Analysis of DNA diversity and meiotic recombination in the human MHC class II region

There is mounting evidence that recombination events are not randomly distributed in the human genome, but tend cluster into distinct regions, so-called recombination hotspots. My PhD work was focussed on developing an understanding of how meiotic recombination events are distributed in the human Ma...

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Main Author: Liisa Kauppi
Format: Thesis
Language:unknown
Published: 2003
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saami
Online Access:https://figshare.com/articles/thesis/Analysis_of_DNA_diversity_and_meiotic_recombination_in_the_human_MHC_class_II_region/10140110
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spelling ftleicesterunfig:oai:figshare.com:article/10140110 2023-05-15T18:08:17+02:00 Analysis of DNA diversity and meiotic recombination in the human MHC class II region Liisa Kauppi 2003-01-01T00:00:00Z https://figshare.com/articles/thesis/Analysis_of_DNA_diversity_and_meiotic_recombination_in_the_human_MHC_class_II_region/10140110 unknown 2381/30346 https://figshare.com/articles/thesis/Analysis_of_DNA_diversity_and_meiotic_recombination_in_the_human_MHC_class_II_region/10140110 All Rights Reserved Uncategorized IR content Text Thesis 2003 ftleicesterunfig 2021-11-11T19:57:33Z There is mounting evidence that recombination events are not randomly distributed in the human genome, but tend cluster into distinct regions, so-called recombination hotspots. My PhD work was focussed on developing an understanding of how meiotic recombination events are distributed in the human Major Histocompatibility (MHC) Class II region. To this end, a large number of SNPs in this region was identified and genotyped, and high-resolution linkage disequilibrium (LD) patterns were examined for evidence of historical recombination. Three regions of LD breakdown, i.e. putative recombination hotspots were localised. For these regions, allele-specific PCR methods were used to selectively amplify recombinant molecules directly from sperm DNA.;This lead to the identification of three novel crossover hotspots, within which I was able to demonstrate an extremely localised nature of crossover breakpoints. Furthermore, molecular characterisation of the three hotspots showed that crossover rates can vary dramatically from one hotspot to the next and that LD patterns cannot be used to readily predict these rates.;I also investigated the relative importance of known recombination hotspots vs. population history in shaping LD in three human populations (UK North Europeans, Saami and Zimbabweans). At least in this segment of the MHC, haplotype structures directly relate to fine-scale patterns of meiotic recombination, even though a distinct paucity of "universal" haplotypes (haplotypes shared by all three populations) was observed. Thesis saami University of Leicester: Figshare
institution Open Polar
collection University of Leicester: Figshare
op_collection_id ftleicesterunfig
language unknown
topic Uncategorized
IR content
spellingShingle Uncategorized
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Liisa Kauppi
Analysis of DNA diversity and meiotic recombination in the human MHC class II region
topic_facet Uncategorized
IR content
description There is mounting evidence that recombination events are not randomly distributed in the human genome, but tend cluster into distinct regions, so-called recombination hotspots. My PhD work was focussed on developing an understanding of how meiotic recombination events are distributed in the human Major Histocompatibility (MHC) Class II region. To this end, a large number of SNPs in this region was identified and genotyped, and high-resolution linkage disequilibrium (LD) patterns were examined for evidence of historical recombination. Three regions of LD breakdown, i.e. putative recombination hotspots were localised. For these regions, allele-specific PCR methods were used to selectively amplify recombinant molecules directly from sperm DNA.;This lead to the identification of three novel crossover hotspots, within which I was able to demonstrate an extremely localised nature of crossover breakpoints. Furthermore, molecular characterisation of the three hotspots showed that crossover rates can vary dramatically from one hotspot to the next and that LD patterns cannot be used to readily predict these rates.;I also investigated the relative importance of known recombination hotspots vs. population history in shaping LD in three human populations (UK North Europeans, Saami and Zimbabweans). At least in this segment of the MHC, haplotype structures directly relate to fine-scale patterns of meiotic recombination, even though a distinct paucity of "universal" haplotypes (haplotypes shared by all three populations) was observed.
format Thesis
author Liisa Kauppi
author_facet Liisa Kauppi
author_sort Liisa Kauppi
title Analysis of DNA diversity and meiotic recombination in the human MHC class II region
title_short Analysis of DNA diversity and meiotic recombination in the human MHC class II region
title_full Analysis of DNA diversity and meiotic recombination in the human MHC class II region
title_fullStr Analysis of DNA diversity and meiotic recombination in the human MHC class II region
title_full_unstemmed Analysis of DNA diversity and meiotic recombination in the human MHC class II region
title_sort analysis of dna diversity and meiotic recombination in the human mhc class ii region
publishDate 2003
url https://figshare.com/articles/thesis/Analysis_of_DNA_diversity_and_meiotic_recombination_in_the_human_MHC_class_II_region/10140110
genre saami
genre_facet saami
op_relation 2381/30346
https://figshare.com/articles/thesis/Analysis_of_DNA_diversity_and_meiotic_recombination_in_the_human_MHC_class_II_region/10140110
op_rights All Rights Reserved
_version_ 1766180551783350272

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