Variant-To-gene-mapping analyses reveal a role for pancreatic islet cells in conferring genetic susceptibility to sleep-related traits

Chiara Lasconi; Matthew C. Pahl; James A. Pippin; Chun Su; Matthew E. Johnson; Alessandra Chesi; Keith Boehm; Elisabetta Manduchi; Kristy Ou; Maria L. Golson; Andrew D. Wells; Klaus H. Kaestner; Struan F.A. Grant

doi:10.1093/sleep/zsac109

Variant-To-gene-mapping analyses reveal a role for pancreatic islet cells in conferring genetic susceptibility to sleep-related traits

Chiara Lasconi, Matthew C. Pahl, James A. Pippin, Chun Su, Matthew E. Johnson, Alessandra Chesi, Keith Boehm, Elisabetta Manduchi, Kristy Ou, Maria L. Golson, Andrew D. Wells, Klaus H. Kaestner, Struan F.A. Grant

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Abstract

We investigated the potential role of sleep-Trait associated genetic loci in conferring a degree of their effect via pancreatic α-and β-cells, given that both sleep disturbances and metabolic disorders, including type 2 diabetes and obesity, involve polygenic contributions and complex interactions. We determined genetic commonalities between sleep and metabolic disorders, conducting linkage disequilibrium genetic correlation analyses with publicly available GWAS summary statistics. Then we investigated possible enrichment of sleep-Trait associated SNPs in promoter-interacting open chromatin regions within α-and β-cells, intersecting public GWAS reports with our own ATAC-seq and high-resolution promoter-focused Capture C data generated from both sorted human α-cells and an established human beta-cell line (EndoC-βH1). Finally, we identified putative effector genes physically interacting with sleep-Trait associated variants in α-and EndoC-βH1cells running variant-To-gene mapping and establish pathways in which these genes are significantly involved. We observed that insomnia, short and long sleep-but not morningness-were significantly correlated with type 2 diabetes, obesity and other metabolic traits. Both the EndoC-βH1 and α-cells were enriched for insomnia loci (p =. 01; p =. 0076), short sleep loci (p =. 017; p =. 022) and morningness loci (p = 2.2 × 10-7; p =. 0016), while the α-cells were also enriched for long sleep loci (p =. 034). Utilizing our promoter contact data, we identified 63 putative effector genes in EndoC-βH1 and 76 putative effector genes in α-cells, with these genes showing significant enrichment for organonitrogen and organophosphate biosynthesis, phosphatidylinositol and phosphorylation, intracellular transport and signaling, stress responses and cell differentiation. Our data suggest that a subset of sleep-related loci confer their effects via cells in pancreatic islets.

Original language	English (US)
Article number	zsac109
Journal	Sleep
Volume	45
Issue number	8
DOIs	https://doi.org/10.1093/sleep/zsac109
State	Published - Aug 1 2022
Externally published	Yes

Keywords

GWAS
alpha cell
beta cell
chromatin conformation capture
epigenetics
metabolism
pancreas
sleep

ASJC Scopus subject areas

Clinical Neurology
Physiology (medical)

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10.1093/sleep/zsac109

Cite this

Lasconi, C., Pahl, M. C., Pippin, J. A., Su, C., Johnson, M. E., Chesi, A., Boehm, K., Manduchi, E., Ou, K., Golson, M. L., Wells, A. D., Kaestner, K. H., & Grant, S. F. A. (2022). Variant-To-gene-mapping analyses reveal a role for pancreatic islet cells in conferring genetic susceptibility to sleep-related traits. Sleep, 45(8), Article zsac109. https://doi.org/10.1093/sleep/zsac109

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title = "Variant-To-gene-mapping analyses reveal a role for pancreatic islet cells in conferring genetic susceptibility to sleep-related traits",

abstract = "We investigated the potential role of sleep-Trait associated genetic loci in conferring a degree of their effect via pancreatic α-and β-cells, given that both sleep disturbances and metabolic disorders, including type 2 diabetes and obesity, involve polygenic contributions and complex interactions. We determined genetic commonalities between sleep and metabolic disorders, conducting linkage disequilibrium genetic correlation analyses with publicly available GWAS summary statistics. Then we investigated possible enrichment of sleep-Trait associated SNPs in promoter-interacting open chromatin regions within α-and β-cells, intersecting public GWAS reports with our own ATAC-seq and high-resolution promoter-focused Capture C data generated from both sorted human α-cells and an established human beta-cell line (EndoC-βH1). Finally, we identified putative effector genes physically interacting with sleep-Trait associated variants in α-and EndoC-βH1cells running variant-To-gene mapping and establish pathways in which these genes are significantly involved. We observed that insomnia, short and long sleep-but not morningness-were significantly correlated with type 2 diabetes, obesity and other metabolic traits. Both the EndoC-βH1 and α-cells were enriched for insomnia loci (p =. 01; p =. 0076), short sleep loci (p =. 017; p =. 022) and morningness loci (p = 2.2 × 10-7; p =. 0016), while the α-cells were also enriched for long sleep loci (p =. 034). Utilizing our promoter contact data, we identified 63 putative effector genes in EndoC-βH1 and 76 putative effector genes in α-cells, with these genes showing significant enrichment for organonitrogen and organophosphate biosynthesis, phosphatidylinositol and phosphorylation, intracellular transport and signaling, stress responses and cell differentiation. Our data suggest that a subset of sleep-related loci confer their effects via cells in pancreatic islets.",

keywords = "GWAS, alpha cell, beta cell, chromatin conformation capture, epigenetics, metabolism, pancreas, sleep",

author = "Chiara Lasconi and Pahl, {Matthew C.} and Pippin, {James A.} and Chun Su and Johnson, {Matthew E.} and Alessandra Chesi and Keith Boehm and Elisabetta Manduchi and Kristy Ou and Golson, {Maria L.} and Wells, {Andrew D.} and Kaestner, {Klaus H.} and Grant, {Struan F.A.}",

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doi = "10.1093/sleep/zsac109",

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T1 - Variant-To-gene-mapping analyses reveal a role for pancreatic islet cells in conferring genetic susceptibility to sleep-related traits

AU - Lasconi, Chiara

AU - Pahl, Matthew C.

AU - Pippin, James A.

AU - Su, Chun

AU - Johnson, Matthew E.

AU - Chesi, Alessandra

AU - Boehm, Keith

AU - Manduchi, Elisabetta

AU - Ou, Kristy

AU - Golson, Maria L.

AU - Wells, Andrew D.

AU - Kaestner, Klaus H.

AU - Grant, Struan F.A.

PY - 2022/8/1

Y1 - 2022/8/1

N2 - We investigated the potential role of sleep-Trait associated genetic loci in conferring a degree of their effect via pancreatic α-and β-cells, given that both sleep disturbances and metabolic disorders, including type 2 diabetes and obesity, involve polygenic contributions and complex interactions. We determined genetic commonalities between sleep and metabolic disorders, conducting linkage disequilibrium genetic correlation analyses with publicly available GWAS summary statistics. Then we investigated possible enrichment of sleep-Trait associated SNPs in promoter-interacting open chromatin regions within α-and β-cells, intersecting public GWAS reports with our own ATAC-seq and high-resolution promoter-focused Capture C data generated from both sorted human α-cells and an established human beta-cell line (EndoC-βH1). Finally, we identified putative effector genes physically interacting with sleep-Trait associated variants in α-and EndoC-βH1cells running variant-To-gene mapping and establish pathways in which these genes are significantly involved. We observed that insomnia, short and long sleep-but not morningness-were significantly correlated with type 2 diabetes, obesity and other metabolic traits. Both the EndoC-βH1 and α-cells were enriched for insomnia loci (p =. 01; p =. 0076), short sleep loci (p =. 017; p =. 022) and morningness loci (p = 2.2 × 10-7; p =. 0016), while the α-cells were also enriched for long sleep loci (p =. 034). Utilizing our promoter contact data, we identified 63 putative effector genes in EndoC-βH1 and 76 putative effector genes in α-cells, with these genes showing significant enrichment for organonitrogen and organophosphate biosynthesis, phosphatidylinositol and phosphorylation, intracellular transport and signaling, stress responses and cell differentiation. Our data suggest that a subset of sleep-related loci confer their effects via cells in pancreatic islets.

AB - We investigated the potential role of sleep-Trait associated genetic loci in conferring a degree of their effect via pancreatic α-and β-cells, given that both sleep disturbances and metabolic disorders, including type 2 diabetes and obesity, involve polygenic contributions and complex interactions. We determined genetic commonalities between sleep and metabolic disorders, conducting linkage disequilibrium genetic correlation analyses with publicly available GWAS summary statistics. Then we investigated possible enrichment of sleep-Trait associated SNPs in promoter-interacting open chromatin regions within α-and β-cells, intersecting public GWAS reports with our own ATAC-seq and high-resolution promoter-focused Capture C data generated from both sorted human α-cells and an established human beta-cell line (EndoC-βH1). Finally, we identified putative effector genes physically interacting with sleep-Trait associated variants in α-and EndoC-βH1cells running variant-To-gene mapping and establish pathways in which these genes are significantly involved. We observed that insomnia, short and long sleep-but not morningness-were significantly correlated with type 2 diabetes, obesity and other metabolic traits. Both the EndoC-βH1 and α-cells were enriched for insomnia loci (p =. 01; p =. 0076), short sleep loci (p =. 017; p =. 022) and morningness loci (p = 2.2 × 10-7; p =. 0016), while the α-cells were also enriched for long sleep loci (p =. 034). Utilizing our promoter contact data, we identified 63 putative effector genes in EndoC-βH1 and 76 putative effector genes in α-cells, with these genes showing significant enrichment for organonitrogen and organophosphate biosynthesis, phosphatidylinositol and phosphorylation, intracellular transport and signaling, stress responses and cell differentiation. Our data suggest that a subset of sleep-related loci confer their effects via cells in pancreatic islets.

KW - GWAS

KW - alpha cell

KW - beta cell

KW - chromatin conformation capture

KW - epigenetics

KW - metabolism

KW - pancreas

KW - sleep

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JO - Sleep

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Variant-To-gene-mapping analyses reveal a role for pancreatic islet cells in conferring genetic susceptibility to sleep-related traits

Abstract

Keywords

ASJC Scopus subject areas

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