Single nucleotide polymorphisms with Cis-regulatory effects on long non-coding transcripts in human primary monocytes

Jonas Carlsson Almlöf; Per Lundmark; Anders Lundmark; Bing Ge; Tomi Pastinen; Alison H. Goodal; François Cambien; Panos Deloukas; Willem H. Ouwehand; Ann Christine Syvänen; Heribert Schunkert; Tony Attwood; Stephanie Belz; Peter Braund; Jessy Brocheton; Jason Cooper; Abi Crisp-Hihn; Patrick Diemert; Jeanette Erdmann; Nicola Foad; Tiphaine Godefroy; Jay Gracey; Emma Gray; Rhian Gwilliams; Susanne Heimerl; Christian Hengstenberg; Jennifer Jolley; Unni Krishnan; Heather Lloyd-Jones; Ulrika Liljedahl; Ingrid Lugauer; Seraya Maouche; Jasbir S. Moore; Gilles Montalescot; David Muir; Elizabeth Murray; Chris P. Nelson; Jessica Neudert; David Niblett; Karen O'Leary; Helen Pollard; Carole Proust; Angela Rankin; Augusto Rendon; Catherine M. Rice; Hendrik Sager; Nilesh J. Samani; Jennifer Sambrook; Gerd Schmitz; Michael Scholz; Laura Schroeder; Jonathan Stephens; Stefanie Tennstedt; Chris Wallace

doi:10.1371/journal.pone.0102612

Single nucleotide polymorphisms with Cis-regulatory effects on long non-coding transcripts in human primary monocytes

Jonas Carlsson Almlöf
, Per Lundmark
, Anders Lundmark
, Bing Ge
, Tomi Pastinen
, Alison H. Goodal
, François Cambien
, Panos Deloukas
, Willem H. Ouwehand
, Ann Christine Syvänen
, Heribert Schunkert
, Tony Attwood
, Stephanie Belz
, Peter Braund
, Jessy Brocheton
, Jason Cooper
, Abi Crisp-Hihn
, Patrick Diemert
, Jeanette Erdmann
, Nicola Foad

Tiphaine Godefroy, Jay Gracey, Emma Gray, Rhian Gwilliams, Susanne Heimerl, Christian Hengstenberg, Jennifer Jolley, Unni Krishnan, Heather Lloyd-Jones, Ulrika Liljedahl, Ingrid Lugauer, Seraya Maouche, Jasbir S. Moore, Gilles Montalescot, David Muir, Elizabeth Murray, Chris P. Nelson, Jessica Neudert, David Niblett, Karen O'Leary, Helen Pollard, Carole Proust, Angela Rankin, Augusto Rendon, Catherine M. Rice, Hendrik Sager, Nilesh J. Samani, Jennifer Sambrook, Gerd Schmitz, Michael Scholz, Laura Schroeder, Jonathan Stephens, Stefanie Tennstedt, Chris Wallace

Uppsala University
McGill University and Génome Québec Innovation Centre
University of Leicester
Glenfield Hospital
INSERM U70
Barts and The London School of Medicine and Dentistry
Wellcome Sanger Institute
King Abdulaziz University
Cambridge Biomedical Campus
University of Lübeck
University of Cambridge
University of Leicester
Cambridge Institute for Medical Research
Klinikum der Universität Regensburg und Medizinische Fakultät
Trium, Analysis Online GmbH
European Bioinformatics Institute
University of Regensburg

Research output: Contribution to journal › Article › peer-review

7 Scopus citations

Abstract

We applied genome-wide allele-specific expression analysis of monocytes from 188 samples. Monocytes were purified from white blood cells of healthy blood donors to detect cis-acting genetic variation that regulates the expression of long non-coding RNAs. We analysed 8929 regions harboring genes for potential long non-coding RNA that were retrieved from data from the ENCODE project. Of these regions, 60% were annotated as intergenic, which implies that they do not overlap with protein-coding genes. Focusing on the intergenic regions, and using stringent analysis of the allele-specific expression data, we detected robust cis-regulatory SNPs in 258 out of 489 informative intergenic regions included in the analysis. The cis-regulatory SNPs that were significantly associated with allele-specific expression of long non-coding RNAs were enriched to enhancer regions marked for active or bivalent, poised chromatin by histone modifications. Out of the lncRNA regions regulated by cis- acting regulatory SNPs, 20% (n = 52) were co-regulated with the closest protein coding gene. We compared the identified cis-regulatory SNPs with those in the catalog of SNPs identified by genome-wide association studies of human diseases and traits. This comparison identified 32 SNPs in loci from genome-wide association studies that displayed a strong association signal with allele-specific expression of non-coding RNAs in monocytes, with p-values ranging from 6.7×10^-7 to 9.5×10^-89. The identified cis-regulatory SNPs are associated with diseases of the immune system, like multiple sclerosis and rheumatoid arthritis.

Original language	English
Article number	e102612
Journal	PLoS ONE
Volume	9
Issue number	7
DOIs	https://doi.org/10.1371/journal.pone.0102612
State	Published - 15 Jul 2014
Externally published	Yes

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10.1371/journal.pone.0102612

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Almlöf, J. C., Lundmark, P., Lundmark, A., Ge, B., Pastinen, T., Goodal, A. H., Cambien, F., Deloukas, P., Ouwehand, W. H., Syvänen, A. C., Schunkert, H., Attwood, T., Belz, S., Braund, P., Brocheton, J., Cooper, J., Crisp-Hihn, A., Diemert, P., Erdmann, J., ... Wallace, C. (2014). Single nucleotide polymorphisms with Cis-regulatory effects on long non-coding transcripts in human primary monocytes. PLoS ONE, 9(7), Article e102612. https://doi.org/10.1371/journal.pone.0102612

@article{19646db214514b2e9c6ecceaf425ddf2,

title = "Single nucleotide polymorphisms with Cis-regulatory effects on long non-coding transcripts in human primary monocytes",

abstract = "We applied genome-wide allele-specific expression analysis of monocytes from 188 samples. Monocytes were purified from white blood cells of healthy blood donors to detect cis-acting genetic variation that regulates the expression of long non-coding RNAs. We analysed 8929 regions harboring genes for potential long non-coding RNA that were retrieved from data from the ENCODE project. Of these regions, 60\% were annotated as intergenic, which implies that they do not overlap with protein-coding genes. Focusing on the intergenic regions, and using stringent analysis of the allele-specific expression data, we detected robust cis-regulatory SNPs in 258 out of 489 informative intergenic regions included in the analysis. The cis-regulatory SNPs that were significantly associated with allele-specific expression of long non-coding RNAs were enriched to enhancer regions marked for active or bivalent, poised chromatin by histone modifications. Out of the lncRNA regions regulated by cis- acting regulatory SNPs, 20\% (n = 52) were co-regulated with the closest protein coding gene. We compared the identified cis-regulatory SNPs with those in the catalog of SNPs identified by genome-wide association studies of human diseases and traits. This comparison identified 32 SNPs in loci from genome-wide association studies that displayed a strong association signal with allele-specific expression of non-coding RNAs in monocytes, with p-values ranging from 6.7×10-7 to 9.5×10-89. The identified cis-regulatory SNPs are associated with diseases of the immune system, like multiple sclerosis and rheumatoid arthritis.",

author = "Alml{\"o}f, \{Jonas Carlsson\} and Per Lundmark and Anders Lundmark and Bing Ge and Tomi Pastinen and Goodal, \{Alison H.\} and Fran{\c c}ois Cambien and Panos Deloukas and Ouwehand, \{Willem H.\} and Syv{\"a}nen, \{Ann Christine\} and Heribert Schunkert and Tony Attwood and Stephanie Belz and Peter Braund and Jessy Brocheton and Jason Cooper and Abi Crisp-Hihn and Patrick Diemert and Jeanette Erdmann and Nicola Foad and Tiphaine Godefroy and Jay Gracey and Emma Gray and Rhian Gwilliams and Susanne Heimerl and Christian Hengstenberg and Jennifer Jolley and Unni Krishnan and Heather Lloyd-Jones and Ulrika Liljedahl and Ingrid Lugauer and Seraya Maouche and Moore, \{Jasbir S.\} and Gilles Montalescot and David Muir and Elizabeth Murray and Nelson, \{Chris P.\} and Jessica Neudert and David Niblett and Karen O'Leary and Helen Pollard and Carole Proust and Angela Rankin and Augusto Rendon and Rice, \{Catherine M.\} and Hendrik Sager and Samani, \{Nilesh J.\} and Jennifer Sambrook and Gerd Schmitz and Michael Scholz and Laura Schroeder and Jonathan Stephens and Stefanie Tennstedt and Chris Wallace",

year = "2014",

month = jul,

day = "15",

doi = "10.1371/journal.pone.0102612",

language = "English",

volume = "9",

journal = "PLoS ONE",

issn = "1932-6203",

publisher = "Public Library of Science",

number = "7",

}

Almlöf, JC, Lundmark, P, Lundmark, A, Ge, B, Pastinen, T, Goodal, AH, Cambien, F, Deloukas, P, Ouwehand, WH, Syvänen, AC, Schunkert, H, Attwood, T, Belz, S, Braund, P, Brocheton, J, Cooper, J, Crisp-Hihn, A, Diemert, P, Erdmann, J, Foad, N, Godefroy, T, Gracey, J, Gray, E, Gwilliams, R, Heimerl, S, Hengstenberg, C, Jolley, J, Krishnan, U, Lloyd-Jones, H, Liljedahl, U, Lugauer, I, Maouche, S, Moore, JS, Montalescot, G, Muir, D, Murray, E, Nelson, CP, Neudert, J, Niblett, D, O'Leary, K, Pollard, H, Proust, C, Rankin, A, Rendon, A, Rice, CM, Sager, H, Samani, NJ, Sambrook, J, Schmitz, G, Scholz, M, Schroeder, L, Stephens, J, Tennstedt, S & Wallace, C 2014, 'Single nucleotide polymorphisms with Cis-regulatory effects on long non-coding transcripts in human primary monocytes', PLoS ONE, vol. 9, no. 7, e102612. https://doi.org/10.1371/journal.pone.0102612

TY - JOUR

T1 - Single nucleotide polymorphisms with Cis-regulatory effects on long non-coding transcripts in human primary monocytes

AU - Almlöf, Jonas Carlsson

AU - Lundmark, Per

AU - Lundmark, Anders

AU - Ge, Bing

AU - Pastinen, Tomi

AU - Goodal, Alison H.

AU - Cambien, François

AU - Deloukas, Panos

AU - Ouwehand, Willem H.

AU - Syvänen, Ann Christine

AU - Schunkert, Heribert

AU - Attwood, Tony

AU - Belz, Stephanie

AU - Braund, Peter

AU - Brocheton, Jessy

AU - Cooper, Jason

AU - Crisp-Hihn, Abi

AU - Diemert, Patrick

AU - Erdmann, Jeanette

AU - Foad, Nicola

AU - Godefroy, Tiphaine

AU - Gracey, Jay

AU - Gray, Emma

AU - Gwilliams, Rhian

AU - Heimerl, Susanne

AU - Hengstenberg, Christian

AU - Jolley, Jennifer

AU - Krishnan, Unni

AU - Lloyd-Jones, Heather

AU - Liljedahl, Ulrika

AU - Lugauer, Ingrid

AU - Maouche, Seraya

AU - Moore, Jasbir S.

AU - Montalescot, Gilles

AU - Muir, David

AU - Murray, Elizabeth

AU - Nelson, Chris P.

AU - Neudert, Jessica

AU - Niblett, David

AU - O'Leary, Karen

AU - Pollard, Helen

AU - Proust, Carole

AU - Rankin, Angela

AU - Rendon, Augusto

AU - Rice, Catherine M.

AU - Sager, Hendrik

AU - Samani, Nilesh J.

AU - Sambrook, Jennifer

AU - Schmitz, Gerd

AU - Scholz, Michael

AU - Schroeder, Laura

AU - Stephens, Jonathan

AU - Tennstedt, Stefanie

AU - Wallace, Chris

PY - 2014/7/15

Y1 - 2014/7/15

N2 - We applied genome-wide allele-specific expression analysis of monocytes from 188 samples. Monocytes were purified from white blood cells of healthy blood donors to detect cis-acting genetic variation that regulates the expression of long non-coding RNAs. We analysed 8929 regions harboring genes for potential long non-coding RNA that were retrieved from data from the ENCODE project. Of these regions, 60% were annotated as intergenic, which implies that they do not overlap with protein-coding genes. Focusing on the intergenic regions, and using stringent analysis of the allele-specific expression data, we detected robust cis-regulatory SNPs in 258 out of 489 informative intergenic regions included in the analysis. The cis-regulatory SNPs that were significantly associated with allele-specific expression of long non-coding RNAs were enriched to enhancer regions marked for active or bivalent, poised chromatin by histone modifications. Out of the lncRNA regions regulated by cis- acting regulatory SNPs, 20% (n = 52) were co-regulated with the closest protein coding gene. We compared the identified cis-regulatory SNPs with those in the catalog of SNPs identified by genome-wide association studies of human diseases and traits. This comparison identified 32 SNPs in loci from genome-wide association studies that displayed a strong association signal with allele-specific expression of non-coding RNAs in monocytes, with p-values ranging from 6.7×10-7 to 9.5×10-89. The identified cis-regulatory SNPs are associated with diseases of the immune system, like multiple sclerosis and rheumatoid arthritis.

AB - We applied genome-wide allele-specific expression analysis of monocytes from 188 samples. Monocytes were purified from white blood cells of healthy blood donors to detect cis-acting genetic variation that regulates the expression of long non-coding RNAs. We analysed 8929 regions harboring genes for potential long non-coding RNA that were retrieved from data from the ENCODE project. Of these regions, 60% were annotated as intergenic, which implies that they do not overlap with protein-coding genes. Focusing on the intergenic regions, and using stringent analysis of the allele-specific expression data, we detected robust cis-regulatory SNPs in 258 out of 489 informative intergenic regions included in the analysis. The cis-regulatory SNPs that were significantly associated with allele-specific expression of long non-coding RNAs were enriched to enhancer regions marked for active or bivalent, poised chromatin by histone modifications. Out of the lncRNA regions regulated by cis- acting regulatory SNPs, 20% (n = 52) were co-regulated with the closest protein coding gene. We compared the identified cis-regulatory SNPs with those in the catalog of SNPs identified by genome-wide association studies of human diseases and traits. This comparison identified 32 SNPs in loci from genome-wide association studies that displayed a strong association signal with allele-specific expression of non-coding RNAs in monocytes, with p-values ranging from 6.7×10-7 to 9.5×10-89. The identified cis-regulatory SNPs are associated with diseases of the immune system, like multiple sclerosis and rheumatoid arthritis.

UR - https://www.scopus.com/pages/publications/84904249622

U2 - 10.1371/journal.pone.0102612

DO - 10.1371/journal.pone.0102612

M3 - Article

C2 - 25025429

AN - SCOPUS:84904249622

SN - 1932-6203

VL - 9

JO - PLoS ONE

JF - PLoS ONE

IS - 7

M1 - e102612

ER -

Single nucleotide polymorphisms with Cis-regulatory effects on long non-coding transcripts in human primary monocytes

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