Type 2 Diabetes–Associated Genetic Variants Regulate Chromatin Accessibility in Human Islets

Khetan, Shubham; Kursawe, Romy; Youn, Ahrim; Lawlor, Nathan; Jillette, Alexandria; Márquez, Eladio J.; Ucar, Duygu; Stitzel, Michael L.

doi:10.2337/db18-0393

Cited by 57 publications

(95 citation statements)

References 56 publications

(99 reference statements)

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“…To confirm library quality, we first analyzed the data as ensemble ATAC-seq by aggregating all high-quality mapped reads irrespective of barcode. Ensemble snATAC-seq from all three samples showed the expected insert size distribution (Supplementary Figure 1a), strong enrichment of signal at transcription start sites (TSS) (Supplementary Figure 1b), and high concordance of signal with published islet ATAC-seq data 14,27–29 (Supplementary Figure 1c).…”

Section: Resultsmentioning

confidence: 59%

Single cell chromatin accessibility reveals pancreatic islet cell type- and state-specific regulatory programs of diabetes risk

Chiou

Zeng

Zhang

et al. 2019

Preprint

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43Genetic risk variants for complex, multifactorial diseases are enriched in cis-regulatory elements. 44Single cell epigenomic technologies create new opportunities to dissect cell type-specific 45 mechanisms of risk variants, yet this approach has not been widely applied to disease-relevant 46 tissues. Given the central role of pancreatic islets in type 2 diabetes (T2D) pathophysiology, we 47 generated accessible chromatin profiles from 14.2k islet cells and identified 13 cell clusters 48 including multiple alpha, beta and delta cell clusters which represented hormone-producing and 49 signal-responsive cell states. We cataloged 244,236 islet cell type accessible chromatin sites and 50 identified transcription factors (TFs) underlying both lineage-and state-specific regulation. We 51 measured the enrichment of T2D and glycemic trait GWAS for the accessible chromatin profiles 52 of single cells, which revealed heterogeneity in the effects of beta cell states and TFs on fasting 53 glucose and T2D risk. We further used machine learning to predict the cell type-specific regulatory 54 function of genetic variants, and single cell co-accessibility to link distal sites to putative cell type-55 specific target genes. We localized 239 fine-mapped T2D risk signals to islet accessible 56 chromatin, and further prioritized variants at these signals with predicted regulatory function and 57 co-accessibility with target genes. At the KCNQ1 locus, the causal T2D variant rs231361 had 58 predicted effects on an enhancer with beta cell-specific, long-range co-accessibility to the insulin 59 promoter, and deletion of this enhancer reduced insulin gene and protein expression in human 60 embryonic stem cell-derived beta cells. Our findings provide a cell type-and state-resolved map 61 of gene regulation in human islets, illuminate likely mechanisms of T2D risk at hundreds of loci, 62 and demonstrate the power of single cell epigenomics for interpreting complex disease genetics. 63 64 65 66 67 68 69 70 71 72 73 Gene regulatory programs are largely orchestrated by cis-regulatory elements that direct the 74 expression of genes in response to specific developmental and environmental cues. Genetic 75 variants associated with disease by genome-wide association studies (GWAS) are highly 76 enriched within putative cis-regulatory elements 1 , highlighting the importance of regulatory 77 sequence in mediating disease risk. The activity of regulatory elements is often restricted to 78 specific cell types and/or cell states, limiting the ability of ATAC-seq and other "ensemble" (or 79 "bulk") epigenomic technologies to map regulatory elements in individual cell types within disease-80 relevant tissues. To overcome this limitation, new approaches to obtain ATAC-seq profiles from 81 single nuclei (snATAC-seq) allow for the disaggregation of open chromatin from heterogenous 82 samples into component cell types and subtypes 2-5 . These developments create opportunities to 83dissect the molecular mechanisms that underlie genetic risk of disease. How...

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Section: Resultsmentioning

confidence: 59%

Single cell chromatin accessibility reveals pancreatic islet cell type- and state-specific regulatory programs of diabetes risk

Chiou

Zeng

Zhang

et al. 2019

Preprint

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“…To test putative islet β cell regulatory sequences for their ability to enhance transcription from a minimal promoter and to identify SNPs that alter regulatory activity, we generated an MPRA library containing: i) 1,910 SNPs significantly associated with changes in human islet chromatin accessibility (caQTLs) 11 ; ii) 2,218 control SNPs overlapping human islet ATAC-seq peaks, which were reported to have no correlation with changes in human islet chromatin accessibility 11 ; and iii) 2,500 index and genetically linked (r 2 >0.8) SNPs/indels corresponding to 259 T2D association signals in the NHGRI/EBI GWAS Catalogue (Figure 1a, Table S2, and Methods). In total, 13,628 two-hundred base pair (bp) sequences from the human genome were included in this MPRA library.…”

Section: Resultsmentioning

confidence: 99%

“…SNPs associated with chromatin accessibility changes in islets (caQTLs) were significantly closer to the ATAC-seq peak summits than control SNPs, which are SNPs that reside in ATAC-seq peaks 11 but were not associated with chromatin accessibility changes in islets (Figure 4a). Consequently, caQTL SNPs were more likely to be MPRA active than were control SNPs (Figure 4b).…”

Section: Resultsmentioning

confidence: 99%

“…Studies designed to identify chromatin accessibility quantitative trait loci (caQTL) are being increasingly applied to nominate SNPs altering CRE activity 9, 10 . Previously, we identified 2,949 caQTLs in human islets 11 , which were significantly enriched for type 2 diabetes (T2D)-associated SNPs, highlighting the utility of this approach to nominate putative disease-associated SNPs affecting CRE activity in relevant cell types. However, caQTLs are correlative associations, and high throughput assays to directly test variant effects are needed to experimentally establish causality.…”

Section: Introductionmentioning

confidence: 99%

“…Although studies over the past several years implicate altered islet CRE function in T2D genetic risk and progression, they have colocalized only ∼1/4 of T2D-associated loci to altered chromatin accessibility and/or gene expression levels in islets 11, 17–20 . We hypothesize that this is partially because previous studies measured chromatin accessibility (caQTLs) and gene expression (eQTL) in islets cultured under steady state conditions 11, 21 , consequently missing important gene-environment interactions characteristic of a complex disorder like T2D. For example, endoplasmic reticulum (ER) stress, which is elicited by the high demands of insulin production and secretion on protein folding capacity in β cells, leads to (patho)physiologic adaptations.…”

Section: Introductionmentioning

confidence: 99%

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Functional characterization of thousands of type 2 diabetes-associated and chromatin-modulating variants under steady state and endoplasmic reticulum stress

Khetan

Kales

Kursawe

et al. 2020

Preprint

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A major goal in functional genomics and complex disease genetics is to identify functional cis-regulatory elements (CREs) and single nucleotide polymorphisms (SNPs) altering CRE activity in disease-relevant cell types and environmental conditions. We tested >13,000 sequences containing each allele of 6,628 SNPs associated with altered in vivo chromatin accessibility in human islets and/or type 2 diabetes risk (T2D GWAS SNPs) for transcriptional activity in ß cell under steady state and endoplasmic reticulum (ER) stress conditions using the massively parallel reporter assay (MPRA). Approximately 30% (n=1,983) of putative CREs were active in at least one condition. SNP allelic effects on in vitro MPRA activity strongly correlated with their effects on in vivo islet chromatin accessibility (Pearson r=0.52), i.e., alleles associated with increased chromatin accessibility exhibited higher MPRA activity. Importantly, MPRA identified 220/2500 T2D GWAS SNPs, representing 104 distinct association signals, that significantly altered transcriptional activity in ß cells. This study has thus identified functional ß cell transcription-activating sequences with in vivo relevance, uncovered regulatory features that modulate transcriptional activity in ß cells under steady state and ER stress conditions, and substantially expanded the set of putative functional variants that modulate transcriptional activity in ß cells from thousands of genetically-linked T2D GWAS SNPs.

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Fine mapping with epigenetic information and 3D structure

Orozco

2022

Semin Immunopathol

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Since 2005, thousands of genome-wide association studies (GWAS) have been published, identifying hundreds of thousands of genetic variants that increase risk of complex traits such as autoimmune diseases. This wealth of data has the potential to improve patient care, through personalized medicine and the identification of novel drug targets. However, the potential of GWAS for clinical translation has not been fully achieved yet, due to the fact that the functional interpretation of risk variants and the identification of causal variants and genes are challenging. The past decade has seen the development of great advances that are facilitating the overcoming of these limitations, by utilizing a plethora of genomics and epigenomics tools to map and characterize regulatory elements and chromatin interactions, which can be used to fine map GWAS loci, and advance our understanding of the biological mechanisms that cause disease.

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Type 2 Diabetes–Associated Genetic Variants Regulate Chromatin Accessibility in Human Islets

Cited by 57 publications

References 56 publications

Single cell chromatin accessibility reveals pancreatic islet cell type- and state-specific regulatory programs of diabetes risk

Single cell chromatin accessibility reveals pancreatic islet cell type- and state-specific regulatory programs of diabetes risk

Functional characterization of thousands of type 2 diabetes-associated and chromatin-modulating variants under steady state and endoplasmic reticulum stress

Fine mapping with epigenetic information and 3D structure

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