Global ETD Search

41	Molecular characterization of the mouse cytoglobin Chow, Kwok-fai, Joseph, 周國輝 January 2006 (has links) published_or_final_version / abstract / Zoology / Doctoral / Doctor of Philosophy Globin. Genomes. Mice - Molecular aspects.
42	The systematic sequencing and functional analysis of the region pheA (240'o)-dnaB(256'o) of the B.subtilis chromosome Carter, Noel Mark January 1998 (has links) No description available. 579 Genomes; Bacilus subtilis; Arabinases
43	The unusual HIV-1 codon bias as a tool for anti-HIV strategies Kotsopoulou, Ekaterini January 1999 (has links) No description available. 579 Genomes; Retroviruses; Gene therapy
44	Neurospora tetrasperma from Natural Populations : Toward the Population Genomics of a Model Fungus Corcoran, Pádraic January 2013 (has links) The study of DNA sequence variation is a powerful approach to study genome evolution, and to reconstruct evolutionary histories of species. In this thesis, I have studied genetic variation in the fungus Neurospora tetrasperma and other closely related Neurospora species. I have focused on N. tetrasperma in my research because it has large regions of suppressed recombination on its mating-type chromosomes, had undergone a recent change in reproductive mode and is composed of multiple reproductively isolated lineages. Using DNA sequence data from a large sample set representing multiple species of Neurospora I estimated that N. tetrasperma evolved ~1 million years ago and that it is composed of at least 10 lineages. My analysis of the type of asexual spores produced using newly described N. tetrasperma populations in Britain revealed that lineages differ considerably in life history characteristics that may have consequences for their evolution. A comparative genomic analysis using three genomes of N. tetrasperma and the genome of N. crassa revealed that the mat a chromosomes in the lineages examine have been introgressed from other Neurospora species and that this introgression has reduced levels of molecular degeneration on the mating-type chromosomes. Finally, I generated a population genomic dataset composed of 92 N. tetrasperma genomes and two genomes of other Neurospora species. Analysis of these genomes revealed that all strains of N. tetrasperma have large regions of suppressed recombination on their mating-type chromosomes ranging from 69-84% of the chromosome and that the extent of divergence between mating-type chromosomes within lineages varies greatly (from 1.3 to 3.2%). I concluded that the source of this great divergence mating-type chromosome is large-scale introgression from other Neurospora species, and that these introgressed tracts have become fixed within N. tetrasperma lineages. I also discovered that genes within non-recombining introgressed regions of the mating-type chromosome have severely reduced levels of genetic variation as compared to the autosomes, and exhibit signatures of reduced molecular degeneration. My analysis of variation in coding regions revealed that positive selection on the introgressed regions has resulted in the removal of deleterious mutations and is responsible for the reductions in molecular degeneration observed. Neurospora poulation genetics genomes introgression
45	Development and assessment of machine learning attributes for ortholog detection Lin, Ying. January 2006 (has links) Thesis (Ph.D.)--University of Delaware, 2006. / Principal faculty advisor: John Case, Dept. of Computer and Information Sciences. Includes bibliographical references.
46	Efficient algorithms for optimizing whole genome alignment Lu, Ning, 陸宁 January 2004 (has links) published_or_final_version / abstract / toc / Computer Science / Master / Master of Philosophy Genomes - Data processing. Algorithms. Bioinformatics.
47	Cbf1 regulates chromatin remodelling of the Saccharomyces cerevisiae genome at multiple binding sites Garduño, Bertha Veronića January 1999 (has links) The centromere binding factor 1, Cbf1, of Saccharomyces cerevisiae is a bHLH/ZIP protein which has been described as a determinant of specific chromatin structures and as a tethering factor for activators of transcription at the promoters of genes of the Methionine Biosynthesis Pathway. Deletion mutants show various phenotypes, among them methionine auxotrophy, an increased rate of chromosome loss, modifications in the growth rate and modification of the chromatin structure at MET genes. Meiosis competence also becomes greatly reduced in cbf1 cells. The sequence motif (RTCACRTG) to which Cbf1p binds is found at multiple loci through the yeast genome. This thesis shows that the chromatin structure is reorganised at multiple Cbf1p binding sites in vivo, when yeast cells are starved to enter meiosis. Extensive remodelling occurs at the MET16, MET17(25), DRS2 and GDH3 loci and at the YAL060W open reading frame, as detected by in vivo digestion of chromatin with micrococcal nuclease and indirect end-labelling. The same kind of analysis showed that the remodelling of chromatin at Cbf1p binding sites is not specific for meiosis, it occurs also in similarly starved haploid cells. The lack of methionine is a key trigger of these changes. This reorganisation of chromatin is dependent on Cbf1p, since starved cbf1 cells do not display any modification in nuclease accessibility patterns at or around Cbf1p binding sites. Mutational analysis revealed that a negative charge at a putative phosphorylation site (serine residue 226) and the DNA-bindmg activity of Cbf1p are both required for the chromatin reorganisation to occur in response to starvation. CBF1 mutants which do not reorganise chromatin were also shown to be unable to enter meiosis, suggesting that the remodelling of chromatin at multiple Cbf1p binding sites may be required to enter pre-meiotic DNA replication, since such cells arrest before the initiation of this process. In summary, the results presented in this thesis are compatible with a model in which Cbf1p plays an active role as part of a mechanism sensing the nutrient availability and regulates the reorganisation of chromatin, at multiple loci through the yeast genome, in response to starvation conditions. 572 Genomes : Binding sites (Biochemistry)
48	Development of electrochemistry-based DNA assay in a silicon/glass bio-device for point-of-care applications / Yeung, Siu Wai. January 2008 (has links) Thesis (Ph.D.)--Hong Kong University of Science and Technology, 2008. / Includes bibliographical references (leaves 181-209). Also available in electronic version.
49	A snapshot of the Artemia genome to code or not to code / Wittig, Stacey Lynn, January 2009 (has links) Thesis (M.S.)--Rutgers University, 2009. / "Graduate Program in Microbiology and Molecular Genetics." Includes bibliographical references (p. 60-62).
50	Transcription of the epstein-barr virus genome in nasopharyngeal carcinoma / Chen, Hong-lin. January 1992 (has links) Thesis (Ph. D.)--University of Hong Kong, 1992. Nasopharynx Epstein-Barr virus. Genomes.

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