Immunochip analyses identify a novel risk locus for primary biliary cirrhosis at 13q14, multiple independent associations at four established risk loci and epistasis between 1p31 and 7q32 risk variants

Brian D Juran; Gideon M Hirschfield; Pietro Invernizzi; Elizabeth J Atkinson; Yafang Li; Gang Xie; Roman Kosoy; Michael Ransom; Ye Sun; Ilaria Bianchi; Erik M Schlicht; Ana Lleo; Catalina Coltescu; Francesca Bernuzzi; Mauro Podda; Craig Lammert; Russell Shigeta; Landon L Chan; Tobias Balschun; Maurizio Marconi; Daniele Cusi; E Jenny Heathcote; Andrew L Mason; Robert P Myers; Piotr Milkiewicz; Joseph A Odin; Velimir A Luketic; Bruce R Bacon; Henry C Bodenheimer; Valentina Liakina; Catherine Vincent; Cynthia Levy; Andre Franke; Peter K Gregersen; Fabrizio Bossa; M Eric Gershwin; Mariza deAndrade; Christopher I Amos; Konstantinos N Lazaridis; Michael F Seldin; Katherine A Siminovitch; Italian PBC Genetics Study Group

doi:10.1093/hmg/dds359

Immunochip analyses identify a novel risk locus for primary biliary cirrhosis at 13q14, multiple independent associations at four established risk loci and epistasis between 1p31 and 7q32 risk variants

Brian D Juran, Gideon M Hirschfield, Pietro Invernizzi, Elizabeth J Atkinson, Yafang Li, Gang Xie, Roman Kosoy, Michael Ransom, Ye Sun, Ilaria Bianchi, Erik M Schlicht, Ana Lleo, Catalina Coltescu, Francesca Bernuzzi, Mauro Podda, Craig Lammert, Russell Shigeta, Landon L Chan, Tobias Balschun, Maurizio MarconiDaniele Cusi, E Jenny Heathcote, Andrew L Mason, Robert P Myers, Piotr Milkiewicz, Joseph A Odin, Velimir A Luketic, Bruce R Bacon, Henry C Bodenheimer, Valentina Liakina, Catherine Vincent, Cynthia Levy, Andre Franke, Peter K Gregersen, Fabrizio Bossa, M Eric Gershwin, Mariza deAndrade, Christopher I Amos, Konstantinos N Lazaridis, Michael F Seldin, Katherine A Siminovitch, Italian PBC Genetics Study Group

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

104 Citations (Scopus)

Abstract

To further characterize the genetic basis of primary biliary cirrhosis (PBC), we genotyped 2426 PBC patients and 5731 unaffected controls from three independent cohorts using a single nucleotide polymorphism (SNP) array (Immunochip) enriched for autoimmune disease risk loci. Meta-analysis of the genotype data sets identified a novel disease-associated locus near the TNFSF11 gene at 13q14, provided evidence for association at six additional immune-related loci not previously implicated in PBC and confirmed associations at 19 of 22 established risk loci. Results of conditional analyses also provided evidence for multiple independent association signals at four risk loci, with haplotype analyses suggesting independent SNP effects at the 2q32 and 16p13 loci, but complex haplotype driven effects at the 3q25 and 6p21 loci. By imputing classical HLA alleles from this data set, four class II alleles independently contributing to the association signal from this region were identified. Imputation of genotypes at the non-HLA loci also provided additional associations, but none with stronger effects than the genotyped variants. An epistatic interaction between the IL12RB2 risk locus at 1p31and the IRF5 risk locus at 7q32 was also identified and suggests a complementary effect of these loci in predisposing to disease. These data expand the repertoire of genes with potential roles in PBC pathogenesis that need to be explored by follow-up biological studies.

Original language	English
Pages (from-to)	5209-21
Number of pages	13
Journal	Human Molecular Genetics
Volume	21
Issue number	23
DOIs	https://doi.org/10.1093/hmg/dds359
Publication status	Published - 1 Dec 2012

Keywords

Alleles
Case-Control Studies
Chromosomes, Human, Pair 1
Chromosomes, Human, Pair 13
Chromosomes, Human, Pair 7
Epistasis, Genetic
Gene Frequency
Genetic Loci
Genetic Predisposition to Disease
Genotype
HLA Antigens
Humans
Liver Cirrhosis, Biliary
Oligonucleotide Array Sequence Analysis
Polymorphism, Single Nucleotide

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1093/hmg/dds359

Cite this

Juran, B. D., Hirschfield, G. M., Invernizzi, P., Atkinson, E. J., Li, Y., Xie, G., Kosoy, R., Ransom, M., Sun, Y., Bianchi, I., Schlicht, E. M., Lleo, A., Coltescu, C., Bernuzzi, F., Podda, M., Lammert, C., Shigeta, R., Chan, L. L., Balschun, T., ... Italian PBC Genetics Study Group (2012). Immunochip analyses identify a novel risk locus for primary biliary cirrhosis at 13q14, multiple independent associations at four established risk loci and epistasis between 1p31 and 7q32 risk variants. Human Molecular Genetics, 21(23), 5209-21. https://doi.org/10.1093/hmg/dds359

@article{9430c93b5ad54984a2f0ec6983f9423b,

title = "Immunochip analyses identify a novel risk locus for primary biliary cirrhosis at 13q14, multiple independent associations at four established risk loci and epistasis between 1p31 and 7q32 risk variants",

abstract = "To further characterize the genetic basis of primary biliary cirrhosis (PBC), we genotyped 2426 PBC patients and 5731 unaffected controls from three independent cohorts using a single nucleotide polymorphism (SNP) array (Immunochip) enriched for autoimmune disease risk loci. Meta-analysis of the genotype data sets identified a novel disease-associated locus near the TNFSF11 gene at 13q14, provided evidence for association at six additional immune-related loci not previously implicated in PBC and confirmed associations at 19 of 22 established risk loci. Results of conditional analyses also provided evidence for multiple independent association signals at four risk loci, with haplotype analyses suggesting independent SNP effects at the 2q32 and 16p13 loci, but complex haplotype driven effects at the 3q25 and 6p21 loci. By imputing classical HLA alleles from this data set, four class II alleles independently contributing to the association signal from this region were identified. Imputation of genotypes at the non-HLA loci also provided additional associations, but none with stronger effects than the genotyped variants. An epistatic interaction between the IL12RB2 risk locus at 1p31and the IRF5 risk locus at 7q32 was also identified and suggests a complementary effect of these loci in predisposing to disease. These data expand the repertoire of genes with potential roles in PBC pathogenesis that need to be explored by follow-up biological studies.",

keywords = "Alleles, Case-Control Studies, Chromosomes, Human, Pair 1, Chromosomes, Human, Pair 13, Chromosomes, Human, Pair 7, Epistasis, Genetic, Gene Frequency, Genetic Loci, Genetic Predisposition to Disease, Genotype, HLA Antigens, Humans, Liver Cirrhosis, Biliary, Oligonucleotide Array Sequence Analysis, Polymorphism, Single Nucleotide",

author = "Juran, {Brian D} and Hirschfield, {Gideon M} and Pietro Invernizzi and Atkinson, {Elizabeth J} and Yafang Li and Gang Xie and Roman Kosoy and Michael Ransom and Ye Sun and Ilaria Bianchi and Schlicht, {Erik M} and Ana Lleo and Catalina Coltescu and Francesca Bernuzzi and Mauro Podda and Craig Lammert and Russell Shigeta and Chan, {Landon L} and Tobias Balschun and Maurizio Marconi and Daniele Cusi and Heathcote, {E Jenny} and Mason, {Andrew L} and Myers, {Robert P} and Piotr Milkiewicz and Odin, {Joseph A} and Luketic, {Velimir A} and Bacon, {Bruce R} and Bodenheimer, {Henry C} and Valentina Liakina and Catherine Vincent and Cynthia Levy and Andre Franke and Gregersen, {Peter K} and Fabrizio Bossa and Gershwin, {M Eric} and Mariza deAndrade and Amos, {Christopher I} and Lazaridis, {Konstantinos N} and Seldin, {Michael F} and Siminovitch, {Katherine A} and {Italian PBC Genetics Study Group}",

year = "2012",

month = dec,

day = "1",

doi = "10.1093/hmg/dds359",

language = "English",

volume = "21",

pages = "5209--21",

journal = "Human Molecular Genetics",

issn = "0964-6906",

publisher = "Oxford University Press",

number = "23",

}

Juran, BD, Hirschfield, GM, Invernizzi, P, Atkinson, EJ, Li, Y, Xie, G, Kosoy, R, Ransom, M, Sun, Y, Bianchi, I, Schlicht, EM, Lleo, A, Coltescu, C, Bernuzzi, F, Podda, M, Lammert, C, Shigeta, R, Chan, LL, Balschun, T, Marconi, M, Cusi, D, Heathcote, EJ, Mason, AL, Myers, RP, Milkiewicz, P, Odin, JA, Luketic, VA, Bacon, BR, Bodenheimer, HC, Liakina, V, Vincent, C, Levy, C, Franke, A, Gregersen, PK, Bossa, F, Gershwin, ME, deAndrade, M, Amos, CI, Lazaridis, KN, Seldin, MF, Siminovitch, KA & Italian PBC Genetics Study Group 2012, 'Immunochip analyses identify a novel risk locus for primary biliary cirrhosis at 13q14, multiple independent associations at four established risk loci and epistasis between 1p31 and 7q32 risk variants', Human Molecular Genetics, vol. 21, no. 23, pp. 5209-21. https://doi.org/10.1093/hmg/dds359

Immunochip analyses identify a novel risk locus for primary biliary cirrhosis at 13q14, multiple independent associations at four established risk loci and epistasis between 1p31 and 7q32 risk variants. / Juran, Brian D; Hirschfield, Gideon M; Invernizzi, Pietro et al.
In: Human Molecular Genetics, Vol. 21, No. 23, 01.12.2012, p. 5209-21.

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

TY - JOUR

T1 - Immunochip analyses identify a novel risk locus for primary biliary cirrhosis at 13q14, multiple independent associations at four established risk loci and epistasis between 1p31 and 7q32 risk variants

AU - Juran, Brian D

AU - Hirschfield, Gideon M

AU - Invernizzi, Pietro

AU - Atkinson, Elizabeth J

AU - Li, Yafang

AU - Xie, Gang

AU - Kosoy, Roman

AU - Ransom, Michael

AU - Sun, Ye

AU - Bianchi, Ilaria

AU - Schlicht, Erik M

AU - Lleo, Ana

AU - Coltescu, Catalina

AU - Bernuzzi, Francesca

AU - Podda, Mauro

AU - Lammert, Craig

AU - Shigeta, Russell

AU - Chan, Landon L

AU - Balschun, Tobias

AU - Marconi, Maurizio

AU - Cusi, Daniele

AU - Heathcote, E Jenny

AU - Mason, Andrew L

AU - Myers, Robert P

AU - Milkiewicz, Piotr

AU - Odin, Joseph A

AU - Luketic, Velimir A

AU - Bacon, Bruce R

AU - Bodenheimer, Henry C

AU - Liakina, Valentina

AU - Vincent, Catherine

AU - Levy, Cynthia

AU - Franke, Andre

AU - Gregersen, Peter K

AU - Bossa, Fabrizio

AU - Gershwin, M Eric

AU - deAndrade, Mariza

AU - Amos, Christopher I

AU - Lazaridis, Konstantinos N

AU - Seldin, Michael F

AU - Siminovitch, Katherine A

AU - Italian PBC Genetics Study Group

PY - 2012/12/1

Y1 - 2012/12/1

N2 - To further characterize the genetic basis of primary biliary cirrhosis (PBC), we genotyped 2426 PBC patients and 5731 unaffected controls from three independent cohorts using a single nucleotide polymorphism (SNP) array (Immunochip) enriched for autoimmune disease risk loci. Meta-analysis of the genotype data sets identified a novel disease-associated locus near the TNFSF11 gene at 13q14, provided evidence for association at six additional immune-related loci not previously implicated in PBC and confirmed associations at 19 of 22 established risk loci. Results of conditional analyses also provided evidence for multiple independent association signals at four risk loci, with haplotype analyses suggesting independent SNP effects at the 2q32 and 16p13 loci, but complex haplotype driven effects at the 3q25 and 6p21 loci. By imputing classical HLA alleles from this data set, four class II alleles independently contributing to the association signal from this region were identified. Imputation of genotypes at the non-HLA loci also provided additional associations, but none with stronger effects than the genotyped variants. An epistatic interaction between the IL12RB2 risk locus at 1p31and the IRF5 risk locus at 7q32 was also identified and suggests a complementary effect of these loci in predisposing to disease. These data expand the repertoire of genes with potential roles in PBC pathogenesis that need to be explored by follow-up biological studies.

AB - To further characterize the genetic basis of primary biliary cirrhosis (PBC), we genotyped 2426 PBC patients and 5731 unaffected controls from three independent cohorts using a single nucleotide polymorphism (SNP) array (Immunochip) enriched for autoimmune disease risk loci. Meta-analysis of the genotype data sets identified a novel disease-associated locus near the TNFSF11 gene at 13q14, provided evidence for association at six additional immune-related loci not previously implicated in PBC and confirmed associations at 19 of 22 established risk loci. Results of conditional analyses also provided evidence for multiple independent association signals at four risk loci, with haplotype analyses suggesting independent SNP effects at the 2q32 and 16p13 loci, but complex haplotype driven effects at the 3q25 and 6p21 loci. By imputing classical HLA alleles from this data set, four class II alleles independently contributing to the association signal from this region were identified. Imputation of genotypes at the non-HLA loci also provided additional associations, but none with stronger effects than the genotyped variants. An epistatic interaction between the IL12RB2 risk locus at 1p31and the IRF5 risk locus at 7q32 was also identified and suggests a complementary effect of these loci in predisposing to disease. These data expand the repertoire of genes with potential roles in PBC pathogenesis that need to be explored by follow-up biological studies.

KW - Alleles

KW - Case-Control Studies

KW - Chromosomes, Human, Pair 1

KW - Chromosomes, Human, Pair 13

KW - Chromosomes, Human, Pair 7

KW - Epistasis, Genetic

KW - Gene Frequency

KW - Genetic Loci

KW - Genetic Predisposition to Disease

KW - Genotype

KW - HLA Antigens

KW - Humans

KW - Liver Cirrhosis, Biliary

KW - Oligonucleotide Array Sequence Analysis

KW - Polymorphism, Single Nucleotide

UR - http://hmg.oxfordjournals.org/content/21/23/5209.long

U2 - 10.1093/hmg/dds359

DO - 10.1093/hmg/dds359

M3 - Article

C2 - 22936693

SN - 0964-6906

VL - 21

SP - 5209

EP - 5221

JO - Human Molecular Genetics

JF - Human Molecular Genetics

IS - 23

ER -

Immunochip analyses identify a novel risk locus for primary biliary cirrhosis at 13q14, multiple independent associations at four established risk loci and epistasis between 1p31 and 7q32 risk variants

Abstract

Keywords

UN SDGs

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