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The Global ETD Search service is a free service for researchers
to find electronic theses and dissertations. This service is
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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.
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Showing 11 to 15 of 15 (0.022 seconds)Spelling suggestions: "subject:"homeotic"" "subject:"homoeotic""
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Suppressor of zeste 12, a Polycomb group gene in Drosophila melanogaster; one piece in the epigenetic puzzleBirve, Anna January 2003 (has links)
In multicellular organisms all cells in one individual have an identical genotype, and yet their bodies consist of many and very different tissues and thus many different cell types. Somehow there must be a difference in how genes are interpreted. So, there must be signals that tell the genes when and where to be active and inactive, respectively. In some instances a specific an expression pattern (active or inactive) is epigenetic; it is established and maintained throughout multiple rounds of cell divisions. In the developing Drosophila embryo, the proper expression pattern of e.g. the homeotic genes Abd-B and Ubx is to be kept active in the posterior part and silenced in the anterior. Properly silenced homeotic genes are crucial for the correct segmentation pattern of the fly and the Polycomb group (Pc-G) proteins are vital for maintaining this type of stable repression. As part of this thesis, Suppressor of zeste 12 (Su(z)12) is characterized as a Drosophila Pc-G gene. Mutations in the gene cause widespread misexpression of several homeotic genes in embryos and larvae. Results show that the silencing of the homeotic genes Abd-B and Ubx, probably is mediated via physical binding of SU(Z)12 to Polycomb Response Elements in the BX-C. Su(z)12 mutations are strong suppressors of position-effect-variegation and the SU(Z)12 protein binds weakly to the heterochromatic centromeric region. These results indicate that SU(Z)12 has a function in heterochromatin-mediated repression, which is an unusual feature for a Pc-G protein. The structure of the Su(z)12 gene was determined and the deduced protein contains a C2-H2 zinc finger domain, several nuclear localization signals, and a region, the VEFS box, with high homology to mammalian and plant homologues. Su(z)12 was originally isolated in a screen for modifiers of the zeste-white interaction and I present results that suggests that this effect is mediated through an interaction between Su(z)12 and zeste. I also show that Su(z)12 interact genetically with other Pc-G mutants and that the SU(Z)12 protein binds more than 100 euchromatic bands on polytene chromosomes. I also present results showing that SU(Z)12 is a subunit of two different E(Z)/ESC embryonic silencing complexes, one 1MDa and one 600 kDa complex, where the larger complex also contains PCL and RPD3. In conclusion, results presented in this thesis show that the recently identified Pc-G gene, Su(z)12, is of vital importance for correct maintenance of silencing of the developmentally important homeotic genes.
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Ecological and molecular characterisation of a naturally occurring floral homeotic variant of Capsella bursa-pastoris (L.) Medik.Hameister, Steffen 07 September 2009 (has links)
The evolutionary relevance of homeotic alterations for the origin of new taxonomic entities is still a controversial objective in plant sciences. In this context, the discovery of a floral homeotic variant of Capsella bursa-pastoris in natural populations offers the unique opportunity to elucidate the evolutionary significance of homeotic mutants in the wild. Since all petals are transformed into additional stamens, the variant was termed Stamenoid petals (Spe). In this thesis, a combination of ecological and molecular characterisation of the variant was performed, to improve the understanding of evolutionary processes in plant populations. Molecular markers were used to analyze genetic differentiation among known provenances and also within a large sympatric population of wild-type and homeotic mutant. The results clearly suggest a repeated evolution of the novel flower morphology. Furthermore, genetic analyses provided substantial evidence, that the two floral variants are well-defined into flower-type dependent sub-samples within one population. The evaluation of phenotypic traits elucidated that the homeotic variant is not hampered in fitness. In greenhouse and field experiments, a significant ecological differentiation in the onset of flowering was detected among variants. Finally, the novel floral phenotype shows a co-dominant inheritance, and a marker-assisted mapping approach exposed a single locus in a genetic map. In conclusion, the comprehensive study of ecological and molecular aspects indicates that the floral homeotic variant may be treated as an established taxonomic entity and proved the predicted role as model for evolutionary objectives. Since morphological alterations like Spe are discussed as a result of macroevolution, the homeotic variant of C. bursa-pastoris provides the opportunity to survey a (macro)evolutionary novelty in association with continuous micro-evolutionary adaptation
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Protein dynamics in the nucleus: Implications for gene expression / Proteindynamik im Zellkern: Auswirkungen auf die GenexpressionFicz, Gabriella 16 July 2005 (has links)
No description available.
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An Anatomical Comparison of Wild Type and Homeotic Mutant Flowers of Clarkia tembloriensisObrebski, Chelsea Elizabeth 14 November 2019 (has links)
No description available.
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Caracterización genética y origen de las neuronas de la región claustroamigdalina en ratón.Legaz Pérez, Isabel 31 July 2006 (has links)
El objetivo de esta Tesis ha sido profundizar en el estudio del desarrollo del complejo claustroamigdalino en ratón. Para ello hemos estudiado: 1) cuales de sus componentes derivan del palio lateral o ventral, en base a expresión diferencial de genes reguladores Dbx1, Lhx9, Lhx2, Lmo3, Lmo4, Cadherina 8 y Emx1 durante el desarrollo embrionario; 2) el desarrollo de las interneuronas del complejo claustroamigdalino que contienen proteínas ligadoras de calcio (incluyendo el desarrollo de sus circuitos locales); 3) el origen histogenético de dichas interneuronas, mediante cultivos organotípicos y el análisis del ratón transgénico Nkx2.1-Cre/Rosa26-GFP (Kessaris y col. 2006). Nuestros datos permiten distinguir los componentes paliales laterales o ventrales del complejo, que contienen múltiples subtipos de interneuronas con orígenes en distintas subdivisiones del subpalio. Esto abre las puertas a futuras investigaciones sobre la conectividad y función de cada subtipo de interneurona, y sobre su grado de implicación en los desórdenes neuropsiquiátricos. / The objective of this Doctoral Thesis was to deepen in the study of the development of the claustroamygdaloid complex in mouse. For that, we pursued to study: 1) which components derive from either the lateral or ventral pallium based on differential expression of regulatory genes (Dbx1, Lhx9, Lhx2, Lmo3, Lmo4, Cadherina 8 y Emx1) during embryonic development; 2) the development of interneurons of the claustroamygdaloid complex that contain calcium binding proteins (including the development of its local circuits); 3) the histogenetic origin of these interneurons, by means of organotypic cultures and analysis of the transgenic mouse Nkx2.1-Cre/Rosa26-GFP (Kessaris and col. 2006). Our data allowed the distinction between lateral and ventral pallial components of the complex, which contain multiple subtypes of interneurons with origins in different subpallial subdivisions. This opens new venues for future investigations on the connectivity and function of each interneuron subtype, and on their involvement in neuropsychiatric disorders.
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