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Refinement of schizophrenia GWAS loci using methylome-wide association data
Refinement of schizophrenia GWAS loci using methylome-wide association data
by Chan, Robin , Kumar, Gaurav , Nerella, Srilaxmi , McClay, Joseph L. , Adkins, Daniel E. , Kim, Yunjung , Sullivan, Patrick F. , Clark, Shaunna L. , van den Oord, Edwin J. C. G. , Aberg, Karolina A. , Shabalin, Andrey A. , Hultman, Christina M. , Xie, Linying , Magnusson, Patrik K. E.
in Analysis / Biomarkers - analysis / Biomedical and Life Sciences / Biomedicine / Case-Control Studies / Computational Biology / Data analysis / Databases, Genetic / Development and progression / DNA Methylation / Epigenomics / Follow-Up Studies / Gene Function / Genome-Wide Association Study / Genomes / Genomics / Human Genetics / Humans / Hypotheses / Linkage Disequilibrium / Meta-Analysis as Topic / Metabolic Diseases / Methylation / Molecular Medicine / Original Investigation / Polymorphism, Single Nucleotide - genetics / Schizophrenia / Schizophrenia - genetics / Single nucleotide polymorphisms / Transcription factors
2015
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Refinement of schizophrenia GWAS loci using methylome-wide association data
by Chan, Robin , Kumar, Gaurav , Nerella, Srilaxmi , McClay, Joseph L. , Adkins, Daniel E. , Kim, Yunjung , Sullivan, Patrick F. , Clark, Shaunna L. , van den Oord, Edwin J. C. G. , Aberg, Karolina A. , Shabalin, Andrey A. , Hultman, Christina M. , Xie, Linying , Magnusson, Patrik K. E.
in Analysis / Biomarkers - analysis / Biomedical and Life Sciences / Biomedicine / Case-Control Studies / Computational Biology / Data analysis / Databases, Genetic / Development and progression / DNA Methylation / Epigenomics / Follow-Up Studies / Gene Function / Genome-Wide Association Study / Genomes / Genomics / Human Genetics / Humans / Hypotheses / Linkage Disequilibrium / Meta-Analysis as Topic / Metabolic Diseases / Methylation / Molecular Medicine / Original Investigation / Polymorphism, Single Nucleotide - genetics / Schizophrenia / Schizophrenia - genetics / Single nucleotide polymorphisms / Transcription factors
2015
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Refinement of schizophrenia GWAS loci using methylome-wide association data
Refinement of schizophrenia GWAS loci using methylome-wide association data
by Chan, Robin , Kumar, Gaurav , Nerella, Srilaxmi , McClay, Joseph L. , Adkins, Daniel E. , Kim, Yunjung , Sullivan, Patrick F. , Clark, Shaunna L. , van den Oord, Edwin J. C. G. , Aberg, Karolina A. , Shabalin, Andrey A. , Hultman, Christina M. , Xie, Linying , Magnusson, Patrik K. E.
in Analysis / Biomarkers - analysis / Biomedical and Life Sciences / Biomedicine / Case-Control Studies / Computational Biology / Data analysis / Databases, Genetic / Development and progression / DNA Methylation / Epigenomics / Follow-Up Studies / Gene Function / Genome-Wide Association Study / Genomes / Genomics / Human Genetics / Humans / Hypotheses / Linkage Disequilibrium / Meta-Analysis as Topic / Metabolic Diseases / Methylation / Molecular Medicine / Original Investigation / Polymorphism, Single Nucleotide - genetics / Schizophrenia / Schizophrenia - genetics / Single nucleotide polymorphisms / Transcription factors
2015

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Refinement of schizophrenia GWAS loci using methylome-wide association data
Refinement of schizophrenia GWAS loci using methylome-wide association data
Journal Article

Refinement of schizophrenia GWAS loci using methylome-wide association data

Chan, Robin,
Kumar, Gaurav,
Nerella, Srilaxmi,
McClay, Joseph L.,
Adkins, Daniel E.,
Kim, Yunjung,
Sullivan, Patrick F.,
Clark, Shaunna L.,
van den Oord, Edwin J. C. G.,
Aberg, Karolina A.,
Shabalin, Andrey A.,
Hultman, Christina M.,
Xie, Linying,
Magnusson, Patrik K. E.
2015
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Overview
Recent genome-wide association studies (GWAS) have made substantial progress in identifying disease loci. The next logical step is to design functional experiments to identify disease mechanisms. This step, however, is often hampered by the large size of loci identified in GWAS that is caused by linkage disequilibrium between SNPs. In this study, we demonstrate how integrating methylome-wide association study (MWAS) results with GWAS findings can narrow down the location for a subset of the putative casual sites. We use the disease schizophrenia as an example. To handle “data analytic” variation, we first combined our MWAS results with two GWAS meta-analyses ( N  = 32,143 and 21,953), that had largely overlapping samples but different data analysis pipelines, separately. Permutation tests showed significant overlapping association signals between GWAS and MWAS findings. This significant overlap justified prioritizing loci based on the concordance principle. To further ensure that the methylation signal was not driven by chance, we successfully replicated the top three methylation findings near genes SDCCAG8 , CREB1 and ATXN7 in an independent sample using targeted pyrosequencing. In contrast to the SNPs in the selected region, the methylation sites were largely uncorrelated explaining why the methylation signals implicated much smaller regions (median size 78 bp). The refined loci showed considerable enrichment of genomic elements of possible functional importance and suggested specific hypotheses about schizophrenia etiology. Several hypotheses involved possible variation in transcription factor-binding efficiencies.
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Publisher
Springer Berlin Heidelberg,Springer,Springer Nature B.V
Subject

Analysis

/ Biomarkers - analysis

/ Biomedical and Life Sciences

/ Biomedicine

/ Case-Control Studies

/ Computational Biology

/ Data analysis

/ Databases, Genetic

/ Development and progression

/ DNA Methylation

/ Epigenomics

/ Follow-Up Studies

/ Gene Function

/ Genome-Wide Association Study

/ Genomes

/ Genomics

/ Human Genetics

/ Humans

/ Hypotheses

/ Linkage Disequilibrium

/ Meta-Analysis as Topic

/ Metabolic Diseases

/ Methylation

/ Molecular Medicine

/ Original Investigation

/ Polymorphism, Single Nucleotide - genetics

/ Schizophrenia

/ Schizophrenia - genetics

/ Single nucleotide polymorphisms

/ Transcription factors

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