reader. Available via World Wide Web. / Abstracts also in Chinese; appendixes includes Chinese.

Allergy--Genetic aspects

Asthma--Genetic aspects

Eczema in children

Vitamin D

Hypersensitivity--genetics

Asthma--genetics

Eczema--genetics

Infant

Child

Vitamin D