Negligible impact of rare autoimmune-locus coding-region variants on missing heritability

Karen A. Hunt; Vanisha Mistry; Nicholas A. Bockett; Tariq Ahmad; Maria Ban; Jonathan N. Barker; Jeffrey C. Barrett; Hannah Blackburn; Oliver Brand; Oliver Burren; Francesca Capon; Alastair Compston; Stephen C. L. Gough; Luke Jostins; Yong Kong; James C. Lee; Monkol Lek; Daniel G. MacArthur; John C. Mansfield; Christopher G. Mathew; Charles A. Mein; Muddassar Mirza; Sarah Nutland; Suna Onengut-Gumuscu; Efterpi Papouli; Miles Parkes; Stephen S. Rich; Steven Sawcer; Jack Satsangi; Matthew J. Simmonds; Richard C. Trembath; Neil M. Walker; Eva Wozniak; John A. Todd; Michael A. Simpson; Vincent Plagnol; David A. van Heel

doi:10.1038/nature12170

Negligible impact of rare autoimmune-locus coding-region variants on missing heritability

Karen A. Hunt, Vanisha Mistry, Nicholas A. Bockett, Tariq Ahmad, Maria Ban, Jonathan N. Barker, Jeffrey C. Barrett, Hannah Blackburn, Oliver Brand, Oliver Burren, Francesca Capon, Alastair Compston, Stephen C. L. Gough, Luke Jostins, Yong Kong, James C. Lee, Monkol Lek, Daniel G. MacArthur, John C. Mansfield, Christopher G. MathewCharles A. Mein, Muddassar Mirza, Sarah Nutland, Suna Onengut-Gumuscu, Efterpi Papouli, Miles Parkes, Stephen S. Rich, Steven Sawcer, Jack Satsangi, Matthew J. Simmonds, Richard C. Trembath, Neil M. Walker, Eva Wozniak, John A. Todd, Michael A. Simpson, Vincent Plagnol, David A. van Heel^*

^*Corresponding author for this work

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

161 Citations (Scopus)

Abstract

Genome-wide association studies(GWAS) have identified common variants of modest-effect size at hundreds of loci for common autoimmune diseases; however, a substantial fraction of heritability remains unexplained, to which rare variants may contribute(1,2). To discover rare variants and test them for association with a phenotype, most studies re-sequence a small initial sample size and then genotype the discovered variants in a larger sample set(3-5). This approach fails to analyse a large fraction of the rare variants present in the entire sample set. Here we perform simultaneous amplicon-sequencing-based variant discovery and genotyping for coding exons of 25 GWAS risk genes in 41,911 UK residents of white European origin, comprising 24,892 subjects with six autoimmune disease phenotypes and 17,019 controls, and show that rare coding-region variants at known loci have a negligible role in common autoimmune disease susceptibility. These results do not support the rare-variant synthetic genome-wide-association hypothesis(6) (in which unobserved rare causal variants lead to association detected at common tag variants). Many known autoimmune disease risk loci contain multiple, independently associated, common and low-frequency variants, and so genes at these loci are a priori stronger candidates for harbouring rare coding-region variants than other genes. Our data indicate that the missing heritability for common autoimmune diseases may not be attributable to the rare coding-region variant portion of the allelic spectrum, but perhaps, as others have proposed, may be a result of many common-variant loci of weak effect(7-10).

Original language	English
Pages (from-to)	232-235
Number of pages	4
Journal	NATURE
Volume	498
Issue number	7453
DOIs	https://doi.org/10.1038/nature12170
Publication status	Published - 13 Jun 2013

Keywords

INFLAMMATORY-BOWEL-DISEASE
GENOME-WIDE ASSOCIATION
PSORIASIS SUSCEPTIBILITY LOCI
RHEUMATOID-ARTHRITIS
COMMON VARIANTS
LOW-FREQUENCY
GENES
RISK
ARCHITECTURE
REVEALS

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Hunt, K. A., Mistry, V., Bockett, N. A., Ahmad, T., Ban, M., Barker, J. N., Barrett, J. C., Blackburn, H., Brand, O., Burren, O., Capon, F., Compston, A., Gough, S. C. L., Jostins, L., Kong, Y., Lee, J. C., Lek, M., MacArthur, D. G., Mansfield, J. C., ... van Heel, D. A. (2013). Negligible impact of rare autoimmune-locus coding-region variants on missing heritability. NATURE, 498(7453), 232-235. https://doi.org/10.1038/nature12170

@article{18b5a3561cae4ca0837919544702a704,

title = "Negligible impact of rare autoimmune-locus coding-region variants on missing heritability",

abstract = "Genome-wide association studies(GWAS) have identified common variants of modest-effect size at hundreds of loci for common autoimmune diseases; however, a substantial fraction of heritability remains unexplained, to which rare variants may contribute(1,2). To discover rare variants and test them for association with a phenotype, most studies re-sequence a small initial sample size and then genotype the discovered variants in a larger sample set(3-5). This approach fails to analyse a large fraction of the rare variants present in the entire sample set. Here we perform simultaneous amplicon-sequencing-based variant discovery and genotyping for coding exons of 25 GWAS risk genes in 41,911 UK residents of white European origin, comprising 24,892 subjects with six autoimmune disease phenotypes and 17,019 controls, and show that rare coding-region variants at known loci have a negligible role in common autoimmune disease susceptibility. These results do not support the rare-variant synthetic genome-wide-association hypothesis(6) (in which unobserved rare causal variants lead to association detected at common tag variants). Many known autoimmune disease risk loci contain multiple, independently associated, common and low-frequency variants, and so genes at these loci are a priori stronger candidates for harbouring rare coding-region variants than other genes. Our data indicate that the missing heritability for common autoimmune diseases may not be attributable to the rare coding-region variant portion of the allelic spectrum, but perhaps, as others have proposed, may be a result of many common-variant loci of weak effect(7-10).",

keywords = "INFLAMMATORY-BOWEL-DISEASE, GENOME-WIDE ASSOCIATION, PSORIASIS SUSCEPTIBILITY LOCI, RHEUMATOID-ARTHRITIS, COMMON VARIANTS, LOW-FREQUENCY, GENES, RISK, ARCHITECTURE, REVEALS",

author = "Hunt, {Karen A.} and Vanisha Mistry and Bockett, {Nicholas A.} and Tariq Ahmad and Maria Ban and Barker, {Jonathan N.} and Barrett, {Jeffrey C.} and Hannah Blackburn and Oliver Brand and Oliver Burren and Francesca Capon and Alastair Compston and Gough, {Stephen C. L.} and Luke Jostins and Yong Kong and Lee, {James C.} and Monkol Lek and MacArthur, {Daniel G.} and Mansfield, {John C.} and Mathew, {Christopher G.} and Mein, {Charles A.} and Muddassar Mirza and Sarah Nutland and Suna Onengut-Gumuscu and Efterpi Papouli and Miles Parkes and Rich, {Stephen S.} and Steven Sawcer and Jack Satsangi and Simmonds, {Matthew J.} and Trembath, {Richard C.} and Walker, {Neil M.} and Eva Wozniak and Todd, {John A.} and Simpson, {Michael A.} and Vincent Plagnol and {van Heel}, {David A.}",

year = "2013",

month = jun,

day = "13",

doi = "10.1038/nature12170",

language = "English",

volume = "498",

pages = "232--235",

journal = "NATURE",

issn = "0028-0836",

publisher = "Nature Publishing Group",

number = "7453",

}

Hunt, KA, Mistry, V, Bockett, NA, Ahmad, T, Ban, M, Barker, JN, Barrett, JC, Blackburn, H, Brand, O, Burren, O, Capon, F, Compston, A, Gough, SCL, Jostins, L, Kong, Y, Lee, JC, Lek, M, MacArthur, DG, Mansfield, JC, Mathew, CG, Mein, CA, Mirza, M, Nutland, S, Onengut-Gumuscu, S, Papouli, E, Parkes, M, Rich, SS, Sawcer, S, Satsangi, J, Simmonds, MJ, Trembath, RC, Walker, NM, Wozniak, E, Todd, JA, Simpson, MA, Plagnol, V & van Heel, DA 2013, 'Negligible impact of rare autoimmune-locus coding-region variants on missing heritability', NATURE, vol. 498, no. 7453, pp. 232-235. https://doi.org/10.1038/nature12170

TY - JOUR

T1 - Negligible impact of rare autoimmune-locus coding-region variants on missing heritability

AU - Hunt, Karen A.

AU - Mistry, Vanisha

AU - Bockett, Nicholas A.

AU - Ahmad, Tariq

AU - Ban, Maria

AU - Barker, Jonathan N.

AU - Barrett, Jeffrey C.

AU - Blackburn, Hannah

AU - Brand, Oliver

AU - Burren, Oliver

AU - Capon, Francesca

AU - Compston, Alastair

AU - Gough, Stephen C. L.

AU - Jostins, Luke

AU - Kong, Yong

AU - Lee, James C.

AU - Lek, Monkol

AU - MacArthur, Daniel G.

AU - Mansfield, John C.

AU - Mathew, Christopher G.

AU - Mein, Charles A.

AU - Mirza, Muddassar

AU - Nutland, Sarah

AU - Onengut-Gumuscu, Suna

AU - Papouli, Efterpi

AU - Parkes, Miles

AU - Rich, Stephen S.

AU - Sawcer, Steven

AU - Satsangi, Jack

AU - Simmonds, Matthew J.

AU - Trembath, Richard C.

AU - Walker, Neil M.

AU - Wozniak, Eva

AU - Todd, John A.

AU - Simpson, Michael A.

AU - Plagnol, Vincent

AU - van Heel, David A.

PY - 2013/6/13

Y1 - 2013/6/13

N2 - Genome-wide association studies(GWAS) have identified common variants of modest-effect size at hundreds of loci for common autoimmune diseases; however, a substantial fraction of heritability remains unexplained, to which rare variants may contribute(1,2). To discover rare variants and test them for association with a phenotype, most studies re-sequence a small initial sample size and then genotype the discovered variants in a larger sample set(3-5). This approach fails to analyse a large fraction of the rare variants present in the entire sample set. Here we perform simultaneous amplicon-sequencing-based variant discovery and genotyping for coding exons of 25 GWAS risk genes in 41,911 UK residents of white European origin, comprising 24,892 subjects with six autoimmune disease phenotypes and 17,019 controls, and show that rare coding-region variants at known loci have a negligible role in common autoimmune disease susceptibility. These results do not support the rare-variant synthetic genome-wide-association hypothesis(6) (in which unobserved rare causal variants lead to association detected at common tag variants). Many known autoimmune disease risk loci contain multiple, independently associated, common and low-frequency variants, and so genes at these loci are a priori stronger candidates for harbouring rare coding-region variants than other genes. Our data indicate that the missing heritability for common autoimmune diseases may not be attributable to the rare coding-region variant portion of the allelic spectrum, but perhaps, as others have proposed, may be a result of many common-variant loci of weak effect(7-10).

AB - Genome-wide association studies(GWAS) have identified common variants of modest-effect size at hundreds of loci for common autoimmune diseases; however, a substantial fraction of heritability remains unexplained, to which rare variants may contribute(1,2). To discover rare variants and test them for association with a phenotype, most studies re-sequence a small initial sample size and then genotype the discovered variants in a larger sample set(3-5). This approach fails to analyse a large fraction of the rare variants present in the entire sample set. Here we perform simultaneous amplicon-sequencing-based variant discovery and genotyping for coding exons of 25 GWAS risk genes in 41,911 UK residents of white European origin, comprising 24,892 subjects with six autoimmune disease phenotypes and 17,019 controls, and show that rare coding-region variants at known loci have a negligible role in common autoimmune disease susceptibility. These results do not support the rare-variant synthetic genome-wide-association hypothesis(6) (in which unobserved rare causal variants lead to association detected at common tag variants). Many known autoimmune disease risk loci contain multiple, independently associated, common and low-frequency variants, and so genes at these loci are a priori stronger candidates for harbouring rare coding-region variants than other genes. Our data indicate that the missing heritability for common autoimmune diseases may not be attributable to the rare coding-region variant portion of the allelic spectrum, but perhaps, as others have proposed, may be a result of many common-variant loci of weak effect(7-10).

KW - INFLAMMATORY-BOWEL-DISEASE

KW - GENOME-WIDE ASSOCIATION

KW - PSORIASIS SUSCEPTIBILITY LOCI

KW - RHEUMATOID-ARTHRITIS

KW - COMMON VARIANTS

KW - LOW-FREQUENCY

KW - GENES

KW - RISK

KW - ARCHITECTURE

KW - REVEALS

U2 - 10.1038/nature12170

DO - 10.1038/nature12170

M3 - Letter

SN - 0028-0836

VL - 498

SP - 232

EP - 235

JO - NATURE

JF - NATURE

IS - 7453

ER -

Negligible impact of rare autoimmune-locus coding-region variants on missing heritability

Abstract

Keywords

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