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Hernandez-Sanchez, Jules. "Gene mapping using linkage disequilibrium". Thesis, University of Edinburgh, 2002. http://hdl.handle.net/1842/14058.
Pełny tekst źródłaVeroneze, Renata. "Linkage disequilibrium and genomic selection in pigs". Universidade Federal de Viçosa, 2015. http://www.locus.ufv.br/handle/123456789/7597.
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A seleção genômica (SG) e associação genômica ampla (GWAS) são métodos que exploram o desequilíbrio de ligação (LD) entre marcadores e loci de características quantitativas (QTL). Um dos fatores limitantes para a implementação da SG é a necessidade de um grande número de animais genotipados e fenotipados para obtenção de valores genéticos com alta acurácia. Essa limitação pode ser superada combinando dados de múltiplas populações ou utilizando dados de animais cruzados. O objetivo geral desta tese foi caracterizar os padrões de LD de diferentes populações de suínos. Além disso, avaliar em que medida as diferenças de LD se refletem na acurácia da seleção genômica quando utilizadas diferentes metodologias e arranjos para população de referência e validação. Os arranjos testados foram: utilização de subconjuntos da mesma população como referência e validação (within), populações diferentes nos conjuntos de referência e validação (across) e combinação de duas populações na referência (multi). Nessa tese foram utilizados dados de suínos de linhas puras e de animais cruzados, genotipados com o PorcineSNP60 BeadChip. A regressão Loess proporcionou melhor ajuste aos dados de LD, bem como em predições mais acuradas em comparação a regressão não linear. Mostrou-se também, que a regressão Loess pode ser utilizada para realizar uma comparação estatística do LD decay de diferentes populações. A persistência de fase do LD entre animais cruzados e as linhas puras parentais foi alta, o que nos leva a hipotetizar que associações marcador-QTL similares poderiam ser encontradas em animais cruzados e as linhas parentais e, portanto, esperava-se encontrar altas acurácias de predição genômica entre essas populações. Entre as linhas puras a persistência de fase foi baixa, logo painéis de SNPs de maior densidade deveriam ser utilizados para manter a mesma associação marcador-QTL entre essas linhas. Acurácias obtidas na predição genômica utilizando animais cruzados assim como os arranjos across e multi, não seguiram as expectativas baseadas em LD. Portanto, a consistência de fase de ligação entre populações pode não ser tão importante para a acurácia da seleção genômica como se pensava, mas sim a ação combinada de LD, arquitetura genética e frequências alélicas. Portanto, foi desenvolvida uma metodologia que leva em consideração differenças nas frequências alélicas, bem como informações dos GWAS para comtemplar a arquitetura genética da característica. Esta estratégia trouxe alguns benefícios para a predição genônima para os arranjos within e multi. Ponderações obtidas por meio de GWAS em diferentes conjuntos de dados (uma única população e combinando múltiplas populações) nem sempre resultou em aumento da acurácia, sendo dependente da linha que estava sob seleção. O uso de pesos advindos do GWAS ao se utilizar uma população combinada resultou nas melhores acurácias tanto para os arranjos within quanto multi. A avaliação e o entendimento de como diferenças de LD, frequências alélicas e arquitetura genética afetam a acurácia da predição genômica é fundamental para otimizar a inserção da seleção genômica no melhoramento de suínos.
Genomic selection and genomic wide association studies (GWAS) are widely used methods that aim to exploit the linkage disequilibrium (LD) between markers and quantitative trait loci (QTL). Securing a sufficiently large set of genotypes and phenotypes can be a limiting factor when implementing genomic selection that may be overcome by combining data from multiple populations or using crossbred information. The overall objective of this thesis was to characterize LD patterns in different pig populations and to evaluate whether the differences in LD determine the accuracy of genomic predictions when using different reference sets (within-, across- and multi- population) and methodologies. In this thesis I used data from pure lines and crossbred pig populations genotyped with PorcineSNP60 BeadChip. Loess regression provided a better fit to the real LD data, and more accurate LD predictions could be made, compared to nonlinear regression. It was also shown that Loess regression can be used to statistically compare the LD decay of different populations. The persistence of LD phase between crosses and the parental pig lines was found to be high, from which it was hypothesized that similar marker-QTL associations would be found in a cross and in their purebred parent populations and therefore accuracies of genomic prediction across these populations should be high. Between the pure lines the persistence of phase was low, thus higher density panels should be used to have the same marker-QTL associations across these lines. Accuracies obtained from across- and multi-population genomic prediction and from using crossbred data did however not follow the expectations based on LD. Having the same LD phase may therefore not be as important for genomic prediction accuracy as previously thought but rather the interplay between LD, genetic architecture and allele frequencies also plays a major role. Differences in allele frequencies between lines and information from GWAS on the genetic architecture of traits for the different lines were taken into account in analyses developed in the later chapters. The use of weights, based on GWAS results, was expected to lead the GBLUP model towards the real genetic architecture of the traits. This strategy was shown to have some benefit for the genomic predictions with single- and multi-population data sets. Weights obtained from GWAS in different data sets (within and combining populations) did not always lead to increased accuracies of prediction, depending on which lines the weights are applied to. Using weights from GWAS in a combined population was the best approach, resulting in higher accuracy of GBLUP predictions within single- as well as in multi-population analysis. Understanding and evaluating how the accuracy of within-, across- and multi-population genomic prediction is affected by differences in LD, in genetic architecture and in allele frequencies is key to optimize the accuracy of genomic prediction in pig breeding.
Liu-Cordero, Shau Neen 1970. "Patterns of linkage disequilibrium in the human genome". Thesis, Massachusetts Institute of Technology, 2002. http://hdl.handle.net/1721.1/89344.
Pełny tekst źródłaIncludes bibliographical references.
Although enormous progress has occurred in the field of human genetics, the cloning of complex trait mutations remains a challenging and unresolved process. This continuing difficulty is responsible for an ever-increasing awareness of the phenomenon of linkage disequilibrium (LD). The principle behind LD is relatively simple. Over the lifetime of a population, the genetic markers that are adjacent to an ancestral mutation will recombine less often than more distant markers. Therefore, the ancestral alleles of the markers closest to the mutation should be most frequent in a collection of disease chromosomes. The allelic association should decrease as the distance from the ancestral disease mutation increases. This thesis is a collection of ideas and experiments aimed at dissecting the behavior of LD in the human genome. Specific studies examine LD in a variety of populations including isolated founder populations, as well as globally diverse population samples. A large number of regions throughout the genome are investigated using both pairwise comparisons of markers, as well as multimarker haplotypes. The X chromosome is more closely scrutinized because of its unique population history, as well as the advantages afforded to haplotyping due to hemizygosity of the X chromosome in males. Major conclusions include the observation that LD between pairs of markers is highly variable even at extremely close distances and multimarker haplotypes better serve to resolve the underlying haplotype structure of the genome.
(cont.) The genome appears to be structured as blocks of limited haplotype diversity that do not exhibit much internal recombination but which are separated by segments that show little or no LD. The lack of LD between haplotype blocks appears to be due to clustering of recombination events into specific hotspots. The size of the blocks and haplotype diversity varies slightly by population. In addition, the identity of the haplotypes varies between populations. The existence of 3-4 major haplotypes for specific regions in a diverse human population sample is a surprising finding that was originally believed to have only existed in very special isolated and young populations.
by Shau Neen Liu-Cordero.
Ph.D.
Li, Na. "Modeling and inference for linkage disequilibrium and recombination /". Thesis, Connect to this title online; UW restricted, 2003. http://hdl.handle.net/1773/9532.
Pełny tekst źródłaCummings, James Rowland Fraser. "Linkage Disequilibrium Mapping of Chromosome 19 on Crohn's Disease". Thesis, University of Oxford, 2009. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.531666.
Pełny tekst źródłaLawrence, Robert W. "Characterizing patterns of linkage disequilibrium in the human genome". Thesis, University of Oxford, 2006. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.496992.
Pełny tekst źródłaHolloway, J. Kim. "Linkage disequilibrium and meiotic recombination in the human genome". Thesis, University of Leicester, 2005. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.426035.
Pełny tekst źródłaDale, Kuys Ruth. "Linkage disequilibrium in the South African abalone, Haliotis midae". Thesis, Stellenbosch : Stellenbosch University, 2015. http://hdl.handle.net/10019.1/97991.
Pełny tekst źródłaENGLISH ABSTRACT: Linkage disequilibrium (LD) is defined as the non-random association of alleles at two or more loci within a population. It is sensitive to a variety of locus-specific- and demographic factors, and can thus provide much insight into the micro-evolutionary factors that have shaped species of interest. It can also be exploited to identify the genomic regions determining complex traits of interest, which can then be applied as performance evaluation markers in marker-assisted selection (MAS). The South African abalone, Haliotis midae, supports a rapidly developing aquaculture production industry, in which genetic improvement potential is high. This species also represents an opportunistic model for studying the effects of early domestication in a shellfish species. The aim of this study was therefore to quantify and characterise levels of genome-wide LD within the South African abalone, and to demonstrate its utility within population genetic investigations and the characterisation of complex traits. Estimates of LD between 112 mapped microsatellite markers within wild and cultured H. midae revealed that levels of LD in abalone are high relative to other aquaculture species. This was attributed primarily to small effective population sizes produced by a combination of natural- and anthropogenic factors. The decay of LD with genetic distance was evident in both cultured cohorts, but almost absent in wild cohorts, likely reflecting the differences in size, age and sampling of wild populations relative to cultured. Putative evidence for the effects of recombination, selection, and epistasis were also evident in distinctive locus-specific patterns of LD on some of the linkage groups, many of which could represent the effects of domestication. The effects of selection associated with the domestication event were further investigated using a candidate locus LD mapping approach to determine the proportion of candidate loci under selection associated with artificial selection for faster growth rate in cultured abalone. Two loci (15%) were found to be significantly associated with differences in size of individual animals, both of which could be linked with genes potentially involved in growth and development. These markers could therefore find application in MAS programmes for abalone. Several promising candidates for natural selection were also identified based on similarity with known genes. As the latter represented the majority, natural selection, rather than artificial selection, appears to be predominant during the early stages of domestication in abalone. While some conclusions within the current study were speculative, both the direct and indirect applications of LD were clearly demonstrated. Linkage disequilibrium data can provide a unique perspective on many of the commonly used population genetic estimates, and is therefore of great value in population genetic investigations. Furthermore, these results also highlighted the effectiveness of the candidate locus approach in species with both limited molecular resources and extensive LD.
AFRIKAANSE OPSOMMING: Koppelingsonewewig (KO) word gedefinieer as die nie-lukrake assosiasie van allele by twee of meer lokusse binne 'n populasie. Koppelingsonewewig is sensitief vir 'n verskeidenheid van lokus-spesifieke- en demografiese faktore, en kan dus insiggewend wees m.b.t. mikro-evolusionêre faktore wat spesies van belang beïnvloed het. Dit kan ook benut word om die genoom-gebiede onderligend tot komplekse eienskappe te bespeur; wat dan aangewend kan word vir prestasie-evaluering m.b.v. merkerbemiddelde seleksie (MBS). Die Suid-Afrikaanse perlemoen, Haliotis midae, ondersteun 'n vinnig ontwikkelende akwakultuur produksie bedryf, waarin genetiese verbeteringspotensiaal hoog is. Hierdie spesie verteenwoordig ook 'n opportunistiese model vir die bestudering van die gevolge van vroeë domestiseering in 'n skulpvis spesie. Die doel van hierdie studie was dus om vlakke van genoom-wye KO binne die Suid-Afrikaanse perlemoen te kwantifiseer en te karakteriseer, en om die toepassing hiervan binne populasiegenetiese ondersoeke en die karakterisering van komplekse eienskappe te demonstreer. Ramings van KO tussen 112 gekarteerde mikrosatelliet-merkers binne wilde en gekultiveerde H. midae het aan die lig gebring dat die vlakke van KO in perlemoen hoog was, in vergelyking met ander akwakultuur spesies. Dit word hoofsaaklik toegeskryf aan klein effektiewe populasiegroottes wat deur 'n kombinasie van natuurlike- en antropogeniese faktore teweeg gebring word. Die verval van KO met genetiese afstand was duidelik waarneembaar in gekultiveerde kohorte, maar amper afwesig in die wilde kohorte, waarskynlik a.g.v. verskille in populasiegrootte, ouderdom, en streekproef-neemings metodieke van die verskeie populasies. Vermeende bewyse vir die gevolge van rekombinasie, seleksie en epistase kon ook gesien word a.g.v. lokus-spesifieke patrone van KO op sommige van die koppelingsgroepe, moontlik ‘n gevolg van domestisering. Die gevolge van seleksie wat verband hou met die domestiseringsgebeurtenis is verder ondersoek m.b.v 'n kandidaat-lokus KO karteringsbenadering om die verhouding van kandidaat lokusse wat geassosieer is met kunsmatige seleksie (vir vinniger groeikoers in perlemoen) te bepaal. Twee lokusse (15%) was beduidend geassosieer met verskille in grootte tussen individuele diere. Beide van die lokusse was gekoppel met gene wat potensieel betrokke is by groei en ontwikkeling. Hierdie merkers kan dus moontlik aangewend word in MBS programme vir perlemoen. Verskeie belowende kandidaat lokusse vir natuurlike seleksie is ook geïdentifiseer gebaseer op ooreenkoms met bekende gene. Gegewe dat die laasgenoemde die meerderheid van die merkers verteenwoordig, kan daar afgelei word dat natuurlike seleksie, eerder as kunsmatige seleksie, oorheersend is in die vroeë stadia van domestisering in perlemoen. Terwyl sommige gevolgtrekkings binne die huidige studie spekulatief was, is beide die direkte en indirekte toepassings van KO duidelik gedemonstreer. Koppelingsonewewig-data kan 'n unieke perspektief gee op baie van die algemeen gebruikte populasie genetiese skattings, en is dus van groot waarde in populasie genetiese ondersoeke. Verder demonstreer hierdie resultate ook die doeltreffendheid van die kandidaat lokus benadering in spesies met beide beperkte molekulêre hulpbronne en uitgebreide KO.
Sjölander, Anders. "Exploring linkage disequilibrium to date admixture using ancient DNA". Thesis, Uppsala universitet, Växtekologi och evolution, 2016. http://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-298198.
Pełny tekst źródłaWebb, Adam J. "Meiotic recombination and linkage disequilibrium in the human genome". Thesis, University of Leicester, 2006. http://hdl.handle.net/2381/30369.
Pełny tekst źródłaZaffaroni, Daniela. "Mapping of skin cancer susceptibility loci in mice". Thesis, Open University, 2003. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.270016.
Pełny tekst źródłaKim, Yunjung. "Analysis of Multilocus Linkage Disequilibrium Structure in the Human Genome". NCSU, 2008. http://www.lib.ncsu.edu/theses/available/etd-03132008-075346/.
Pełny tekst źródłaJohnson, Randall. "Modeling of linkage disequilibrium in whole genome genetic association studies". Thesis, Paris, CNAM, 2014. http://www.theses.fr/2015CNAM0963/document.
Pełny tekst źródłaGWAS is an essential tool for disease gene discovery, but has severe problems of statistical power when it is impractical to genetically sample tens of thousands of subjects. The results presented here—a novel, effective correction for local ancestral population LD allowing use of dense markers in MALD using the ALDsuite and the demonstration that the simpleM method provides an optimum Bonferroni correction for multiple comparisons in GWAS, reiterate the value of PCA for capturing the essential part of the complexity of high- dimensional systems. PCA is already standard for correcting for population substructure in GWAS; my results point to it’s broader applicability as a general strategy for dealing with the high dimensionality of genomic association data
Thunga, Venkata Raghava Pavankumar. "Nucleotide diversity and Linkage disequilibrium in Norway spruce (Picea abies)". Thesis, Uppsala universitet, Institutionen för biologisk grundutbildning, 2014. http://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-221359.
Pełny tekst źródłaPetryshen, Tracey Lynn. "Localization of susceptibility genes involved in phonological coding dyslexia by family linkage and linkage disequilibrium studies". Thesis, National Library of Canada = Bibliothèque nationale du Canada, 2001. http://www.collectionscanada.ca/obj/s4/f2/dsk3/ftp04/NQ64882.pdf.
Pełny tekst źródłaZhao, Honghua. "Use of linkage disequilibrium for quantitative trait loci mapping in livestock". [Ames, Iowa : Iowa State University], 2006.
Znajdź pełny tekst źródłaLau, Winston Wai Shing. "Exploiting large scale computing for the analysis of genetic linkage disequilibrium". Thesis, University of Southampton, 2007. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.443042.
Pełny tekst źródłaYounkin, Samuel G. "The Linkage Disequilibrium LASSO for SNP Selection in Genetic Association Studies". Case Western Reserve University School of Graduate Studies / OhioLINK, 2011. http://rave.ohiolink.edu/etdc/view?acc_num=case1291219489.
Pełny tekst źródłaDehman, Alia. "Spatial clustering of linkage disequilibrium blocks for genome-wide association studies". Thesis, Université Paris-Saclay (ComUE), 2015. http://www.theses.fr/2015SACLE013/document.
Pełny tekst źródłaWith recent development of high-throughput genotyping technologies, the usage of Genome-Wide Association Studies (GWAS) has become widespread in genetic research. By screening large portions of the genome, these studies aim to characterize genetic factors involved in the development of complex genetic diseases. GWAS are also based on the existence of statistical dependencies, called Linkage Disequilibrium (LD) usually observed between nearby loci on DNA. LD is defined as the non-random association of alleles at different loci on the same chromosome or on different chromosomes in a population. This biological feature is of fundamental importance in association studies as it provides a fine location of unobserved causal mutations using adjacent genetic markers. Nevertheless, the complex block structure induced by LD as well as the large volume of genetic data arekey issues that have arisen with GWA studies. The contributions presented in this manuscript are in twofold, both methodological and algorithmic. On the methodological part, we propose a three-step approach that explicitly takes advantage of the grouping structure induced by LD in order to identify common variants which may have been missed by single marker analyses. In thefirst step, we perform a hierarchical clustering of SNPs with anadjacency constraint using LD as a similarity measure. In the second step, we apply a model selection approach to the obtained hierarchy in order to define LD blocks. Finally, we perform Group Lasso regression on the inferred LD blocks. The efficiency of the proposed approach is investigated compared to state-of-the art regression methods on simulated, semi-simulated and real GWAS data. On the algorithmic part, we focus on the spatially-constrained hierarchical clustering algorithm whose quadratic time complexity is not adapted to the high-dimensionality of GWAS data. We then present, in this manuscript, an efficient implementation of such an algorithm in the general context of anysimilarity measure. By introducing a user-parameter $h$ and using the min-heap structure, we obtain a sub-quadratic time complexity of the adjacency-constrained hierarchical clustering algorithm, as well as a linear space complexity in thenumber of items to be clustered. The interest of this novel algorithm is illustrated in GWAS applications
WANG, TAO. "MODELING AND INFERRING QUANTITATIVE TRAIT LOCI USING LINKAGE DISEQUILIBRIUM IN NATURAL POPULATIONS". NCSU, 2001. http://www.lib.ncsu.edu/theses/available/etd-20011012-133341.
Pełny tekst źródłaQuantitative trait loci (QTL) are those chromosome regions that contribute to variation of quantitative traits. Analysis of QTL is helpful for further study of molecular basis of the quantitative genetic variation. The discovery of highly abundant and dense polymorphic markers (e.g., single nucleotide polynorphisms, or SNPs) covering a whole genome provides an opportunity to localize QTL in a variety of populations. While classical linkage studies have a relatively limited resolution in QTL localization, the association mapping or linkage disequilibrium (LD) mapping approach can offer an alternative way for fine mapping of genes. Currently there are few LD methods available for QTL mapping in natural populations. Development of more efficient methods is still a challenging problem. In this thesis, we first review the LD approach for fine mapping of QTL in Chapter 1. Some basic issues in LD analysis and recent developments in LD methodology are discussed. Particular attention is paid to limitations and potential problems of these methods. This provides the motivation for the research in this thesis.Next, we explore Cockerham's genetic model (Cockerham, 1954) for quantitative traits in Chapter 2. A revised form of the Cockerham model is presented using some coding variables. The relationship between Cockerham model and some specific genetic models for designed experimental populations, such as backcross or F2, is then established. We study extensively the properties of QTL effects and partitions of various genetic variance components for these reduced models under both linkage equilibrium and linkage disequilibrium situations. A general multi-locus-two-allele model is also proposed that may serve as a basis for mapping QTL in natural populations. The main research of the thesis is on development of an exact multipoint likelihood approach to infer QTL in natural populations. In Chapter 3, we first generalize the formulation of the likelihood analysis for a polymorphic marker locus and a trait locus in a general natural population. From this generalization, we derive a closed form solutionof an efficient EM algorithm for the likelihood analysis. This is a major achievement of the research. The importance of this generalization is that it can be readily and systematically extended to multiple markers and multiple QTL.Based on this formulation, a multipoint likelihood analysis with the EM algorithm is developed that can take into account higher-order linkage disequilibria between QTL and markers without making approximation to the likelihood function. This analysis can offer a simultaneous estimation of the linkage disequilibrium structure between a QTL and multiple markers. From this estimation, we find that the linkage disequilibrium between one or a subset of markers and a QTL conditional on other markers can offer as a more accurate measure for fine mapping of QTL. In Chapter 4, we further extend the analysis to multiple QTL and propose a general framework for likelihood analysis of multiple QTL and markers. With this approach, the joint gametic frequencies of QTL and markers (thus various measures of linkage disequilibria between QTL and markers) as well as various genetic effects of QTL (including epistasis) can be estimated simultaneously. This general approach has a lot of potential for a complete analysis of genetic architecture of quantitative traits in natural populations. Although the foundation of this general framework has been laid down, more studies are still needed on a number of issues, such as efficiency and reliability of the optimization algorithm, statistical tests for QTL identification, model selection of complex QTL, and more efficient approaches to analyze large data sets. In the last chapter (Chapter 5), we draw some general conclusions from the research. We discuss the advantages as well as limitations of the approach developed in this thesis and problems for further research.
Li, Tao. "Linkage disequilibrium mapping of schizophrenia and related traits in a Chinese population". Thesis, King's College London (University of London), 2005. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.416371.
Pełny tekst źródłaJia, Tianye. "Strategies and statistical methods for linkage disequilibrium-based mapping of complex traits". Thesis, University of Birmingham, 2012. http://etheses.bham.ac.uk//id/eprint/3292/.
Pełny tekst źródłaOudot, Tiphaine. "Recherche de gènes de prédisposition à une maladie à hérédité complexe : le psoriasis". Thesis, Evry-Val d'Essonne, 2009. http://www.theses.fr/2008EVRY0034/document.
Pełny tekst źródłaThe psoriasis is a complex chronic inflammatory skin disease due to a strong genetic component as well as environmental factors. The only major locus for psoriasis susceptibility implicated to date, named PSORS1 on chromosome 6p21, has been demonstrated in various populations in linkage and association studies. It could nevertheless be responsible for up to 50% of the genetic contribution to the disease. The aim of my thesis was thus to identify the other genetic factors, in particular in the French population. To identify the loci, a linkage study was carried out, showing possible regions on 12q, 14q, 16p, 20p, in addition to that on 6p. Two loci on 6p and 20p were studied in more detail, revealing the contribution of the two genes, HLA-C and ADAM33. In parallel, a "candidate gene" strategy was undertaken, exposing a probable role of FLG, TGM5, CARD15 and CYLD genes and a confirmed role of SLC12A8 gene in the etiology of psoriasis
Lee, Yiu-fai. "Analysis for segmental sharing and linkage disequilibrium a genomewide association study on myopia /". Click to view the E-thesis via HKUTO, 2009. http://sunzi.lib.hku.hk/hkuto/record/B43912217.
Pełny tekst źródłaAdams, David R. "The low-density lipoprotein receptor as a model for studying candidate-locus linkage disequilibrium and allelic association /". Thesis, Connect to this title online; UW restricted, 1998. http://hdl.handle.net/1773/10852.
Pełny tekst źródłaChapman, J. M. "Statistical methods for linkage disequilibrium mapping of disease susceptibility genes in candidate regions". Thesis, University of Cambridge, 2005. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.597484.
Pełny tekst źródłaLee, Yiu-fai, i 李耀暉. "Analysis for segmental sharing and linkage disequilibrium: a genomewide association study on myopia". Thesis, The University of Hong Kong (Pokfulam, Hong Kong), 2009. http://hub.hku.hk/bib/B43912217.
Pełny tekst źródłaJiang, Ning. "Linkage disequilibrium based eQTL analysis and comparative evolutionary epigenetic regulation of gene transcription". Thesis, University of Birmingham, 2013. http://etheses.bham.ac.uk//id/eprint/4031/.
Pełny tekst źródłaMacpherson, James Neil. "Linkage disequilibrium between DNA polymorphisms in a natural population of Drosophila melanogaster Meigen". Thesis, University of Edinburgh, 1989. http://hdl.handle.net/1842/12530.
Pełny tekst źródłaSchramm, Heather Elizabeth. "Development of mapping by admixture linkage disequilibrium for understanding human complex genetic diseases /". For electronic version search Digital dissertations database. Restricted to UC campuses. Access is free to UC campus dissertations, 2003. http://uclibs.org/PID/11984.
Pełny tekst źródłaCarvalho, Santos Pablo Sandro [Verfasser]. "Linkage disequilibrium and transmission distortion affecting human chromosome 6p / Pablo Sandro Carvalho Santos". Berlin : Freie Universität Berlin, 2010. http://d-nb.info/1025127048/34.
Pełny tekst źródłaJung, Jeesun. "High resolution linkage and association study of quantitative trait loci". Texas A&M University, 2004. http://hdl.handle.net/1969.1/2681.
Pełny tekst źródłaHyten, David Lee. "Genetic diversity and linkage disequilibrium in wild soybean, landraces, ancestral, and elite soybean populations". College Park, Md. : University of Maryland, 2005. http://hdl.handle.net/1903/2441.
Pełny tekst źródłaThesis research directed by: Natural Resource Sciences. Title from t.p. of PDF. Includes bibliographical references. Published by UMI Dissertation Services, Ann Arbor, Mich. Also available in paper.
Zhu, Guohua. "Ascertainment in two-phase sampling designs for segregation and linkage analysis /". Connect to text online, 2005. http://rave.ohiolink.edu/etdc/view?acc%5Fnum=case1112844349.
Pełny tekst źródła[School of Medicine] Department of Epidemiology and Biostatistics. Includes bibliographical references. Available online via OhioLINK's ETD Center.
Larsson, Hanna. "Population Genetics and Genome Organization of Norway Spruce". Doctoral thesis, Uppsala universitet, Växtekologi och evolution, 2012. http://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-180370.
Pełny tekst źródłaLarsson, Hanna, Thomas Kallman, Niclas Gyllenstrand i Martin Lascoux. "Distribution of Long-Range Linkage Disequilibrium and Tajima's D Values in Scandinavian Populations of Norway Spruce (Picea abies)". Uppsala universitet, Växtekologi och evolution, 2013. http://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-202930.
Pełny tekst źródłaKuo, Tai-Yue. "The construction of linkage disequilibrium maps and their application to association mapping of disease genes". Thesis, University of Southampton, 2008. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.485527.
Pełny tekst źródłaBackström, Niclas. "Gene Mapping in Ficedula Flycatchers". Doctoral thesis, Uppsala universitet, Institutionen för evolution, genomik och systematik, 2009. http://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-9513.
Pełny tekst źródłaPungliya, Manish S. "Single nucleotide polymorphism analysis in application to fine gene mapping". Digital WPI, 2001. https://digitalcommons.wpi.edu/etd-theses/642.
Pełny tekst źródłaLiu, Jin. "Penalized methods in genome-wide association studies". Diss., University of Iowa, 2011. https://ir.uiowa.edu/etd/1242.
Pełny tekst źródłaGraham, Jinko. "Disequilibrium fine-mapping of a rare allele via coalescent models of gene ancestry /". Thesis, Connect to this title online; UW restricted, 1998. http://hdl.handle.net/1773/9568.
Pełny tekst źródłaLõhmussaar, Elin. "The comparative patterns of linkage disequilibrium in European populations and its implication for genetic association studies /". Tartu, Estonia, 2006. http://dspace.utlib.ee/dspace/bitstream/10062/978/5/lohmussaar.pdf.
Pełny tekst źródłaTenesa-Prunyonosa, Albert. "Population-wide linkage disequilibrium and its uses in QTL mapping and estimation of ancestral population size". Thesis, University of Edinburgh, 2003. http://hdl.handle.net/1842/11451.
Pełny tekst źródłaVarilo, Teppo. "[The]age of the mutations in the Finnish disease heritage : a genealogical and linkage disequilibrium study". Helsinki : University of Helsinki, 1999. http://ethesis.helsinki.fi/julkaisut/laa/haart/vk/varilo/.
Pełny tekst źródłaLiu, Lian. "Topics in measurement error and missing data problems". Thesis, [College Station, Tex. : Texas A&M University, 2007. http://hdl.handle.net/1969.1/ETD-TAMU-1627.
Pełny tekst źródłaSöderholm, Simon. "The Complex Genetics of Multiple Sclerosis : A preliminary study of MS-associated SNPs prior to a larger genotyping project". Thesis, Linköpings universitet, Institutionen för fysik, kemi och biologi, 2016. http://urn.kb.se/resolve?urn=urn:nbn:se:liu:diva-129423.
Pełny tekst źródłaDoecke, James. "Genetic variation in Runx2 related to bone mineral density". Thesis, Griffith University, 2006. http://hdl.handle.net/10072/367841.
Pełny tekst źródłaThesis (PhD Doctorate)
Doctor of Philosophy (PhD)
School of Medical Science
Griffith Health
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Soliai, Marcus Makina. "De novo Genome Assembly and SNP Marker Development of Pyrenophora semeniperda". BYU ScholarsArchive, 2011. https://scholarsarchive.byu.edu/etd/2960.
Pełny tekst źródłaGibson, Jane. "Defining linkage disequilibrium patterns and tracts of extended homozygosity to compare populations and search for disease genes". Thesis, University of Southampton, 2008. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.509463.
Pełny tekst źródłaChretien, Jean-Paul. "Genetic mapping of between-population variation using mapping by admixture linkage disequilibrium methodology and application to lipoprotein(A) /". Available to US Hopkins community, 2003. http://wwwlib.umi.com/dissertations/dlnow/3080642.
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