Genomics and bioinformatics strategies in the study of aging and Alzheimer disease
To understand complex phenotypes, medical research has evolved from the study of single genes and proteins to approaches that encompass more comprehensive catalogues of molecules. Among the more widely used are genome-wide expression and high-throughput genotyping, the latter primarily making use of single nucleotide polymorphisms (SNPs) in what has been termed genome-wide association studies (GWAS). Because of the scale of the data sets that are being produced, unique problems have emerged that necessitate the extensive use of bioinformatics tools. This thesis has entailed the analysis of several such large data sets in the context of biological pathways and introduces several bioinformatics solutions. Paper III, IV, and V deal with this topic. This thesis is primarily oriented around the study of Alzheimer disease (AD) and aging. The questions about the etiology of AD are often concurrent with questions about the biology of aging. This thesis pursues insight on genomic factors pertaining to both inquiries, acknowledging that both the AD state and aging itself are complex and multi-factorial. Two constituent papers (I and III) address aging and two papers (II and V) deal with genetic models in the study of AD.
In paper I, we examined the association of age with several genetic markers in the insulin degrading enzyme (IDE) and explored possible molecular mechanisms. In contrast to women, both age-at-sampling and age-at-death of the males were significantly lower in individuals that were heterozygous at genetic loci spanning the IDE locus. Plasma insulin levels and the expression levels of the gene were found to be higher in those same heterozygous males.
In paper II, SNPs in 25 genes involved in cholesterol metabolism were tested for association with AD and dementia. Genetic markers in a large linkage disequilibrium block spanning SREBF1, TOM1L2, and ATPAF2 were significantly associated with disease. Gene expression and gene network analyses supported the findings.
In paper III, we investigated the biological pathway basis of age in human brain and lymphocytes. Mitochondrial genes were negatively regulated in both tissue samples, while the protein translation genes appeared to decrease in lymphocytes but increase in brain. Those observations indicated that there are common themes across tissues, but also tissue specific changes in gene regulation. We also examined the genomic architecture of the age-regulated genes, and found that the expression of non-compact genes tend to decrease with advancing age.
A large number of genome-wide association studies (GWAS) have now been performed over the past few years. In paper IV, we developed a program that automates the conversion of SNPs to representative gene lists in order to facilitate the exploration of biological pathway in the context of GWAS.
In paper V, we employed the software developed in study IV to identify biological pathways enriched among the genes that were significantly associated from a GWAS of AD. Genes involved in intracellular protein transmembrane transport were found to be significantly overrepresented. These results highlighted the possibility that TOMM40 contributes to AD pathology together with other translocases.
Through this thesis, several biological relationships have been identified linking AD and aging. Genetic markers in IDE, a gene previously claimed to be associated with AD, also associate with age. With advancing age, mitochondrial gene expression deteriorates significantly. TOMM40 may contribute the AD pathology, together with other genes that encode proteins of the intracellular transmembrane protein transport pathway. Methodologically, pathway analyses were conducted successfully with the program, ProxyGeneLD. This enabled discoveries and discussion of the challenges that face the exploration of GWAS data sets in a pathway context. In the future, more sophisticated bioinformatics tools and enhanced gene annotation may lead to the discovery of the molecular mechanisms that dominate complex diseases and traits.
List of scientific papers
I. Mun-Gwan Hong, Chandra Reynolds, Margaret Gatz, Boo Johansson, Jennifer C. Palmer, Harvest F. Gu, Kaj Blennow, Patrick G. Kehoe, Ulf de Faire, Nancy L. Pedersen and Jonathan A. Prince. Evidence that the gene encoding insulin degrading enzyme influences human lifespan. Human Molecular Genetics. (2008) 17:2370-2378.
https://doi.org/10.1093/hmg/ddn137
II. Chandra A. Reynolds, Mun-Gwan Hong, Ulrika K. Eriksson, Kaj Blennow, Fredrik Wiklund, Boo Johansson, Bo Malmberg, Stig Berg, Andrey Alexeyenko, Henrik Grönberg, Margaret Gatz, Nancy L. Pedersen and Jonathan A. Prince. Analysis of lipid pathway genes indicates association of sequence variation near SREBF1/TOM1L2/ATPAF2 with dementia risk. Human Molecular Genetics. (2010) 19:2068-2078.
https://doi.org/10.1093/hmg/ddq079
III. Mun-Gwan Hong, Amanda J. Myers, Patrik K. E. Magnusson and Jonathan A. Prince. Transcriptome-wide assessment of human brain and lymphocyte senescence. PLoS ONE. (2008) 3:e3024.
https://doi.org/10.1371/journal.pone.0003024
IV. Mun-Gwan Hong, Yudi Pawitan, Patrik K. E. Magnusson and Jonathan A. Prince. Strategies and issues in the detection of pathway enrichment in genome-wide association studies. Human Genetics. (2009) 126:289-301.
https://doi.org/10.1007/s00439-009-0676-z
V. Mun-Gwan Hong, Andrey Alexeyenko, Jean-Charles Lambert, Philippe Amouyel and Jonathan A Prince. Genome-wide pathway analysis implicates intracellular transmembrane protein transport in Alzheimer disease. Journal of Human Genetics. (2010) 55:707–709.
https://doi.org/10.1038/jhg.2010.92
History
Defence date
2011-03-11Department
- Department of Medical Epidemiology and Biostatistics
Publisher/Institution
Karolinska InstitutetPublication year
2011Thesis type
- Doctoral thesis
ISBN
978-91-7457-251-3Number of supporting papers
5Language
- eng