Genetic testing in the age of anxiety. From rhetoric to narrative.

Leontini, Rose, School of Sociology, UNSW

January 2005

The debate on genetic testing for Huntington???s disease has been dominated heavily by the bioethical and biomedical discourses. Yet upon analysis, both discourses are highly inadequate for understanding the complexity of the difficult choices people are faced with, and the inter-personal relations that are central to decisions regarding the uptake of genetic tests. The purpose of this thesis is two-fold. Firstly, to conduct a theoretically-informed critical analysis of the existing bioethical discourse on genetic testing for Huntington???s disease, that draws primarily on the work of contemporary feminist thinkers. Secondly, to explore how people with a genetic risk for Huntington???s disease negotiate the available choices between certainty and uncertainty; how they experience the liminality of ???being at risk??? in everyday life; how they manage their social environments; and how they interpret their own situation. The matter of ???choice??? is heightened because of the ready availability of genetic testing for Huntington???s disease, and the moral rhetoric that accompanies the provision of genetic services. Empirically, the research draws on the narratives by eleven people with a family history of Huntington???s disease, through which they discuss their fears of living in the shadow of the fatal disease, and consider their choices on reproduction and genetic testing. Their narratives will be analysed through the work of Foucault and Goffman, as well as a wide range of contemporary sociologists.The thesis being proposed is that decisions on genetic testing cannot be said to be ???individual???, but are instead dispersed among the social relations between the self and others, reflecting and transforming the values, competing desires, and the discourses that are prevalent in their social worlds. This is achieved through the discursive production of a web of narratives through which both individuals and institutions attempt to govern, with varying degrees of success, the implications of this relatively new field of knowledge.

Huntington's chorea -- Genetic aspects

Optimizing expression of recombinant porcine growth hormone in E. coli / by Carol Senn.

Senn, Carol

January 1995

Bibliography: leaves 239-259. / 259 leaves : ill. ; 30 cm. / Title page, contents and abstract only. The complete thesis in print form is available from the University Library. / Concentrations of minimal medium components and fermentation parameters were optimized for high level constituitive expression of recombinant methionyl porcine growth hormone in E. coli. Improved yields were obtained when the magnesium concentration was reduced, and the ammonium chloride concentration increased. / Thesis (Ph.D.)--University of Adelaide, Dept. of Biochemistry, 1995

Porcine somatotropin Genetic aspects.

Molecular genetics of epilepsy / by Robyn Wallace.

Wallace, Robyn, 1967-

January 1997

Errata pasted onto back end-paper. / Copies of author's previously published articles inserted. / Bibliography : leaves 157-176. / viii, 176, [62] leaves : ill. (col.) ; 30 cm. / Title page, contents and abstract only. The complete thesis in print form is available from the University Library. / Thesis (Ph.D.)--University of Adelaide, Dept. of Paediatrics, 1997

Epilepsy Genetic aspects.

Genetic localisation and molecular characterisation of genes for inherited ataxias / Kathryn Louise Friend.

Friend, Kathryn L.

January 2000

Copy of author's previously published work inserted. / Bibliography: leaves 193-216. / ix, 268 leaves : ill. ; 30 cm. / Title page, contents and abstract only. The complete thesis in print form is available from the University Library. / Thesis which examines in detail the genetics of congental ataxias, and early and late onset ataxias. / Thesis (Ph.D.)--University of Adelaide, Dept. of Paediatrics, 2000

Ataxia Genetic aspects.

Optimizing expression of recombinant porcine growth hormone in E. coli / by Carol Senn.

Senn, Carol

January 1995

Bibliography: leaves 239-259. / 259 leaves : ill. ; 30 cm. / Title page, contents and abstract only. The complete thesis in print form is available from the University Library. / Concentrations of minimal medium components and fermentation parameters were optimized for high level constituitive expression of recombinant methionyl porcine growth hormone in E. coli. Improved yields were obtained when the magnesium concentration was reduced, and the ammonium chloride concentration increased. / Thesis (Ph.D.)--University of Adelaide, Dept. of Biochemistry, 1995

Porcine somatotropin Genetic aspects.

Exploring the Genetics Regulating Kidney Function

Sheehan, Susan

January 2007

No description available.

Kidneys -- Diseases -- Genetic aspects

Mutagenesis and antimutagenesis in Big Blue ® lacI transgenic rats

Yang, Haiyan

23 October 2018

The initiation of the cancer process is associated with mutations. Analysis of environmental exposure to chemical or physical agents causing these genetic alterations is of great importance in order to develop strategies for avoiding or reducing cancer risk in humans. The causality between mutagenesis and carcinogenesis also prompts the concept that the modifying effect on mutagenesis by a compound would be predictive of the cancer preventive potential of that compound. The Big Blue© transgenic assay, using the E. coli lacI gene as the mutational target provides an opportunity to evaluate mutagenesis and its modulation m vivo. This model system was used to study the tissue-specific effect of the potential chemopreventive agent conjugated linoleic acid (CLA), on the mutagenicity of the suspected human carcinogen, 2-amino-1 -methyl-6- phenylimidazo[4,5-b]pyridine (PhIP). PhIP and CLA were selected for study since both compounds are consumed by humans on a daily basis, and are suspected to be related to the human risk of colon, breast, and prostate cancers. The mutagenicity of PhIP in Big Blue© rats was shown to be tissue-, sex-, and dose-dependent. PhIP was found to be a potent mutagen in the colon, followed by the cecum, prostate, and kidney. Compared with the background mutational spectra, the PhlP-induced spectra were characterized by an elevated proportion o f-1 frameshifts, consisting mainly of deletions of single G:C base pair. However, the induced spectra varied among tissues. A sex-dependent induction of mutation by PhIP was observed in the kidney such that the PhlP-induced mutation frequency was twice as high in male rats as in female rats; the biological significance of this difference is not clear. In contrast, although PhIP has been shown to induce colon tumors preferentially in male rats, and only rarely in female rats, no difference in mutational response was detected between the colons of male and female rats treated with PhIP. Experiments were performed to examine the in vivo effect of CLA on mutagenesis. Similar to what is seen for the mutagenicity of PhIP, the modification by CLA depends on tissue, sex, and dose of administration. CLA showed a modest protection against PhlP-induced mutagenesis in the distal part of the colon, in the prostate, and in the kidney of female rats. However, significant changes in the overall PhlP-induced mutation spectrum were seen only in the prostate. The antimutagenic effect of CLA may be directly responsible for its cancer prevention «^lability, since PhlP-induced aberrant crypt foci in the colon of male rats were completely inhibited by CLA However, CLA was not totally innocuous. When supplemented at 0.5%, CLA acted as a comutagen of PhIP, increasing the PhlP-induced MF in the cecum, although this effect was not observed when CLA was supplemented at 1%. The differences in effect may be related to the antioxidant or pro-oxidant activities of CLA isomers under experimental conditions. Due to the artificial nature of the lambda/LIZ lacI transgene and the possible absence of DNA repair in this transgene, the suitability of the Big Blue© transgenic assay as a mutational test system has been questioned. We examined the repair of UV- and benzo(α)pyrene diol epoxide-induced DNA damage in this non-transcribed lambda construct of the Big Blue© rat-2 transgenic cell line and demonstrated that DNA damage is indeed repaired in this transgenic construct. Lastly, since CLA altered the mutational spectra in the prostate in a way consistent with an effect of mismatch repair, the possibility of an effect of CLA on mismatch repair was explored in bacteria. Although CLA was found to increase mutant frequency in a mismatch repair proficient E. coli strain, but not in deficient strains, the mechanism by which CLA operates remains unclear. Altogether, the data demonstrate the mutagenicity of PhIP and its modulation by CLA as a function of tissue, sex, and dose of administration, and support the application of the Big Blue© transgenic assay as a screening tool for mutagens and chemopreventive agent / Graduate

Mutagenesis

Cancer

Genetic aspects

The role of Msh2 DNA mismatch pair and P27(kip1) cell cycle regulation on mutagenesis and carcinogenesis

Zhang, Shulin

23 October 2018

Transgenic rodents harbouring the E. coli lacI gene greatly facilitate the study of mutations in vivo where the effects of age, diet, lifestyle, sex, tissue and species specificity can be assessed. In addition, it also permits the investigation of mutations in a specifically altered genetic background. In this thesis, I used the lacI transgenic rodents to study the effect of strains and species difference on spontaneous mutation in the liver, as well as the influence of the DNA repair gene Msh2 and the cell cycle regulation gene p27 on mutagenesis and carcinogenesis. By studying spontaneous mutations in different strains and species of rodents which has different transgene insertion sites and constructs, we demonstrate that despite such differences, the spontaneous mutation frequency and spectra are similar. The major parts of the thesis demonstrate the impact of a deficiency in the Msh2 and p27 gene on spontaneous and chemically induced mutations. The mutator phenotype of thymic lymphoma arising in an Msh2 deficient background was also studied. A deficiency in the Msh2 gene caused an significant increase in mutation frequency in three parts of the colon with a distinct mutational spectrum characterized by an increase of G:C>A:T transitions. However, we did not detect the differences in mutation frequency and spectrum among the three parts of the colon. The mutagenesis of a colonic mutagen and carcinogen 2-amino-1 -methyl-6-phenolimidazo[4,5-b]pyridine (PhIP) was investigated. Msh2 deficiency was found to increase PhIP induced colon mutagenesis in a synergistic manner. Msh2+/- mice displayed a significantly increased frequency of -1 frameshifts in the spontaneous and PhIP treatment group indicating that Msh2 germ line mutation carriers are also at an increased risk of developing cancers. Msh2 thymic lymphomas exhibit a large increase in mutation frequency and an altered mutational spectrum featured by an increase of base substitutions occurring at A:T basepairs, -1 frameshifts and complex mutations. The influence of a deficiency in the p27 cell cycle control gene on mutagenesis is addressed in the next section of the thesis. We created a novel double transgenic mouse strain bearing a different functional status of p27 gene as well as the lacI transgene. P27 deficient mice exhibit similar levels of spontaneous mutation and a similar mutational spectrum as p27 wild type and heterozygous mice. However, after N-nitroso-N-ethylurea (ENU) treatment, hypermutability was detected in p27-/- mice. Interestingly, p27 heterozygous mice displayed an intermediate sensitivity upon ENU treatment indicating an haplo-insufficiency of the p27 gene in protecting against chemically induced mutagenesis. All three genotypes of p27 mice displayed a similar mutational specificity after ENU treatment characterized by the mutations occurring at A:T base pairs. These results show that both Msh2 and p27 homozygous deficient mice are more susceptible to chemically induced mutation than wild type mice. In contrast to the finding of Msh2 mice, p27 functional status does not affect the mutational spectrum recovered in lacI transgene. This illustrates the different mechanisms of DNA mismatch repair and cell cycle regulation in maintaining genomic integrity. The haplo-insufficiency of some genes in safeguarding genomic stability highlights the importance of tumor screening in carrier populations. / Graduate

Mutagenesis

Cancer

Genetic aspects

Discovery and application of genetic variants for obesity related traits

Day, Felix Ranulf

January 2014

No description available.

Obesity--Genetic aspects

Genetic aspects of branchio-oto-renal dysplasia : the BOR syndrome

Sproule, James Robert.

January 1979

No description available.

Deafness -- Genetic aspects.