Дисертації з теми "Chromosome inversions"
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Bhatt, Samarth. "Segregation analysis of paracentric inversions in human sperm." Montpellier 1, 2008. http://www.theses.fr/2008MON1T002.
Повний текст джерелаYue, Ying. "[Breakpoint analysis of human chromosome 3 inversions during hominoid evolution]." [S.l.] : [s.n.], 2005. http://deposit.ddb.de/cgi-bin/dokserv?idn=976057794.
Повний текст джерелаChan, David Yiu Leung. "Analysis of artificial chromosomes and factors affecting stability in murine and human cultured and embryonic stem cells." Thesis, University of Oxford, 2010. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.568074.
Повний текст джерелаMautras, Albert. "Les inversions paracentriques du chromosome sept : à propos de deux observations." Bordeaux 2, 1989. http://www.theses.fr/1989BOR25067.
Повний текст джерелаNanassy, Oliver Zoltan. "Genetic and biochemical analysis of the Salmonella typhimurium Hin DNA recombinase /." Thesis, Connect to this title online; UW restricted, 1999. http://hdl.handle.net/1773/11525.
Повний текст джерелаRocha, Felipe Bastos 1981. "Pigmentação em Drosophila mediopunctata : plasticidade fenotipica e herdabilidade." [s.n.], 2007. http://repositorio.unicamp.br/jspui/handle/REPOSIP/316971.
Повний текст джерелаDissertação (mestrado) - Universidade Estadual de Campinas, Instituto de Biologia
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Resumo: Drosophila mediopunctata é uma espécie pertencente ao grupo tripunctata, que tem como traço marcante um padrão de pigmentação abdominal, sob a forma de três pintas na região mediana dos últimos tergitos. Nesta espécie, este padrão é variável, havendo indivíduos com quatro fenótipos, que vão de zero a três pintas. Já se observou que esta variação tem determinação genética, com marcada influência do cromossomo II, e alta plasticidade fenotípica em resposta à temperatura de desenvolvimento. Neste trabalho, buscou-se caracterizar parte destas duas fontes de variação. Por um lado, foram estudadas as normas de reação da pigmentação a um gradiente térmico, investigando-se classes fenotípicas contrastantes. Devido ao desenho experimental, que buscou separar os efeitos desta variável de um possível papel das inversões do cromossomo II, foi possível evidenciar um forte efeito das classes fenotípicas utilizadas sobre a resposta das estirpes ao gradiente térmico, independente do cariótipo. Foram descritos, por polinômios, dois tipos de norma de reação relacionados ao fenótipo, ambos com forma de parábola, mas diferindo em relação ao coeficiente de curvatura. O grupo de estirpes de pigmentação clara apresentou uma curva côncava e o grupo escuro uma curva convexa. A norma de reação da taxa de desenvolvimento de ovo a adulto foi caracterizada a partir do mesmo procedimento. Entretanto, apesar dos efeitos significativos do cariótipo e da classe fenotípica, a homogeneidade das normas de reação descritas por regressões lineares não possibilitou uma interpretação clara destes efeitos. A plasticidade do caráter também foi investigada quanto ao período de desenvolvimento termo-sensível. Assim, foi possível determinar a porção final da fase de pupa como o período no qual ocorre a influência da temperatura sobre o fenótipo de pintas do adulto. Por outro lado, em relação à determinação genética do caráter, foram obtidas estimativas de herdabilidade para o número de pintas abdominais, em condições quase naturais. Visando estabelecer um parâmetro de comparação com outros trabalhos, foi estimada a herdabilidade do tamanho do tórax a partir do mesmo material. Os resultados deste experimento, apresentaram grande contraste entre os dois traços: as estimativas foram baixas ou não significativas para o tamanho do tórax e, em geral, altas e significativas para o número de pintas
Abstract: Drosophila mediopunctata belongs to the tripunctata species group, which has a typical abdomen pigmentation pattern, consisting of three dark spots in the last tergites. In this species, this pattern is variable, with the phenotypes ranging from zero to three spots. It has been noted that this variation has genetical determination, with strong influence from the second chromosome, and high phenotypic plasticity in response to the developmental temperature. In this work, we attempted to describe part of these two variation sources. On one side, the pigmentation reaction norm to a thermal gradient was studied, by investigating the influence of contrasting phenotypical classes. Given the experimental design, which was planned to separate the effects of this variable from a possible influence of the second chromosome inversions, it was possible to detect a strong effect of the phenotypical classes on the lineages response to the thermal gradient, independent of the kariotype. Two types of reaction norms, related to the phenotype, were detected and described by polynomial adjustment. Both had a parabolic shape, but with different curvature coefficients. The light pigmentation lineage group showed a concave curve, and the dark group had a convex curve. The reaction norm of development rate from egg to adult was described according to the same procedure. However, despite the significant effects of the karyotype and phenotypical classes, the homogeneity of reaction norms, described by linear regression, hindered a clear interpretation of these effects. The character plasticity was also investigated in respect to the developmental thermosensitive period. Thus, it was possible to determine that the period in which the temperature influence on the adult phenotype occurs is the last portion of the pupal phase. On another side, relative to the character genetic determination, heritability estimates for the number of abdominal spots were obtained, in nearly natural conditions. Aiming to establish a comparison parameter with other studies, the heritability of thorax length was estimated based on the same material. The results of this experiment reveal a great contrast between these trait estimates: for the thorax they were low or non-significant, and, in general, for the abdominal spot number, they were high and significant
Mestrado
Genetica Animal e Evolução
Mestre em Genética e Biologia Molecular
Garmendia, Eva. "A Unified Multitude : Experimental Studies of Bacterial Chromosome Organization." Doctoral thesis, Uppsala universitet, Institutionen för medicinsk biokemi och mikrobiologi, 2017. http://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-332471.
Повний текст джерелаTodd, Roger Benedict. "Molecular analysis of a 7q inversion associated with myelodysplasia." Thesis, University College London (University of London), 2001. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.248167.
Повний текст джерелаFellmann, Florence. "Inversion paracentrique : marqueur ou anomalie ; a propos d'une inversion paracentrique du chromosome 13 transmise sur 5 generations d'une famille de 162 membres." Nancy 1, 1993. http://www.theses.fr/1993NAN11162.
Повний текст джерелаNelson, Tanya N. "Molecular genetic analysis of human 8p inversion duplication chromosomes." Thesis, National Library of Canada = Bibliothèque nationale du Canada, 1998. http://www.collectionscanada.ca/obj/s4/f2/dsk2/ftp02/NQ34598.pdf.
Повний текст джерелаGiner, Delgado Carla. "Large-scale evolutionary analysis of polymorphic inversions in the human genome." Doctoral thesis, Universitat Autònoma de Barcelona, 2017. http://hdl.handle.net/10803/459114.
Повний текст джерелаChromosomal inversions are structural variants that invert a fragment of the genome without usually modifying its content, and their subtle but powerful effects in natural populations have fascinated evolutionary biologists for a long time. Discovered a century ago in fruit flies, their association with different evolutionary processes, such as local adaptation and speciation, was soon evident in several species. However, in the current era of genomics and big data, inversions frequently escape the grasp of current technologies and remain largely overlooked in humans. During the last few years, the InvFEST Project has aimed to address the missing knowledge about human inversions by validating and genotyping a large fraction of predicted polymorphisms. In particular, it has generated one of the most useful data sets on human inversions, consisting of 45 common inversions (with sizes from 83 bp to 415 kbp) genotyped at high-quality in 550 individuals of seven populations of diverse ancestry. This thesis takes advantage of the available population-scale information, combined with whole-genome sequences available from the 1000 Genomes Project, to carry out the first detailed analysis of the evolutionary properties of human polymorphic inversions. The methods used combine theoretical models, simulations and empirical comparisons with other mutation types. Besides the complete characterization of the data set, the results confirm fundamental differences between inversions created by different mechanisms. The frequency distribution of the 21 inversions originated by non-homologous mechanisms (NH) is similar to that expected for neutral variants when controlling for detection biases, which indicates that they are not subjected to strong negative selection. Recombination is completely inhibited across the whole inversion length, with no clear genetic exchange found, and possibly over a few kbp beyond the breakpoints. As a result, NH inversions strongly affect local genome variation levels, as predicted by computer simulations, with older inversions increasing total nucleotide diversity, while younger ones at very high frequency could have the opposite effect. In contrast, most inversions created by non-allelic homologous recombination (NAHR) (19/24) have appeared independently in different haplotypes in the sample. These high recurrence levels are reflected in several measures: they are enriched in intermediate frequencies, share multiple nucleotide polymorphisms between orientations, and have little linkage disequilibrium with neighbouring variants, which limits their detection by tag SNP strategies. Finally, in order to find inversions that are functional candidates, different signatures of selection on inversions were explored based on their frequencies, population differentiation and sequence variation patterns. Ten candidates were revealed, with three of them found to be >1.5 million years old and maintained at intermediate frequencies, possibly by balancing selection. One of these was also found in archaic hominins. Other candidates seem to have reached high frequencies in a short period of time in some populations, consistent with positive selection. Notably, over half of the candidates are located within gene regions, which suggests that they may have functional effects. Thus, this work offers an overview of inversion dynamics and their role as genomic modifiers, opening interesting avenues of investigation.
Prinz, zu Salm-Horstmar Maximilian Philipp Albrecht. "The Chromosome 8p23.1 Inversion : High-Throughput Detection & Investigation of Phenotypic Impact." Thesis, Imperial College London, 2009. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.516479.
Повний текст джерелаGutiérrez, Arumi Armand 1980. "Ancestral genomic submicroscopic inversions of human genome and their relation with multifactorial human diseases." Doctoral thesis, Universitat Pompeu Fabra, 2016. http://hdl.handle.net/10803/454777.
Повний текст джерелаS'han realitzat grans avenços en caracterització dels diferents tipus de variació en el genoma humà, com ara mutacions puntuals, insercions, delecions, etc., però encara existeix un component genètic de les malalties, determinada per l'heretabilitat, que és desconeguda. Les Inversions són mutacions cromosòmiques en què un fragment de cromosoma canvia la seva orientació respecte a la de referència i són difícils de genotipar per ser neutres en nombre de còpies. El nostre grup ha desenvolupat una eina per inferir algunes variants d’inversions submicroscòpiques ancestrals (0.5MB - 5MB) per mètodes computacionals utilitzant microarrays d’SNPs, i ha documentat que es correlacionen amb expressió gènica. El nostre objectiu ha estat intentar determinar la contribució de les inversions cromosòmiques al fenotip en quatre models de malalties complexa: autisme, esquizofrènia, artritis reumàtica i colitis ulcerosa. Realitzat estudis de cas control i de segregació en trios, els nostres resultats han determinat que: • Les inversions 17q21.31 i 8p23 s’associen a risc d’autisme i esquizofrènia. Concretament, la 17q21.31, s’associa especialment amb aquells individus provinents de famílies multiplex (OR=1.20 p-value 9.52e-05). Per altra banda, l’al•lel contrari (17q) confereix risc d’esquizofrènia (OR=0.86 p-value 0.007). • Hem caracteritzat tres haplotips relacionat amb la inversió de la regió 15q24 (NI, Ia i Ib) que segueixen un patró d'herència Mendeliana amb una alta frequència en Europeus (NI=20%, Ia=50%, Ib=30%). L'homozigositat per l'al•lel no invertit correlaciona amb la sobre-expressió de MAN2C1 en varies àrees del cervell (mentres que l'al•lel Ib està sota expresat). • Pel que fa a l’artritis reumàtica (RA) i la colitis ulcerosa (UC), hem trobat unes regions d’homozigositat 4q32 (RA OR=9.32 95%CI [2.66-63.45]) i 3p24.3 (UC OR=7.77 95% CI [2.08-54.56]) . Addicionalment, també hem trobat uns haplotips que podien ser inversions que també hi estarien associats però estan pendents de validacions addicionals.
Ruiz, Arenas Carlos 1990. "Methods and bioinformatic tools to study polymorphic inversions in complex diseases." Doctoral thesis, Universitat Pompeu Fabra, 2019. http://hdl.handle.net/10803/666582.
Повний текст джерелаChromosomal inversions are structural variants where a segment changes its orientation. Chromosomal inversions reduce homologous recombination, producing different haplotypes in standard and inverted chromosomes. As a result, they influence adaptation and selection and play a role in susceptibility to human diseases. Inversions can be studied using experimental and bioinformatic methods. SNP array data can be used to call inversion genotypes by using haplotype differences between inverted and standard chromosomes. However, these methods are not optimized for large cohorts (thousands of individuals from existing databases such as dbGaP or UK Biobank). Also, current methods can only genotype inversions with two haplotypes and the inversion calling is difficult to be harmonized among cohorts. Finally, it is recognized that chromosomal inversions affect gene expression and DNA methylation. However, there are no accurate methods to globally assess the effect of inversions on local gene expression or DNA methylation. The main aim of this thesis is to develop new robust and scalable methods and bioinformatic tools to study the phenotypic and functional effects of chromosomal inversions by overcoming the existing limitations. To this end, I have developed a new method to genotype chromosomal inversions that can be used in large cohorts, inversions with multiple haplotypes and that uses reference haplotypes allowing the integrative analysis of multiple cohorts. Second, I have implemented a multivariate method based on redundancy analysis to study the effects of chromosomal inversions on local DNA methylation and gene expression. Then, I applied both methods to study the role of chromosomal inversions in two groups of complex diseases: neurodevelopmental disorders and cancer. Finally, I developed a new method to study how chromosomal inversions affect recombination patterns. This method is extendable to any genomic regions containing subpopulations with different recombination patterns, allowing associating these subpopulations to phenotypic traits.
Lerga, Jaso Jon. "Integrative analysis of the functional consequences of inversions in the human genome." Doctoral thesis, Universitat Autònoma de Barcelona, 2019. http://hdl.handle.net/10803/669344.
Повний текст джерелаStructural variation contributes substantially to the genetic diversity, but its association with complex traits and diseases is not well understood and deserves detailed characterisation. This is particularly true for chromosomal inversions, whose functional consequences have remained elusive in humans, with very few notable exceptions. Despite the rising interest in identifying all types of genomic variants, inversions have been often set aside due to the presence of repetitive regions in their breakpoints along with their balanced nature. The InvFEST Project has tried to overcome this technical challenge by developing unique methods for inversion genotyping. Thanks to this effort, a total of 111 polymorphic human inversions have been accurately genotyped in a large number of individuals from diverse populations, becoming the most complete and reliable resource of this type of variation available to date. In the current era of precision medicine, quantitative trait loci (QTL) analysis has emerged as a key approach to determine how genetic polymorphisms influence gene expression and, in turn, phenotypic traits. Thus, this thesis makes the most of the great amount of data generated to perform for the first time a systematic quantification of the functional impact of human polymorphic inversions. The results show that inversions can affect gene expression by maintaining differentiated haplotypes, disrupting or reorganizing gene structures, creating novel fusion transcripts or acting through changes in epigenetic patterns. Strikingly, half of the inversions analysed act as lead QTLs or are in high linkage disequilibrium (LD) with top QTLs for gene expression and epigenetic changes across different tissues and cell lines, which suggests that inversions are enriched for functional effects. In particular, this influence on molecular phenotypes is even stronger for long inversions (>100kb), which are involved in 80% of the QTL associations. Although structural variants are known to have a higher chance to be associated with expression levels and complex traits, the detected inversion effects may reflect a trade-off between beneficial expression changes and potential negative costs on fertility due to production of unbalanced gametes by recombination. Furthermore, inversions present an enrichment of genome-wide association studies (GWAS) signals in their surrounding area, and 14 of them are in high LD with trait-associated variants, supporting their potential implication in human phenotypes. Finally, the phenotypic consequences of two interesting inversions have been investigated in detail. HsInv0102 inverts an alternative non-coding exon from the RHOH gene. Interestingly, this inversion is also associated with RhoH protein levels and the inverted allele could act as a moderate protective locus on blood cancer susceptibility. On the other hand, HsInv0124 regulates the expression of several genes in the IFITM region, including IFITM2 and IFITM3, through changes in histone modification patterns. Moreover, under infection conditions, this inversion has a pervasive effect on the expression of genes related with immune response, indicating that it may play an important role in defense against viral infections. All together, these findings illustrate the potential functional impact of inversions on the human genome and help to uncover previously missing variants related to phenotype variability.
Entesarian, Miriam. "Molecular Genetic Studies of ALSG, Kostmann Syndrome and a Novel Chromosome 10 Inversion." Doctoral thesis, Uppsala universitet, Institutionen för genetik och patologi, 2009. http://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-100598.
Повний текст джерелаDelauney, Jean-Philippe. "Cartographie du chromosome 4p par des techniques de biologie moléculaire : étude d'une inversion-délétion du chromosome 4 chez une patiente présentant un syndrome de Wolf-Hirschhorn et une chorée." Bordeaux 2, 1996. http://www.theses.fr/1996BOR23030.
Повний текст джерелаBrooks, Samantha Ann. "STUDIES OF GENETIC VARIATION AT THE KIT LOCUS AND WHITE SPOTTING PATTERNS IN THE HORSE." UKnowledge, 2006. http://uknowledge.uky.edu/gradschool_diss/479.
Повний текст джерелаNaseeb, Samina. "Molecular evolution in yeast : role of chromosomal inversions and translocations in speciation, adaptation and gene expression." Thesis, University of Manchester, 2011. https://www.research.manchester.ac.uk/portal/en/theses/molecular-evolution-in-yeast-role-of-chromosomal-inversions-and-translocations-in-speciation-adaptation-and-gene-expression(58fd85d1-fd26-426e-8643-482cd20447d4).html.
Повний текст джерелаBriault, Sylvain. "Inversion paracentrique cytogénétiquement équilibrée du chromosome x cosegregeant dans une famille avec une déficience mentale liée au sexe : approche moléculaire des points de cassure." Tours, 1997. http://www.theses.fr/1997TOUR3303.
Повний текст джерелаWettwer, Marco [Verfasser], and Ortrud [Akademischer Betreuer] Steinlein. "Molekularzytogenetische Charakterisierung der perizentrischen Inversion des Chromosoms 9 : Bruchpunktanalyse und zusätzliche Strukturaberrationen / Marco Wettwer ; Betreuer: Ortrud Steinlein." München : Universitätsbibliothek der Ludwig-Maximilians-Universität, 2017. http://d-nb.info/1148275827/34.
Повний текст джерелаRouen, Alexandre. "Réarrangements chromosomiques chez l'homme : ségrégation des chromosomes à la méiose et procréation." Thesis, Paris 6, 2016. http://www.theses.fr/2016PA066735.
Повний текст джерелаChromosomal translocations and other balanced rearrangements, although usually associated with a normal phenotype, can lead to the transmission of an abnormal unbalanced genetic content to the offspring. Balanced and unbalanced spermatozoa are indistinguishable, making it impossible to select them prior to in vitro fertilization. We conducted a series of research projects aimed at evidencing specific characterics for unbalanced spermatozoa, in a way to ultimately distinguish them from balanced ones during in vitro fertilization. We showed that unbalanced spermatozoa had higher DNA fragmentation rates, were less dense, and that their nuclear volume was higher. This led to developing a selection procedure for balanced spermatozoa in rearrangement carriers. Using the hypo-osmotic swelling test (HOST), we showed that a specific flagellar morphology was associated with balanced chromosomal status. We suggest using this procedure prior to ICSI in order to improve the reproductive prognosis in those patients. We also suggest evaluating the proportion of unbalanced spermatozoa in every patient with a chromosomal rearrangement. Although this proportion varies among patients, it is stable over time for a given patient. We believe this is a decisive element in choosing between the different available options : natural conception, artificial insemination with discontinuous gradient centrifugation, ICSI with HOST-based selection, and pre-implantation genetic diagnosis (PGD)
Puig, Giribets Marta. "Evolution of the hsp70 gene family at the nucleotide, genome organization and gene expression levels in Drosophila subobscura." Doctoral thesis, Universitat Autònoma de Barcelona, 2018. http://hdl.handle.net/10803/663952.
Повний текст джерелаNumerous studies have confirmed the adaptive value of the rich chromosomal inversion polymorphism in the drosophilid D. subobscura. However, until recently very little was known about the molecular basis behind its maintenance in natural populations. In search of candidate loci, a previous heat shock experiment quantified Hsp70 protein levels in homokaryotypic strains for the OST, O3+4+8 and O3+4 arrangements. Unexpectedly, individuals of the warm climate-associated O3+4 arrangement showed increased levels in absence of thermal stress that did not boost after the heat shock. Unfortunately, by the time this experiment was performed there was very little data available on the molecular organization of the Hsp70IR locus in D. subobscura. The previously mentioned results led to the present thesis work, whose objectives are to locate the Hsp70IR locus in the karyotype and to know the genomic organization, molecular characteristics and gene expression patterns in several representative chromosomal arrangements that comprise the genomic region where the hsp70 gene family is located: O3+4+16+2, O3+4+8, O3+4 and OST. Using the sequence of a clone from an OST line genomic library and contigs from the unassembled genome of D. subobscura, we designed a probe from the hsp70 coding region that enabled us to determine the location of the locus by in situ (ISH) hybridization. Concomitantly, we completed the sequencing of a 9-10 kb region in the Hsp70IR locus in 12 lines isogenic for the aforementioned arrangements and in D. madeirensis and D. guanche to shed light on the evolution of this locus in the last 1.8 - 2.8 million years (myr). ISH results showed a single hybridization site in the 94A band in the distal segment (SI) of the O chromosome coincident in the 4 studied karyotypes: O3+4+16+2, O3+4+8, O3+4 and OST. The sequences corresponding to the 12 isogenic lines and to D. madeirensis and D. guanche indicated that in these three species of the subobscura cluster, the Hsp70IR locus consists of two 2.5 - 3.0 kb long paralogous copies in divergent orientation separated by a 0.5 - 1.4 kb nonduplicated central spacer region. The two copies show a high degree of conservation between the different gene arrangements and species analyzed, while the central spacer region is highly polymorphic. Among the most relevant aspects of polymorphism analyses, we highlight the high degree of conservation in the coding regions (CDSs) and the cis-regulatory elements (CREs) in the proximal promoter of all the analyzed hsp70 genes, which might indicate that these are functional in all studied lines, and that their regulation might be similar. Curiously, at the sequence level, the paralogous 5'-UTR and CDS regions tend to be significantly more similar within the same arrangement and, in some cases, within the same line, probably as a result of ectopic gene conversion. Lastly, we carried out the quantification of basal hsp70 mRNA and protein levels in adult males and females of six lines isogenic for the cold climate-associated OST and six for the warm climate-associated O3+4 arrangements. Basal mRNA quantification results indicate that the two arrangements exhibit similar levels, yet significant differences are observed between males and females of the warm O3+4 arrangement. Regarding the quantification of basal Hsp70 protein levels, these suggest that there are no differences between sexes nor between the two arrangements, but instead we observe a significant interaction between sex and arrangement. Overall, the results for both, mRNA and protein data, indicate that hsp70 expression might be influenced by sex.
François, Vincent. "Mise en evidence de regions non divisibles sur le chromosome d'escherichia coli : relation avec la terminaison de la replication." Toulouse 3, 1989. http://www.theses.fr/1989TOU30020.
Повний текст джерелаDolgova, Olga. "Genetic and phenotypic differentiation in three chromosomal arrangements of drosophila subobscura." Doctoral thesis, Universitat Autònoma de Barcelona, 2013. http://hdl.handle.net/10803/129183.
Повний текст джерелаBackground Global warming is affecting many wild species in different ways. One of the species demonstrating thermal adaptation on the population genetic level is Drosophila subobscura. Latitudinal clines in the frequency of many chromosomal inversions of this species were well documented in the original Palearctic populations, and the discovery of parallel clinal patterns a few years after the colonization of South and North Americas provided compelling evidence that the clines evolved by natural selection. However, the selective process maintaining inversions in populations is not yet clear. Traditionally three selective hypotheses have been advanced to explain the maintenance of the chromosomal polymorphism, according to the level of operation of natural selection: chromosome, coadapted genes (“supergenes”) and individual genes. Objectives To distinguish between different hypotheses the following aspects were studied in D. subobscura: 1. The distribution of chromosomal arrangements along the thermal gradient; 2. The nucleotide variation in six genes inside the three most frequent chromosomal inversions; 3. The genetic basis of thermal preference and heat shock tolerance in isochromosomal lines. Results and conclusions The frequencies of the most abundant chromosomal arrangements in general correlated with temperature gradient, forming latitudinal clines. The arrangement OST positively correlated with latitude and its frequency increased from the south to the north. At the same time the frequency of O3+4+7 shows a negative correlation with latitude and reaches its maximum frequency in the south of Europe disappearing in the north. The O3+4 arrangement has a negative correlation with the latitude. Therefore, the arrangement OST is supposed to be cold-adapted while the other arrangements are considered to be warm-adapted. The nucleotide variation of the most frequent chromosome arrangements was analyzed in two distant Spanish populations situated along a latitudinal gradient. No within-inversion genetic differences were detected among populations, which suggest that the gene content along the gradient is rather constant for the various chromosomal arrangements and genetic flow is high. Although gene flux between different inversions was detected, significant genetic differentiation among inversions for all genes was found. Genetic differentiation between arrangements was also detected by linkage disequilibrium analysis, showing significant associations between informative sites when comparing arrangement pairs, which could be explained by low recombination rate between inversions and probable epistasis between some genes. The footprints of selection nearly in all genes, either in coding or noncoding parts, were detected using several neutrality tests. The Local Adaptation hypothesis is the one that fits better to our data and would explain the maintenance of the coadapted gene complexes within inversions in D. subobscura. Our results corroborate that arrangements on chromosome O affect adult thermal preference in a laboratory temperature gradient, with cold-climate OST carriers displaying a lower thermal preference than their warm-climate O3+4 and O3+4+8 counterparts. However, these chromosome arrangements did not have any effect on adult heat tolerance and, hence, we putatively discard a genetic covariance between both traits arising from linkage disequilibrium between genes affecting thermal preference and genes of heat shock resistance. Therefore, thermal preference and heat tolerance in the isochromosomal lines of D. subobscura appear to be genetically independent, which might potentially prevent a coherent response of behavior and physiology (i.e., coadaptation) to thermal selection. If this pattern were general to all chromosomes, then any correlation between thermal preference and heat resistance across latitudinal gradients would likely reflect a pattern of correlated selection rather than genetic correlation.
Calabria, Garcia Gemma. "Inversions cromosòmiques, clines i adaptació a "Drosophila suboscura": aproximació mitjançant marcadors moleculars." Doctoral thesis, Universitat de Barcelona, 2012. http://hdl.handle.net/10803/97297.
Повний текст джерелаDrosophila subobscura is a species with a highly rich inversion polymorphism, which has been shown to be adaptive and responding to global warming. However, the selective pressures acting on inversion how are they maintained in the populations are still unclear. Three main hypotheses have been proposed to explain the adaptive value of inversions: the Coadaptation hypothesis by Dobszhansky, the supergene selection postulated by Wassermann and the Local adaptation hypothesis of Kirkpatrick and Barton. In the present work we aimed to study in D. subobscura the role of chromosomal inversions in the adaptation to the environment and how are they maintained in the populations. To discriminate between the different hypotheses, the genetic content of the four more frequent arrangements of the O chromosome was analyzed in seven different populations located along a latitudinal cline. Different molecular markers such as microsatellite loci and candidate genes for thermal adaptation were used. The results showed a high genetic uniformity of inversions along the latitudinal cline, suggesting that the genetic content of each arrangement it is constant in all populations. Moreover, when comparing different arrangements, a high differentiation was found, being the OST the most different. The strong linkage disequilibrium found between two of the genes, despite being located 14Mb apart and inside and outside O7 inversion respectively could suggest the existence of epistatic interactions between them. Thus, the Local Adaptation hypothesis is the one that fits better our data and would explain the maintenance of the arrangements of the O chromosome of D. subobscura. Moreover, we have studied the relationship of the different chromosomal arrangements with the thermotolerance and the heat shock response. The results showed that O3+4 outbred individuals presented very high basal values of Hsp70 levels, equivalent to those measured after a heat shock in all the homokaryotypes independently of the arrangement. This, together with higher thermotolerance and thermopreference when comparing with the individuals carrying the OST arrangement, could be related whit the latitudinal cline of frequency that the O3+4 arrangement presents.
Engelbrecht, Adriaan. "Phylogeography of the southern African vlei rat, Otomys irroratus, inferred from chromosomal and DNA sequence data." Thesis, Stellenbosch : University of Stellenbosch, 2010. http://hdl.handle.net/10019.1/5476.
Повний текст джерелаENGLISH ABSTRACT: This study examines the phylogeography of the southern African vlei rat, Otomys irroratus using the mtDNA cyt b gene and chromosomal data derived using G-, and C-banding, Ag-NOR staining and fluorescence in situ hybridization (FISH using flow sorts of Myotomys unisulcatus). A total of N = 102 specimens were used from the Western Cape, Eastern Cape, Northern Cape, Free State, Mpumalanga and KwaZulu-Natal provinces of South Africa. Of the N = 102, N = 55 comprised fresh material while N = 47 comprises museum material obtained from the Durban Natural Science Museum of South Africa. Cytogentic analysis of N = 55 specimens collected from seven localities in South Africa revealed intra-specific variation resulting from two rearrangements, namely pericentric inversions and heterochromatin variation. Of the 55 specimens that were analyzed 47% contained inversions or centromeric shifts on four autosomes (OIR1, OIR4, OIR6 and OIR10) which were present singly in specimens (i.e. none of the specimens contained all four inversions concurrently). These inversions were present in both homozygous and heterozygous state over a wide geographic range suggesting that they are floating polymorphisms. Given the potential role of inversions in post-mating isolation (through production of aneuploid gametes), the prevalence of inversions as floating polymorphisms in the vlei rats suggest that they are probably retained in the population through suppression of recombination in the inverted regions of the chromosomes. In addition, differences between populations is due to the presence or absence of heterochromatic arms (and not inversions), which cause variation in the NFa (40 – 49) and supernumerary B chromosomes, resulting in the variation in diploid number (2n = 28 – 32). Analysis of N = 55 specimens revealed Ag-NORs on 7 autosomal pairs 1, 2, 5, 7, 8 and 9 proximal to the centromere on the short arm of the chromosome. Pair 8 also displayed Ag-NOR at the distal end of the long arm of the chromosome in individuals from the Free State province. Pair 3 showed two Ag- NORs occurring proximal to the centromere on the short arm and on the terminal end of the long arm, respectively. I obtained 953bp of mtDNA cyt b from fresh material and 400bp from museum material. Using maximum parsimony and Bayesian inference two main clades were retrieved. Clade A specimens occur mainly in the Western and Eastern Cape provinces of South Africa. Clade B specimens occur in the Eastern Cape, Free State, KwaZulu-Natal, Northern Cape and Mpumalanga provinces of South Africa. The mean sequence divergence between the main clades (A and B) is 7.0% and between sub-clades comprising clade B is 4.8%, while within clade A the sequence divergence was 1.91%. Nested clade analysis revealed allopatric fragmentation within O. irroratus. Chromosomal characters also support the two evolutionary lineages as clade A has pericentric inversions which occur as floating polymorphisms which are absent in clade B. Clade B in turn is fixed for a complex tandem fusion rearrangement which is absent from clade A. Divergence date estimates indicate that the two clades separated around 1.1 MYA, which coincides with climate changes since the late Pliocene/Pleistocene epochs. Cladogenesis within this species complex could therefore have been influenced by habitat fragmentation. A full taxonomic review of O. irroratus is therefore warranted by this study.
AFRIKAANSE OPSOMMING: Die suider Afrikaanse vlei rot, Otomys irroratus word gekenmerk deur fenotipiese konservatisme regoor die spesie se verspreiding en het groot chromosomale variasie met diploied chromosoom getalle wat reeks vanaf 2n = 23 tot 2n = 32. Hierdie variasie binne O. irroratus het gelei tot die beskrywing van drie chromosomale groupe naamlik die A sitotipe wat gekenmerk word deur 'n akrosentriese komplement. Die tweede groep wat die B sitotipe genoem word besit ten minste agt chromosoom pare met heterokromatiese kort arms, onderwyl die derde group (die C sitotipe) vier chromosoom pare het met heterokromatiese kort arms. Hierdie studie bestudeer die bevolkings genetika struktuur van O. irroratus deur 102 monsters te analiseer wat gekollekteer was regoor die spesie se verspreiding binne Suid-Afrika en die mitochondriale merker sitokroom b sowel as chromosoom fluoressent hibridisasie te gebruik. Ek het 55 monsters van sewe lokaliteite binne Suid-Afrika sitogeneties geanaliseer deur gebruik te maak van G- en C-bandbepaling asook die hibridisasie patrone geproduseer deur die vloeisorteerde chromosoome van Myotomys unisulcatus. Die analise het gewys dat 47% van die monsters perisentromeriese inversies besit het, wat slegs aangetref was of die outosome OIR1, OIR4, OIR6 en OIR10. Hierdie inversies was nooit almal teenwoordig binne dieselfde monster nie en was gevind in beide heterosigotiese en homosigotiese vorm. Die inversies kom ook voor oor 'n wye verspreiding wat daarop aandui dat dit swerwende polymorfisme is. Omdat inversies lei tot die produksie van aneuploiede gamete speel hulle 'n belangrike rol in post-parings reproduktiewe isolasie, die verskyning van swerwende inversies binne vlei rotte dui dus daarop dat hulle onderhou word binne populasie verband deur die onderdrukking van rekombinasie in die gedeeltes van die chromosoom. Verdere verskille tussen populasies behels die voorkoms of afwesigheid van heterochromatiese kort arms wat (nie inversies) wat lei tot die variasies in die Nfa (40 – 49). Die variasie in diploied getal (2n = 28 – 32) is eksklusief as gevolg van B chromosoome. Ag-NOR banding het ook gewys dat daar twee evolusionêre lyne binne O. irroratus voorkom. Verder het filogenetiese analise van al die monsters verkryg deur volgorde-bepaling met behulp van maksimale parsimonie en Bayesian afleiding twee klades geidentifiseer. Klade A diere kom voor in die Wes en Oos-Kaap provinsies van Suid-Afrika terwyl klade B diere voorkom in die Oos-Kaap, Vrystaat, KwaZulu-Natal, Noord-Kaap en Mpumalanga provinsies onderskeidelik van Suid-Afrika. Die gemiddelde volgorde-bepalings verskille beloop 7% tussen die twee hoof klades (A en B) en tussen sub-klades 4.8%, terwyl binne klade A die verskille slegs 1.91% beloop het. Analise van die verwantskap tussen die klades het gewys dat allopatriese fragmentasie heel waarskynlik gelei het tot die populasie genetiese struktuur binne O. irroratus. Chromosoom karakters onderskraag die twee evolusionêre lyne waar klade A slegs perisentriese inversies besit wat swerwend wat ontbreek in klade B. Klade B op sy beurt besit 'n komplekse tandemme fusie wat glad nie voorkom in klade A nie. Molekulêre datering het verder gewys dat die twee klades omtrent 1.1 miljoen jaar gelede versprei het, wat ooreenstem met die klimaats veranderinge wat sedert die Peioceen en Pleistoceen plaasgevind het. Klade vorming binne die spesies komples kan daarom as gevolg van habitat fragmentasie plaasgevind het. Hierdie studie dus noodsaak 'n volle taksonomiese ondersoek van O. irroratus ten einde vas te stel hoeveel spesies binne die komplex voorkom.
Sun, Yu. "Genome Evolution of Neurospora tetrasperma." Doctoral thesis, Uppsala universitet, Evolutionsbiologi, 2013. http://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-207330.
Повний текст джерелаSilva, Laura Helena Hafner da. "Variação morfologica em populações brasileiras de Drosophila melanogaster : variação latitudinal e temporal, herdabilidade e associação com inversões cromossomicas." [s.n.], 2006. http://repositorio.unicamp.br/jspui/handle/REPOSIP/316970.
Повний текст джерелаDissertação (mestrado) - Universidade Estadual de Campinas, Instituto de Biologia
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Resumo: O presente trabalho tem como objetivo caracterizar a variação do tamanho e forma das asas de populações de Drosophila melanogaster em três pontos ao longo de uma grande amplitude latitudinal na costa brasileira. O trabalho foi feito a partir de coletas realizadas no Recife, Rio de Janeiro e Porto Alegre, e os seguintes aspectos foram abordados: 1) variação geográfica; 2) variação temporal; 3) herdabilidade; e 4) a influência de inversões cromossômicas. Para este fim, o método da elipse foi aplicado a imagens digitalizadas das asas, e foram analisados: o tamanho das asas, sua forma e as posições dos pontos de junção e das extremidades das veias (caracterizadas por suas coordenadas angulares é radiais, essas padronizadas pelo tamanho da asa). Os resultados obtidos mostraram que a variação de tamanho em D. melanogaster no Brasil segue a tendência mundial de formação de clines latitudinais, com indiv.íduos maiores sendo encontrados a latitudes também maiores. No entanto, a herdabilidade e a variação temporal entre múltiplas coletas realizadas no Recife e no Rio de Janeiro não apresentou um padrão regular nítido. O único efeito consistente e significativo de inversões cromossômicas que pudemos observar foi o de In(3R)Payne sobre o tamanho corporal, sendo também consistente com achados prévios descritos na literatura. Entretanto, não detectamos efeito significativo de interação genótipo-ambiente, quer entre coletas, quer entre localidades
Abstract: The present work aims to characterize the variation of wing size and shape in Drosophila melanogaster populations from three localities distributed along a wide latitudinal range of the Brazilian coast. The work was performed based on collections made in the cities of Recife, Rio de Janeiro and Porto Alegre. The aspects studied were: 1) geographic variation; 2) temporal variation; 3) heritability; and 4) the influence of chromosomal inversions. To this end, the ellipse method was applied to digitized images of the wings. We analyzed wing size, wing shape and the position of vein junctions and extremities (characterized by their angular and radial coordinates, the latter being standardized by wing size). The results obtained showed that size variatiorn in Brazilian D. melanogaster follows the worldwide tendency toward the formation of latitudinal clines, with larger individuaJs being found at higher latitudes. However, the heritability and temporal variation among multiple collections performed in Recife and Rio de Janeiro did not show a clear regular pattern. The only consistent and significant effect of chromosomal inversions that we could observe was that of In(3R)Payne on body size, which is also consistent with previous findings reported in the literature. However, we did not detect a significant effect of genotype-environment interactions, neither among collections, nor among localities
Mestrado
Genetica Animal e Evolução
Mestre em Genética e Biologia Molecular
Hatadani, Luciane Mendes. "Sistematica molecular e variação morfometrica da asa de especies de Drosophila da radiação tripunctata." [s.n.], 2007. http://repositorio.unicamp.br/jspui/handle/REPOSIP/316981.
Повний текст джерелаTese (doutorado) - Universidade Estadual de Campinas, Instituto de Biologia
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Resumo: O grupo tripunctata e o segundo maior grupo neotropical de Drosophila em numero de espécies e foi incluído na radiação tripunctata ¿ que inclui outros grupos próximos. O segundo cromossomo de Drosophila medipunctata (espécie que pertence ao grupo tripunctata) e altamente polimorfico para inversões. Trabalhos anteriores sugeriram a presença de interação genotipo-ambiente para tamanho da asa, mas não para forma. Experimentos de laboratório foram realizados para testar os efeitos combinados de temperatura e inversão cromossômica no tamanho e forma da asa de D. mediopuncta. A morfologia da asa foi analisada por métodos de morfometria geométrica. Os resultados mostraram que tamanho e forma da asa são influenciados por temperatura, sexo e cariótipo. Também foram encontradas evidencias que sugeriram a existência entre os efeitos de cariótipo e temperatura para forma da asa, mas nao para tamanho, indicando a presença de interação genotipo-ambiente para forma da asa em D. mediopunctata. Sugerimos que outros fatores ecológicos ¿ tais como densidade de larvas ¿ ou variação sazonal de conteúdo genético das inversões poderia explicar os resultados anteriores. Alem disso, uma nova hipótese filogenética para a radiação tripunctata e sugerida com base em dados de seqüências dos genes mitocôndrias das subunidades I e II da citocromo oxidase, e a variação de tamanho e forma da asa e descrita com bases na nova hipótese filogenética. As arvores filogenéticas foram reconstruídas por métodos de parcimônia, máxima verossimilhança e inferência Bayesiana. Os resultados rejeitaram a hipótese de monofila para o grupo tripunctata, enquanto esta hipótese não foi rejeitada para a radiação tripunctata e outros grupos específicos dentro da radiação. Ambos tamanho e forma da asa apresentaram sinal filogenético e diferentes padrões de tamanho e forma puderam ser identificados para cada um dos agrupamentos mais importantes detectados pela analise filogenética
Abstract: The tripunctata group is the second largest Neotropical group of Drosophila in number of species and was included in the tripunctata radiation ¿ which comprises other closely related groups. The second chromosome of Drosophila mediopunctata (a species that belongs to the tripunctata group) is highly polymorphic for inversions. Previous work suggested the presence of genotype-environment interaction for wing size but not for shape. We performed experiments in the laboratory to test for the joint effects of temperature and chromosome inversions on size and shape of the wing in D. mediopunctata. Wing morphology was analyzed by methods of geometric morphometrics. Our findings show that wing size and shape are influenced by temperature, sex, and karyotype. We also found evidence suggestive of an interaction between the effects of karyotype and temperature on wing shape (but not for size), indicating the existence of genotype-environment interaction for wing shape in D. mediopunctata. We suggest that other ecological factors ¿ such as larval crowding ¿ or seasonal variation of genetic content within inversions may explain the previous results. Moreover, we suggest a new phylogenetic hypothesis for the tripunctata radiation based on sequences of mitochondrial genes of cytochrome oxidase subunits I and II, and describe wing size and shape variation in different species based on this new phylogenetic hypothesis. Phylogenetic trees were reconstructed by parsimony, maximum likelihood and bayesian inference. Results reject the monophyly hypothesis for the tripunctata group whereas monophyly is not rejected for the tripunctata radiation and other specific groups within the radiation. Both wing size and shape displayed phylogenetic signal and different patterns of size and shape could be identified for each of the most important clusters detected by phylogenetic analysis
Doutorado
Genetica Animal e Evolução
Doutor em Genetica e Biologia Molecular
Chardard, Dominique. "Séquences homologues au gène sry et activité de l'aromatase lors de la différenciation du sexe des gonades et de leurs inversions sexuelles par la température ou par les hormones stéroïdes chez pleurodèles Waltl (Amphibien Urodèle)." Nancy 1, 1996. http://docnum.univ-lorraine.fr/public/SCD_T_1996_0118_CHARDARD.pdf.
Повний текст джерелаPäällysaho, S. (Seliina). "Contribution of X chromosomal and autosomal genes to species differences in male courtship songs of the Drosophila virilis group species." Doctoral thesis, University of Oulu, 2001. http://urn.fi/urn:isbn:9514265831.
Повний текст джерелаDorazi, Robert. "Construction d'un modèle théorique de l'inversion sexuelle chez le pleurodèle : caractérisation d'un antigène ovocytaire (p55) chez pleurodèles waltl." Nancy 1, 1995. http://www.theses.fr/1995NAN10143.
Повний текст джерелаHayes, Matthew. "Algorithms to Resolve Large Scale and Complex StructuralVariants in the Human Genome." Case Western Reserve University School of Graduate Studies / OhioLINK, 2013. http://rave.ohiolink.edu/etdc/view?acc_num=case1372864570.
Повний текст джерелаBosch, Pages Nina. "Duplicacions segmentàries a la regió cromosòmica humana 8P23.1: evolució i expansió d'una nova família gènica." Doctoral thesis, Universitat Pompeu Fabra, 2008. http://www.tdx.cat/TDX-0521109-141419.
Повний текст джерелаEl treball realitzat en aquesta tesi doctoral pretén aprofundir en la caracterització de la complexa arquitectura genòmica d'aquesta regió. En la nostra primera aproximació a l'estudi de les DSs que flanquegen la regió cromosòmica 8p23.1, es va identificar una nova família gènica específica de primats, la família gènica FAM90A.Així, bona part d'aquesta tesi doctoral està centrada en l'anàlisi de l'origen, formació, evolució i expansió de FAM90A en els homínids.
Per altra banda també s'ha analitzant en detall la variabilitat de FAM90A com a variant en número de còpia (CNV) en diferents poblacions humanes.
Finalment, s'ha establert la freqüència de la inversió que afecta a 8p23.1 en població espanyola. També s'ha procedit a genotipar diversos individus homozigots per la inversió i s'ha predit l' estatus de la inversió en 150 individus del projecte HapMap i s'ha analitzat l'efecte que té aquesta reorganització sobre els nivells d'expressió dels gens de la regió.
Segmental duplications (SDs), also known as duplicons or Low Copy Repeats (LCRs), are regions of a minimum of 1 kb with a high sequence identity level (>90%), which are present at least two times in the genome. The 8p23.1 region extends 6.5 Mb at the distal part of the short arm of chromosome 8 and it is flanked by segmental duplications. Due to its genomic architecture the region is prone to suffer rearrangements mediated by non-allelic homologous recombination between these SDs, such as the polymorphic inversion of 8p23.1 [inv(8)(p23)], which is present in one out of every four of European and Japanese general population individuals, as well as other less frequent rearrangements.
The aim of the work presented in this doctoral thesis is to get insights in the characterization of the genomic architecture of this complex region. Our first approach to study the SDs flanking 8p23.1 region resulted in the identification of a novel gene family which is primate specific, the FAM90A gene family. Thus, this doctoral thesis is mainly focused on the analysis of the origins, formation, evolution and expansion of FAM90A in hominoids.
It has also been analyzed in detail the variability of FAM90A as a copy number variant (CNV) in different human populations.
Finally, it has been established the frequency of the inversion affecting 8p23.1 region in the Spanish population. Several homozygous inverted individuals have been genotyped and the status for the inversion has been predicted for 150 HapMap individuals, as well as the effect of this rearrangement on the gene expression levels of the genes contained in the region.
Guerrero, Rafael Felipe. "Models and analyses of chromosome evolution." 2013. http://hdl.handle.net/2152/21626.
Повний текст джерелаtext
Yue, Ying [Verfasser]. "[Breakpoint analysis of human chromosome 3 inversions during hominoid evolution] / Ying Yue." 2005. http://d-nb.info/976057794/34.
Повний текст джерелаCasey, Graham M. "Linkage analysis of a kindred segregating an inversion of chromosome 3." 1991. http://hdl.handle.net/1993/17330.
Повний текст джерелаCardoso, Manuela Pinto. "Molecular pathogenesis of a malformation syndrome associated with a pericentric chromosome 2 inversion." Master's thesis, 2017. http://hdl.handle.net/10451/27503.
Повний текст джерелаAs síndromes de malformação congénitas são um dos principais grupos de patologias que afetam neonatos e crianças em países desenvolvidos. Muitos destes casos têm como base genética os arranjos genómicos ou cromossómicos. No entanto, por norma, devido à complexidade inerente às síndromes de malformação, é difícil e laborioso identificar com exatidão a alteração molecular que lhes deu origem. Aliado à inexistência atual de um genoma humano completamente anotado, torna-se complicado a compreensão e a previsão das consequências fenotípicas dos rearranjos cromossómicos. As inversões cromossómicas são rearranjos que ocorrem quando dois pontos de quebra ocorrem num mesmo cromossoma e são reinseridos invertidos, sem alteração de número de cópia. Normalmente as inversões são subclínicas, sem um fenótipo clínico associado. Se estes forem transmitidos a mais de 1% de uma dada população, tratam-se de polimorfismos. Se um rearranjo afectar transcritos ou a arquitetura genética junto dos pontos de quebra, perturbando assim o normal funcionamento dos genes, sobretudo os de expressão indispensável, este estará envolvido na etiologia de uma patologia potencialmente grave. Comparado com outros rearranjos cromossómicos, são poucas as inversões atualmente detalhadamente caracterizadas, frequentemente devido a dificuldades técnicas relacionadas com regiões repetitivas, frequentes nos pontos de quebra das inversões. Metodologias clássicas de citogenética são de baixa resolução e por vezes incapazes de identificar determinadas anomalias estruturais. As tecnologias atualmente mais avançadas para o estudo de rearranjos incluem microarrays genómicos, ideal na análise de variações no número de cópias, e a sequenciação de próxima geração (NGS), mais concretamente sequenciação pangenómica, para a generalidade dos rearranjos cromossómicos. Esta última tem a particularidade de ser eficiente na identificação de alterações crípticas, de oferecer uma potencial resolução bastante elevada (em certos casos nucleotídica) e de gerar grande quantidade de dados rapidamente. Das plataformas NGS existentes, as mais aptas para a análise de inversões envolvem a construção de bibliotecas mate-pair de grandes insertos, cuja distância entre pares de leitura é de 2 a 6 kb, permitindo superar dificuldades técnicas com zonas repetitivas e pequenas alterações junto aos pontos de quebra. Esta tese pretende identificar as alterações moleculares responsáveis pela síndrome de malformação congénita num indivíduo portador de uma inversão cromossómica pericêntrica aparentemente equilibrada de origem materna. O caso índex, portador da síndrome de malformação, apresenta acentuado atraso de desenvolvimento mental e psicomotor, dismorfia facial e perturbações do espectro do autismo. Ele tem muito baixo peso e altura para a idade. Foram também diagnosticadas cardiopatias, criptorquidia, escoliose e hipotonia generalizada. Estudos citogenéticos detetaram a existência de uma inversão pericêntrica no cromossoma 2, também encontrada na mãe. Os pais têm fenótipo aparentemente normal. Primeiramente, procedeu-se à identificação de alterações estruturais desequilibradas no indivíduo índex. Foram detetaram várias alterações de número de cópia, na maioria pequenas (< 100kb) e sem envolver genes OMIM, com a exceção da duplicação de 590 kb em 2q21.1. Os genes na duplicação não aparentam estar relacionados com o fenótipo observado. Ademais, foi detetado uma duplicação de 610 kb no pai nesta mesma região genómica, sugerindo que se trata de uma alteração de origem paterna, muito provavelmente não-patogénica e possivelmente de natureza polimórfica. Sequenciação pangenómica de grandes insertos (large-insert whole-genome sequencing) usando ácido desoxirribonucleico (ADN) do caso índex foi realizada para a identificação dos pontos de quebra da inversão no cromossoma 2. Uma vez delimitado a região dos pontos de quebra por NGS, foram desenhados oligonucleotídeos específicos para a amplificação dos fragmentos de junção e, seguidamente, procedeu-se à análise de segregação familiar e determinação nucleotídica dos pontos de quebra através de sequenciação Sanger. O estudo do perfil de expressão genética foi feito com Human Transcriptome Assay (HTA 2.0) da Affymetrix, utilizando ácido desoxirribonucleico (ARN) da linha celular linfoblastóide do indivíduo índex. Os dados obtidos por NGS permitiram a redefinição da localização genómica da inversão. O cariótipo do caso índex foi assim redefinido como 46, XY, inv(2)(p16.1q14.3)mat. Os pontos de quebra da inversão no cromossoma 2, no caso índex e na sua mãe, foram determinados. Estes localizam-se na posição chr2:55,935,064 e chr2:123,767,685 (GRCh37), respetivamente, nas bandas p16.1 e q14.3. Na sequência invertida ocorreu a deleção de 5 bases. Os pontos de quebra da inversão são iguais em ambos os indivíduos, sem quaisquer alterações detetadas nos fragmentos de junção. Segundo a nomenclatura baseada em citogenética de próxima geração, esta inversão é descrita como seq[GRCh37] inv(2)(pter→2p16.1(55,935,06{1-3})::2q14.3(123,767,68{3-1})→2p16.1 (55,935,06{5-4})::2q14.3(123,767,68{4-5})→qter). Os pontos de quebra não interrompem diretamente genes conhecidos. Em inv2p16.1, este é flanqueado a 5’ pelo gene polirribonucleotídeo nucleotidiltransferase 1 (PNPT1; chr2:55,861,198-55,921,045, GRCh37; OMIM *610316), e a 3’ pelo gene proteína 1 da matriz extracelular tipo-fibulina contendo EGF (EFEMP1; chr2:56,093,097-56,151,298, GRCh37; OMIM *601548) a 158 kb. O PNPT1 está envolvido na cadeia respiratória mitocondrial. Mutações em homozigotia foram associadas com deficiência na fosforilação oxidativa (OMIM #614932), originando nomeadamente encefalopatias, e com a surdez hereditária autossómica recessiva 70 (OMIM #614934). Em murganhos, tem expressão acentuada na cóclea. EFEMP1 é essencial para a correta formação de fibras elásticas em tecido conjuntivo, tendo elevada expressão nos pulmões e esófago em murganhos, e baixa no cérebro e coração. Mutações neste gene estão descritas como causa genética da distrofia da retina de Doyne (OMIM #126600), patologia autossómica dominante com início na segunda década de vida, causando perda progressiva de visão. O ponto de quebra em inv2q14.3 situa-se numa região pobre em genes. O gene translina (TSN; chr2:122,513,120-122,525,428, GRCh37; OMIM *600575) franqueia o ponto de quebra proximamente a 1240 kb, enquanto o gene tipo-proteína associada à contatina 5 (CNTNAP5; chr2:124,782,863-125,672,953, GRCh37; OMIM *610519) localiza-se 1020 kb distal do ponto de quebra. TSN codifica uma proteína que reconhece sequências-alvo em junções de pontos de quebra de translocações em doentes com leucemia, e está envolvido no mecanismo de reparação de ADN e transporte de ARN em neurónios. Em murganhos, expressa-se preferencialmente no tecido adiposo. O CNTNAP5 produz uma proteína que atua no sistema nervoso como moléculas de adesão celular e de recetor na comunicação intercelular. Em murganhos, expressa-se predominantemente no sistema nervoso. Existe suspeita de que mutações pontuais possam conferir suscetibilidade a comportamentos do espectro do autismo. Quanto à expressão genética, os resultados mostraram que os genes que flanqueiam a inversão não aparentam ter nível de expressão significativamente alterada comparativamente com os controlos. O estudo aprofundado de expressão a nível genómico está a decorrer. Os restantes genes próximos dos pontos de quebra da inversão relevaram baixa probabilidade de serem as alterações causadoras do fenótipo, nomeadamente a nível das doenças associadas. Tendo em conta os resultados obtidos, especialmente a confirmação da origem materna da inversão, esta alteração não aparenta ser a principal e única causa molecular do fenótipo. Ademais, esta conclusão é suportada pela pouca sobreposição clínica dos genes flanqueadores com a síndrome de malformação congénita, e da expressão génica aparentemente não alterada. Assim, atualmente, a relação causal entre o fenótipo observado e a inversão no cromossoma 2 foi excluída. Esta inversão é muito provavelmente não-patogénica por si só. Até ao momento e com os dados disponíveis, não foi possível identificar genes candidatos nem as alterações moleculares por detrás da síndrome de malformação congénita no caso índex. Informação médica disponível exclui influência de fatores ambientais na embriogénese. Futuramente, sugere-se recorrer à sequenciação do exoma, visto que tem uma sensibilidade muito superior para a deteção de pequenas em exões, potencialmente não detestáveis pelas abordagens até ao momento utilizadas. Adicionalmente, o estudo nos restantes membros da família permitirão obter uma melhor visão sobre a segregação familiar.
Congenital malformation syndromes can be caused by genomic and/or chromosome rearrangements. It is difficult to establish the underlying causes of malformations because of their high level of complexity. Although balanced chromosome inversions are in most cases subclinical, those disrupting transcripts or affecting the genomic architecture at breakpoint regions may well be pathogenic. Currently, the lack of a fully annotated human genome hinders the predictability of the phonotypic consequences of such rearrangements. The aim of this study is the identification of potential candidate genes for a malformation syndrome in an individual with an apparently balanced maternally inherited pericentric chromosome inversion inv(2)(p16.1;q14.3)mat. The proband has severe congenital malformation with multiple psychomotor and developmental anomalies, dismorphism and autistic features. The parents are phenotypically normal. Classical cytogenetic methods are of low resolution, often in the magnitude of a 5 to 10 Mb. Whole-genome Next-Generation Sequencing (NGS) of large-insert sequencing library (liWGS) has the capability to detect structural rearrangements with incomparably higher resolution, including cryptic alterations. As consequence, it was applied for the identification of inv(2)(p16.1;q14.3) breakpoints in the proband. Familial segregation analysis and definition of the inversion breakpoints at a nucleotide resolution were performed by amplification of junction fragments and Sanger sequencing. Genome and transcriptome array analysis were also carried out, for detection of additional genomic alterations and for gene expression profiling, respectively. Additionally, a possibly polymorphic duplication at 2q21.1, inherited from his father, was found. No apparent pathogenic genomic imbalances were identified in the proband. The inversion breakpoints are located at chr2:55,935,064 and chr2:123,767,685 (GRCh37), respectively, in 2p16.1 and 2q14.3. The inv2p16.1 breakpoint is flanked 14 kb proximal by the gene polyribonucleotide nucleotidyltransferase 1 (PNPT1; chr2:55,861,198-55,921,045, GRCh37; OMIM *610316) and 172 kb distal by EGF containing fibulin-like extracellular matrix protein 1 (EFEMP1; chr2:56,093,097-56,151,298, GRCh37; OMIM *601548). PNPT1, highly expressed in mice cochlea, has been associated with deafness (OMIM #614934) and with combined oxidative phosphorylation deficiency (OMIM #614932), both autosomal recessive. Meanwhile, the autosomal dominant Doyne honeycomb retinal dystrophy (OMIM #126600) is reported to be associated with mutations in EFEMP1. This gene is essential for the formation of elastic fibers in connective tissue. The 2q14.3 breakpoint is in a gene-poor region. Located 1.2 Mb proximal to the breakpoint is translin (TSN; chr2:122,513,120-122,525,428, GRCh37; OMIM *600575). Involved in DNA damage repair and RNA trafficking in neurons, TSN codes for a protein that specifically binds to breakpoint junctions of translocations in acute leukemia. The gene contactin-associated protein-like 5 (CNTNAP5; chr2:124,782,863-125,672,953, GRCh37; OMIM *610519) is localized 1 Mb, distal. CNTNAP5 is involved in cell adhesion and intercellular communication. Susceptibility to autistic syndromes has been suspected. The above described breakpoints at nucleotide resolution are the same in the proband’s mother, and did not directly disrupt any gene. Publicly available clinical information on alterations affecting the inversion flanking genes revealed no major similarity with the proband’s phenotype. Furthermore, no significant alteration in their expression level was observed. In-depth analysis of genome-wide expression data is in progress. Based on these findings, the causal relationship between clinical phenotype and the inv(2)(p16.1;q14.3) is most likely excluded, since the inversion is most likely non-pathogenic. Therefore it is not yet possible to identity the underlying genetic cause of the malformation syndrome reported in this subject. Whole-exome sequencing is proposed as a future task to detect the disease causing alteration. This study highlights the application of NGS-based methodology, with its capability in mapping chromosome inversion breakpoints at a very high resolution. Large scale application of this approach will represent a hallmark in the characterization of congenital malformations associated with structural chromosomal abnormalities.
Yang, Yeng-Yuh, and 楊永裕. "The interaction between chromosomal inversions and recessive let- hal alleles in Drosophila." Thesis, 1996. http://ndltd.ncl.edu.tw/handle/79712113701016105867.
Повний текст джерелаHenderson, Karen Gwen. "Characterization of an inversion duplication of human chromosome 8 by fluorescent in situ hybridization." Thesis, 1992. http://hdl.handle.net/2429/3323.
Повний текст джерелаAlves, João Miguel Fernandes. "Understanding the impact of chromosomal inversion on the evolution of the human genome." Tese, 2014. https://repositorio-aberto.up.pt/handle/10216/77298.
Повний текст джерелаAlves, João Miguel Fernandes. "Understanding the impact of chromosomal inversion on the evolution of the human genome." Doctoral thesis, 2014. https://repositorio-aberto.up.pt/handle/10216/77298.
Повний текст джерелаTung, Shih-Fan, and 董詩凡. "Association between Chromosomal Inversion Polymorphisms and Accumulation of Recessive Deleterious Mutations in Drosophila melanogaster." Thesis, 2012. http://ndltd.ncl.edu.tw/handle/66773674668407138286.
Повний текст джерела國立臺灣大學
生態學與演化生物學研究所
100
Chromosomal inversion polymorphisms have been demonstrated to play adaptive roles in natural populations by capturing local co-adapted alleles within recombination-suppressed regions of inversion heterozygotes. On the other hand, a less studied but important role of inversion polymorphisms is that recombination suppression by heterozygous chromosomal rearrangement may accumulate recessive deleterious mutations and thus cause a great amount of mutation load. Deleterious mutations will be eliminated when homozygotes and in turn increase heterozygosity of various inversions. The Afrotropical population of Drosophila melanogaster with high chromosomal inversion heterozygosity and high ratio of recessive lethals provides an ideal material to test any association between them by examining the accumulation pattern of recessive lethals. Recessive lethals are predicted to locate near the inversion breakpoints where the recombination is greatly suppressed by inversion heterokaryotypes. By using recombination and deficiency mappings, 14 recessive lethal alleles from eight lethal-bearing third chromosomes (each from eight distinct isofemale lines, respectively) were identified. All of recessive lethals were mapped into the regions close to (less than 3 centi-Morgan) the inversion breakpoints which were polymorphic in the African population. This result clearly shows that recessive lethal alleles are accumulated by recombination suppression and distributed non-randomly along inverted chromosomes. The data also provide the strong association between chromosomal inversions and the accumulation of recessive deleterious mutations.
Dutta, Usha Rani [Verfasser]. "Molecular characterization of a pericentric inversion of chromosome 3 in a 3-generation family with short stature / von Dutta Usha Rani." 2008. http://d-nb.info/994457936/34.
Повний текст джерелаLowry, David Bryant. "Integrating genetics, geography, and local adaptation to understand ecotype formation in the yellow monkeyflower, Mimulus guttatus." Diss., 2010. http://hdl.handle.net/10161/2383.
Повний текст джерелаSpeciation is a constantly ongoing process whereby reproductive isolating baririer build up over time until groups of organisms can no longer exchange genes with each other. Adaptation is thought to play a major role in the formation of these barriers, although the genetic mechanisms and geographic mode underlying the spread of barriers due to adaptive evolution is poorly understood. Critically, speciation may occur in stages through the formation of intermediate partially reproductively isolated groups. The idea of such widespread ecotypes has been the subject of great controversy over the last century. Even so, we have relatively little understanding about whether widespread ecotypes exist, wheather they are reproductively isolated, and how adaptive alleles are distributed among partially isolated groups. In this dissertation, I examined these issues in widespread coastal perennial and inland annual ecotypes of the yellow monkeyflower, Mimulus guttatus. First, I determined that coastal and inland populations comprise distinct ecotypic groups. I then determined that these ecotypes are adapted to their respective habitats through genetically based flowering time and salt tolerance differences. I assessed the genetic architecture of these adaptations through quantitative trait loci (QTL) analysis and determined the geographic distribution of the underlying alleles through latitudinally replicated mapping populations. I quantified the contribution of these loci to adaptation in the field through the incorporation of advance generation hybrids in reciprocal transplant experiments. In the process, I discovered a widespread chromosomal inversion to be involved in the adaptive flowering time and annual/perennial life-history shift among the ecotypes. Overall, the results of this study suggest that widespread reproductively isolated ecotypes can form through the spread adaptive standing genetic variation between habitats and that chromosomal rearrangements can integral to this process.
Dissertation