Long-range DNA looping and gene expression analyses identify DEXI as an autoimmune disease candidate gene

Lucy J. Davison; Chris Wallace; Jason D. Cooper; Nathan F. Cope; Nicola K. Wilson; Deborah J. Smyth; Joanna M.M. Howson; Nada Saleh; Abdullah Al-Jeffery; Karen L. Angus; Helen E. Stevens; Sarah Nutland; Simon Duley; Richard M.R. Coulson; Neil M. Walker; Oliver S. Burren; Catherine M. Rice; Francois Cambien; Tanja Zeller; Thomas Munzel; Karl Lackner; Stefan Blankenberg; Peter Fraser; Berthold Gottgens; John A. Todd; Stephanie Tennstedt

doi:10.1093/hmg/ddr468

Long-range DNA looping and gene expression analyses identify DEXI as an autoimmune disease candidate gene

Lucy J. Davison^*, Chris Wallace, Jason D. Cooper, Nathan F. Cope, Nicola K. Wilson, Deborah J. Smyth, Joanna M.M. Howson, Nada Saleh, Abdullah Al-Jeffery, Karen L. Angus, Helen E. Stevens, Sarah Nutland, Simon Duley, Richard M.R. Coulson, Neil M. Walker, Oliver S. Burren, Catherine M. Rice, Francois Cambien, Tanja Zeller, Thomas MunzelKarl Lackner, Stefan Blankenberg, Peter Fraser, Berthold Gottgens, John A. Todd, Stephanie Tennstedt

^*Korrespondierende/r Autor/-in für diese Arbeit

Institut für Kardiogenetik

96 Zitate (Scopus)

Abstract

The chromosome 16p13 region has been associated with several autoimmune diseases, including type 1 diabetes (T1D) and multiple sclerosis (MS). CLEC16A has been reported as the most likely candidate gene in the region, since it contains the most disease-associated single-nucleotide polymorphisms (SNPs), as well as an imunoreceptor tyrosine-based activation motif. However, here we report that intron 19 of CLEC16A, containing the most autoimmune disease-associated SNPs, appears to behave as a regulatory sequence, affecting the expression of a neighbouring gene, DEXI. The CLEC16A alleles that are protective from T1D and MS are associated with increased expression of DEXI, and no other genes in the region, in two independent monocyte gene expression data sets. Critically, using chromosome conformation capture (3C), we identified physical proximity between the DEXI promoter region and intron 19 of CLEC16A, separated by a loop of >150 kb. In reciprocal experiments, a 20 kb fragment of intron 19 of CLEC16A, containing SNPs associated with T1D and MS, as well as with DEXI expression, interacted with the promotor region of DEXI but not with candidate DNA fragments containing other potential causal genes in the region, including CLEC16A. Intron 19 of CLEC16A is highly enriched for transcription-factor-binding events and markers associated with enhancer activity. Taken together, these data indicate that although the causal variants in the 16p13 region lie within CLEC16A, DEXI is an unappreciated autoimmune disease candidate gene, and illustrate the power of the 3C approach in progressing from genome-wide association studies results to candidate causal genes.

Originalsprache	Englisch
Aufsatznummer	ddr468
Zeitschrift	Human Molecular Genetics
Jahrgang	21
Ausgabenummer	2
Seiten (von - bis)	322-333
Seitenumfang	12
ISSN	0964-6906
DOIs	https://doi.org/10.1093/hmg/ddr468
Publikationsstatus	Veröffentlicht - 01.01.2012

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Bioinformatic and T1DBase support was provided by O.S.B. and R.M.R.C. This study makes use of data generated by the Wellcome Trust Case Control Consortium. A full list of the investigators who contributed to the generation of the data is available from http://www.wtccc.org.uk/. We also thank P. Clarke, G. Coleman, D. Harrison, S. Hawkins, M. Maisuria-Armer, T. Mistry and N. Taylor for the preparation of DNA samples. We thank Bing Ge and Tomi Pastinen for sharing their PeakPicker software. We are grateful to Randy Read for helpful discussion. We acknowledge the use of DNA from The UK Blood Services collection of Common Controls (UKBS collection), funded by the Wellcome Trust grant 076113/C/04/Z, by the Wellcome Trust/Juvenile Diabetes Research Foundation grant 061858 and by the National Institute of Health Research of England. The collection was established as part of the Wellcome Trust Case-Control Consortium. Funding for the project was provided by the Wellcome Trust under award 076113. L.J.D. is supported by a Wellcome Trust Intermediate Clinical Fellowship (082549/Z/07/Z). C.W. is supported by a Wellcome Trust Career Development Fellowship (089989/Z/09/Z). K.L.A. is supported by a 4-year Wellcome Trust CIMR PhD studentship. N.K.W. is supported by the Medical Research Council. N.S. and A.A. are supported by King Saud bin Abdu-laziz University of Health Sciences and the Saudi Ministry for Higher Education. This work was funded by the Juvenile Diabetes Research Foundation International, the Wellcome Trust and the National Institute for Health Research Cambridge Biomedical Centre. The Cambridge Institute for Medical Research (CIMR) is in receipt of a Wellcome Trust Strategic Award (079895). The Gutenberg Health Study is funded through the government of Rheinland-Pfalz (Stiftung Rheinland Pfalz für Innovation, contract number AZ 961-386261/ 733), the research programs Wissen schafft Zukunft and Schwerpunkt Vaskuläre Prävention of the Johannes Gutenberg-University of Mainz and its contract with Boehringer Ingelheim and PHILIPS Medical Systems including an unrestricted grant for the Gutenberg Health Study. Specifically, the research reported in this article was supported by the National Genome Network NGFNplus (contract number project A3 01GS0833) by the Federal Ministry of Education and Research, Germany. Funding to pay the Open Access publication charges for this article was provided by the Wellcome Trust.

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Davison, L. J., Wallace, C., Cooper, J. D., Cope, N. F., Wilson, N. K., Smyth, D. J., Howson, J. M. M., Saleh, N., Al-Jeffery, A., Angus, K. L., Stevens, H. E., Nutland, S., Duley, S., Coulson, R. M. R., Walker, N. M., Burren, O. S., Rice, C. M., Cambien, F., Zeller, T., ... Tennstedt, S. (2012). Long-range DNA looping and gene expression analyses identify DEXI as an autoimmune disease candidate gene. Human Molecular Genetics, 21(2), 322-333. Artikel ddr468. https://doi.org/10.1093/hmg/ddr468

@article{65b6121317ee486bac0301eeebe9d045,

title = "Long-range DNA looping and gene expression analyses identify DEXI as an autoimmune disease candidate gene",

abstract = "The chromosome 16p13 region has been associated with several autoimmune diseases, including type 1 diabetes (T1D) and multiple sclerosis (MS). CLEC16A has been reported as the most likely candidate gene in the region, since it contains the most disease-associated single-nucleotide polymorphisms (SNPs), as well as an imunoreceptor tyrosine-based activation motif. However, here we report that intron 19 of CLEC16A, containing the most autoimmune disease-associated SNPs, appears to behave as a regulatory sequence, affecting the expression of a neighbouring gene, DEXI. The CLEC16A alleles that are protective from T1D and MS are associated with increased expression of DEXI, and no other genes in the region, in two independent monocyte gene expression data sets. Critically, using chromosome conformation capture (3C), we identified physical proximity between the DEXI promoter region and intron 19 of CLEC16A, separated by a loop of >150 kb. In reciprocal experiments, a 20 kb fragment of intron 19 of CLEC16A, containing SNPs associated with T1D and MS, as well as with DEXI expression, interacted with the promotor region of DEXI but not with candidate DNA fragments containing other potential causal genes in the region, including CLEC16A. Intron 19 of CLEC16A is highly enriched for transcription-factor-binding events and markers associated with enhancer activity. Taken together, these data indicate that although the causal variants in the 16p13 region lie within CLEC16A, DEXI is an unappreciated autoimmune disease candidate gene, and illustrate the power of the 3C approach in progressing from genome-wide association studies results to candidate causal genes.",

author = "Davison, \{Lucy J.\} and Chris Wallace and Cooper, \{Jason D.\} and Cope, \{Nathan F.\} and Wilson, \{Nicola K.\} and Smyth, \{Deborah J.\} and Howson, \{Joanna M.M.\} and Nada Saleh and Abdullah Al-Jeffery and Angus, \{Karen L.\} and Stevens, \{Helen E.\} and Sarah Nutland and Simon Duley and Coulson, \{Richard M.R.\} and Walker, \{Neil M.\} and Burren, \{Oliver S.\} and Rice, \{Catherine M.\} and Francois Cambien and Tanja Zeller and Thomas Munzel and Karl Lackner and Stefan Blankenberg and Peter Fraser and Berthold Gottgens and Todd, \{John A.\} and Stephanie Tennstedt",

year = "2012",

month = jan,

day = "1",

doi = "10.1093/hmg/ddr468",

language = "English",

volume = "21",

pages = "322--333",

journal = "Human Molecular Genetics",

issn = "0964-6906",

publisher = "Oxford University Press",

number = "2",

}

Davison, LJ, Wallace, C, Cooper, JD, Cope, NF, Wilson, NK, Smyth, DJ, Howson, JMM, Saleh, N, Al-Jeffery, A, Angus, KL, Stevens, HE, Nutland, S, Duley, S, Coulson, RMR, Walker, NM, Burren, OS, Rice, CM, Cambien, F, Zeller, T, Munzel, T, Lackner, K, Blankenberg, S, Fraser, P, Gottgens, B, Todd, JA & Tennstedt, S 2012, 'Long-range DNA looping and gene expression analyses identify DEXI as an autoimmune disease candidate gene', Human Molecular Genetics, Jg. 21, Nr. 2, ddr468, S. 322-333. https://doi.org/10.1093/hmg/ddr468

TY - JOUR

T1 - Long-range DNA looping and gene expression analyses identify DEXI as an autoimmune disease candidate gene

AU - Davison, Lucy J.

AU - Wallace, Chris

AU - Cooper, Jason D.

AU - Cope, Nathan F.

AU - Wilson, Nicola K.

AU - Smyth, Deborah J.

AU - Howson, Joanna M.M.

AU - Saleh, Nada

AU - Al-Jeffery, Abdullah

AU - Angus, Karen L.

AU - Stevens, Helen E.

AU - Nutland, Sarah

AU - Duley, Simon

AU - Coulson, Richard M.R.

AU - Walker, Neil M.

AU - Burren, Oliver S.

AU - Rice, Catherine M.

AU - Cambien, Francois

AU - Zeller, Tanja

AU - Munzel, Thomas

AU - Lackner, Karl

AU - Blankenberg, Stefan

AU - Fraser, Peter

AU - Gottgens, Berthold

AU - Todd, John A.

AU - Tennstedt, Stephanie

PY - 2012/1/1

Y1 - 2012/1/1

N2 - The chromosome 16p13 region has been associated with several autoimmune diseases, including type 1 diabetes (T1D) and multiple sclerosis (MS). CLEC16A has been reported as the most likely candidate gene in the region, since it contains the most disease-associated single-nucleotide polymorphisms (SNPs), as well as an imunoreceptor tyrosine-based activation motif. However, here we report that intron 19 of CLEC16A, containing the most autoimmune disease-associated SNPs, appears to behave as a regulatory sequence, affecting the expression of a neighbouring gene, DEXI. The CLEC16A alleles that are protective from T1D and MS are associated with increased expression of DEXI, and no other genes in the region, in two independent monocyte gene expression data sets. Critically, using chromosome conformation capture (3C), we identified physical proximity between the DEXI promoter region and intron 19 of CLEC16A, separated by a loop of >150 kb. In reciprocal experiments, a 20 kb fragment of intron 19 of CLEC16A, containing SNPs associated with T1D and MS, as well as with DEXI expression, interacted with the promotor region of DEXI but not with candidate DNA fragments containing other potential causal genes in the region, including CLEC16A. Intron 19 of CLEC16A is highly enriched for transcription-factor-binding events and markers associated with enhancer activity. Taken together, these data indicate that although the causal variants in the 16p13 region lie within CLEC16A, DEXI is an unappreciated autoimmune disease candidate gene, and illustrate the power of the 3C approach in progressing from genome-wide association studies results to candidate causal genes.

AB - The chromosome 16p13 region has been associated with several autoimmune diseases, including type 1 diabetes (T1D) and multiple sclerosis (MS). CLEC16A has been reported as the most likely candidate gene in the region, since it contains the most disease-associated single-nucleotide polymorphisms (SNPs), as well as an imunoreceptor tyrosine-based activation motif. However, here we report that intron 19 of CLEC16A, containing the most autoimmune disease-associated SNPs, appears to behave as a regulatory sequence, affecting the expression of a neighbouring gene, DEXI. The CLEC16A alleles that are protective from T1D and MS are associated with increased expression of DEXI, and no other genes in the region, in two independent monocyte gene expression data sets. Critically, using chromosome conformation capture (3C), we identified physical proximity between the DEXI promoter region and intron 19 of CLEC16A, separated by a loop of >150 kb. In reciprocal experiments, a 20 kb fragment of intron 19 of CLEC16A, containing SNPs associated with T1D and MS, as well as with DEXI expression, interacted with the promotor region of DEXI but not with candidate DNA fragments containing other potential causal genes in the region, including CLEC16A. Intron 19 of CLEC16A is highly enriched for transcription-factor-binding events and markers associated with enhancer activity. Taken together, these data indicate that although the causal variants in the 16p13 region lie within CLEC16A, DEXI is an unappreciated autoimmune disease candidate gene, and illustrate the power of the 3C approach in progressing from genome-wide association studies results to candidate causal genes.

UR - https://www.scopus.com/pages/publications/84855363144

U2 - 10.1093/hmg/ddr468

DO - 10.1093/hmg/ddr468

M3 - Journal articles

C2 - 21989056

AN - SCOPUS:84855363144

SN - 0964-6906

VL - 21

SP - 322

EP - 333

JO - Human Molecular Genetics

JF - Human Molecular Genetics

IS - 2

M1 - ddr468

ER -

Long-range DNA looping and gene expression analyses identify DEXI as an autoimmune disease candidate gene

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