A promoter interaction map for cardiovascular disease genetics

Over 500 genetic loci have been associated with risk of cardiovascular diseases (CVDs); however, most loci are located in gene-distal non-coding regions and their target genes are not known. Here, we generated high-resolution promoter capture Hi-C (PCHi-C) maps in human induced pluripotent stem cell...

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Vydáno v:eLife Ročník 7
Hlavní autoři: Montefiori, Lindsey E, Sobreira, Debora R, Sakabe, Noboru J, Aneas, Ivy, Joslin, Amelia C, Hansen, Grace T, Bozek, Grazyna, Moskowitz, Ivan P, McNally, Elizabeth M, Nóbrega, Marcelo A
Médium: Journal Article
Jazyk:angličtina
Vydáno: England eLife Sciences Publications Ltd 10.07.2018
eLife Sciences Publications, Ltd
Témata:
capture Hi-C
Cardiomyocytes
Cardiovascular disease
Cardiovascular diseases
Cardiovascular Diseases - genetics
Chromatin
Chromosomes and Gene Expression
Epigenetics
Gene expression
Gene Expression Regulation
Gene mapping
gene regulation
Gene Regulatory Networks
Genetic Loci
Genetics
Genome, Human
Genome-Wide Association Study
Genomes
Genomics
GWAS
Human Biology and Medicine
Humans
Induced Pluripotent Stem Cells - cytology
Induced Pluripotent Stem Cells - metabolism
Myocytes, Cardiac - cytology
Myocytes, Cardiac - metabolism
Pluripotency
Polymorphism, Single Nucleotide
Promoter Regions, Genetic
Regulatory Elements, Transcriptional
Single-nucleotide polymorphism
Stem cells
Tools and Resources
United States > US
Chicago Illinois
cardiomyocytes
human biology
cardiovascular disease
GWAS
gene regulation
chromosomes
medicine
capture Hi-C
human
gene expression
ISSN:2050-084X, 2050-084X
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Popis
Shrnutí:Over 500 genetic loci have been associated with risk of cardiovascular diseases (CVDs); however, most loci are located in gene-distal non-coding regions and their target genes are not known. Here, we generated high-resolution promoter capture Hi-C (PCHi-C) maps in human induced pluripotent stem cells (iPSCs) and iPSC-derived cardiomyocytes (CMs) to provide a resource for identifying and prioritizing the functional targets of CVD associations. We validate these maps by demonstrating that promoters preferentially contact distal sequences enriched for tissue-specific transcription factor motifs and are enriched for chromatin marks that correlate with dynamic changes in gene expression. Using the CM PCHi-C map, we linked 1999 CVD-associated SNPs to 347 target genes. Remarkably, more than 90% of SNP-target gene interactions did not involve the nearest gene, while 40% of SNPs interacted with at least two genes, demonstrating the importance of considering long-range chromatin interactions when interpreting functional targets of disease loci. Our genomes contain around 20,000 different genes that code for instructions to create proteins and other important molecules. When changes, or mutations, occur within these genes, malfunctioning proteins that are damaging to the cell may be produced. Researchers of human genetics have tried to spot the genetic mutations that are associated with illnesses, for example heart diseases. However, they found that most of these mutations are actually located outside of genes, in the ‘non-coding’ areas that make up the majority of our genome. These mutations do not modify proteins directly, which makes it challenging to understand how they may be related to heart conditions. One possibility is that the genetic changes affect regions called enhancers, which control where, when and how much a gene is turned on by physically interacting with it. Mutations in enhancers could lead to a gene producing too much or too little of a protein, which might create problems in the cell. Yet, it is difficult to match an enhancer with the gene or genes it controls. One reason is that a non-coding region can influence a gene placed far away on the DNA strand. Indeed, the long DNA molecule precisely folds in on itself to fit inside its compartment in the cell, which can bring together distant sequences. Montefiori et al. take over 500 non-coding areas, which can carry mutations associated with heart diseases, and use a technique called Hi-C to try to identify which genes these regions may control. The tool can model the 3D organization of the genome, and it was further modified to capture only the regions of the genome that contain genes, and the DNA sequences that interact with them, in human heart cells. This helped to create a 3D map of 347 genes which come in contact with the non-coding areas that carry mutations associated with heart diseases. In fact, deleting those genes often causes heart disorders in mice. In addition, Montefiori et al. reveal that 90% of the non-coding regions examined were influencing genes that were far away. This shows that, despite a common assumption, enhancers often do not regulate the coding sequences they are nearest to on the DNA strand. Pinpointing the genes regulated by the non-coding regions involved in cardiovascular diseases could lead to new ways of treating or preventing these conditions. The 3D map created by Montefiori et al. may also help to visualize how the genetic information is organized in heart cells. This will contribute to the current effort to understand the role of the 3D structure of the genome, especially in different cell types.
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SourceType-Scholarly Journals-1
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ISSN:2050-084X
2050-084X
DOI:10.7554/eLife.35788