Systematic interpretation of large-scale GWAS analyses of 5,035 phenotypes
Kuupäev
2024
Autorid
Ajakirja pealkiri
Ajakirja ISSN
Köite pealkiri
Kirjastaja
Tartu Ülikool
Abstrakt
This thesis presents the systematic interpretation of 5,035 genome-wide association studies
(GWAS) conducted within the Estonian Biobank, aiming to elucidate the genetic determinants
influencing a diverse array of phenotypic traits. Through a review of existing literature and
the application of advanced bioinformatic tools, the work done in this thesis outlined the
results of main post-GWAS methods, such as the identification of novel variants, SNP
heritability estimation, fine-mapping of causal variants, and prioritization of genes associated
with complex traits. Around 26% of the variants identified as lead ones in this work are novel
and had not been implicated by GWASs before. Fine mapping prioritized single genetic
variants for 10.3% of investigated loci, providing hypotheses for further functional studies,
and the gene prioritization approach identified the 2,402 lead variants to be related to 804
genes, several of those biologically interpretable. Heritability was reliably inferred for 25% of
studied phenotypes, the most heritable traits being “Other specified hypothyroidism” (ICD-10
code E03.8), “Obesity due to excess calories” (E66.0), “Obesity” (E66), “Myopia” (H52.1),
and “Hypertension” (I10). These findings are a good starting point for a more in-depth
interpretation of loci associated with complex diseases in the Estonian Biobank.
Kirjeldus
Märksõnad
Genome-wide association studies, Post-GWAS analysis, Large-scale analysis