Genome-Wide Associations between Genetic and Epigenetic Variation Influence mRNA Expression and Insulin Secretion in Human Pancreatic Islets

Genetic and epigenetic mechanisms may interact and together affect biological processes and disease development. However, most previous studies have investigated genetic and epigenetic mechanisms independently, and studies examining their interactions throughout the human genome are lacking. To iden...

Descripción completa

Detalles Bibliográficos
Autores principales: Olsson, Anders H., Volkov, Petr, Bacos, Karl, Dayeh, Tasnim, Hall, Elin, Nilsson, Emma A., Ladenvall, Claes, Rönn, Tina, Ling, Charlotte
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4222689/
https://www.ncbi.nlm.nih.gov/pubmed/25375650
http://dx.doi.org/10.1371/journal.pgen.1004735
_version_ 1782343081685680128
author Olsson, Anders H.
Volkov, Petr
Bacos, Karl
Dayeh, Tasnim
Hall, Elin
Nilsson, Emma A.
Ladenvall, Claes
Rönn, Tina
Ling, Charlotte
author_facet Olsson, Anders H.
Volkov, Petr
Bacos, Karl
Dayeh, Tasnim
Hall, Elin
Nilsson, Emma A.
Ladenvall, Claes
Rönn, Tina
Ling, Charlotte
author_sort Olsson, Anders H.
collection PubMed
description Genetic and epigenetic mechanisms may interact and together affect biological processes and disease development. However, most previous studies have investigated genetic and epigenetic mechanisms independently, and studies examining their interactions throughout the human genome are lacking. To identify genetic loci that interact with the epigenome, we performed the first genome-wide DNA methylation quantitative trait locus (mQTL) analysis in human pancreatic islets. We related 574,553 single nucleotide polymorphisms (SNPs) with genome-wide DNA methylation data of 468,787 CpG sites targeting 99% of RefSeq genes in islets from 89 donors. We identified 67,438 SNP-CpG pairs in cis, corresponding to 36,783 SNPs (6.4% of tested SNPs) and 11,735 CpG sites (2.5% of tested CpGs), and 2,562 significant SNP-CpG pairs in trans, corresponding to 1,465 SNPs (0.3% of tested SNPs) and 383 CpG sites (0.08% of tested CpGs), showing significant associations after correction for multiple testing. These include reported diabetes loci, e.g. ADCY5, KCNJ11, HLA-DQA1, INS, PDX1 and GRB10. CpGs of significant cis-mQTLs were overrepresented in the gene body and outside of CpG islands. Follow-up analyses further identified mQTLs associated with gene expression and insulin secretion in human islets. Causal inference test (CIT) identified SNP-CpG pairs where DNA methylation in human islets is the potential mediator of the genetic association with gene expression or insulin secretion. Functional analyses further demonstrated that identified candidate genes (GPX7, GSTT1 and SNX19) directly affect key biological processes such as proliferation and apoptosis in pancreatic β-cells. Finally, we found direct correlations between DNA methylation of 22,773 (4.9%) CpGs with mRNA expression of 4,876 genes, where 90% of the correlations were negative when CpGs were located in the region surrounding transcription start site. Our study demonstrates for the first time how genome-wide genetic and epigenetic variation interacts to influence gene expression, islet function and potential diabetes risk in humans.
format Online
Article
Text
id pubmed-4222689
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-42226892014-11-13 Genome-Wide Associations between Genetic and Epigenetic Variation Influence mRNA Expression and Insulin Secretion in Human Pancreatic Islets Olsson, Anders H. Volkov, Petr Bacos, Karl Dayeh, Tasnim Hall, Elin Nilsson, Emma A. Ladenvall, Claes Rönn, Tina Ling, Charlotte PLoS Genet Research Article Genetic and epigenetic mechanisms may interact and together affect biological processes and disease development. However, most previous studies have investigated genetic and epigenetic mechanisms independently, and studies examining their interactions throughout the human genome are lacking. To identify genetic loci that interact with the epigenome, we performed the first genome-wide DNA methylation quantitative trait locus (mQTL) analysis in human pancreatic islets. We related 574,553 single nucleotide polymorphisms (SNPs) with genome-wide DNA methylation data of 468,787 CpG sites targeting 99% of RefSeq genes in islets from 89 donors. We identified 67,438 SNP-CpG pairs in cis, corresponding to 36,783 SNPs (6.4% of tested SNPs) and 11,735 CpG sites (2.5% of tested CpGs), and 2,562 significant SNP-CpG pairs in trans, corresponding to 1,465 SNPs (0.3% of tested SNPs) and 383 CpG sites (0.08% of tested CpGs), showing significant associations after correction for multiple testing. These include reported diabetes loci, e.g. ADCY5, KCNJ11, HLA-DQA1, INS, PDX1 and GRB10. CpGs of significant cis-mQTLs were overrepresented in the gene body and outside of CpG islands. Follow-up analyses further identified mQTLs associated with gene expression and insulin secretion in human islets. Causal inference test (CIT) identified SNP-CpG pairs where DNA methylation in human islets is the potential mediator of the genetic association with gene expression or insulin secretion. Functional analyses further demonstrated that identified candidate genes (GPX7, GSTT1 and SNX19) directly affect key biological processes such as proliferation and apoptosis in pancreatic β-cells. Finally, we found direct correlations between DNA methylation of 22,773 (4.9%) CpGs with mRNA expression of 4,876 genes, where 90% of the correlations were negative when CpGs were located in the region surrounding transcription start site. Our study demonstrates for the first time how genome-wide genetic and epigenetic variation interacts to influence gene expression, islet function and potential diabetes risk in humans. Public Library of Science 2014-11-06 /pmc/articles/PMC4222689/ /pubmed/25375650 http://dx.doi.org/10.1371/journal.pgen.1004735 Text en © 2014 Olsson et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Olsson, Anders H.
Volkov, Petr
Bacos, Karl
Dayeh, Tasnim
Hall, Elin
Nilsson, Emma A.
Ladenvall, Claes
Rönn, Tina
Ling, Charlotte
Genome-Wide Associations between Genetic and Epigenetic Variation Influence mRNA Expression and Insulin Secretion in Human Pancreatic Islets
title Genome-Wide Associations between Genetic and Epigenetic Variation Influence mRNA Expression and Insulin Secretion in Human Pancreatic Islets
title_full Genome-Wide Associations between Genetic and Epigenetic Variation Influence mRNA Expression and Insulin Secretion in Human Pancreatic Islets
title_fullStr Genome-Wide Associations between Genetic and Epigenetic Variation Influence mRNA Expression and Insulin Secretion in Human Pancreatic Islets
title_full_unstemmed Genome-Wide Associations between Genetic and Epigenetic Variation Influence mRNA Expression and Insulin Secretion in Human Pancreatic Islets
title_short Genome-Wide Associations between Genetic and Epigenetic Variation Influence mRNA Expression and Insulin Secretion in Human Pancreatic Islets
title_sort genome-wide associations between genetic and epigenetic variation influence mrna expression and insulin secretion in human pancreatic islets
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4222689/
https://www.ncbi.nlm.nih.gov/pubmed/25375650
http://dx.doi.org/10.1371/journal.pgen.1004735
work_keys_str_mv AT olssonandersh genomewideassociationsbetweengeneticandepigeneticvariationinfluencemrnaexpressionandinsulinsecretioninhumanpancreaticislets
AT volkovpetr genomewideassociationsbetweengeneticandepigeneticvariationinfluencemrnaexpressionandinsulinsecretioninhumanpancreaticislets
AT bacoskarl genomewideassociationsbetweengeneticandepigeneticvariationinfluencemrnaexpressionandinsulinsecretioninhumanpancreaticislets
AT dayehtasnim genomewideassociationsbetweengeneticandepigeneticvariationinfluencemrnaexpressionandinsulinsecretioninhumanpancreaticislets
AT hallelin genomewideassociationsbetweengeneticandepigeneticvariationinfluencemrnaexpressionandinsulinsecretioninhumanpancreaticislets
AT nilssonemmaa genomewideassociationsbetweengeneticandepigeneticvariationinfluencemrnaexpressionandinsulinsecretioninhumanpancreaticislets
AT ladenvallclaes genomewideassociationsbetweengeneticandepigeneticvariationinfluencemrnaexpressionandinsulinsecretioninhumanpancreaticislets
AT ronntina genomewideassociationsbetweengeneticandepigeneticvariationinfluencemrnaexpressionandinsulinsecretioninhumanpancreaticislets
AT lingcharlotte genomewideassociationsbetweengeneticandepigeneticvariationinfluencemrnaexpressionandinsulinsecretioninhumanpancreaticislets

Ejemplares similares