Genome-wide association studies identify IL23R-IL12RB2 and IL10 as Behçet's disease susceptibility loci

Mizuki, Nobuhisa; Meguro, Akira; Ôta, Masao; Ohno, Shigeaki; Shiota, Tomoko; Kawagoe, Tatsukata; Ito, Norihiko; Kera, Jiro; Okada, Eiichi; Yatsu, Keisuke; Song, Yeong Wook; Kitaichi, Nobuyoshi; Namba, Kenichi; Horie, Yukihiro; Takeno, Mitsuhiro; Sugita, Sunao; Mochizuki, Manabu; Bahram, Seiamak; Ishigatsubo, Yoshiaki; Inoko, Hidetoshi

doi:10.1038/ng.624

Cited by 470 publications

(379 citation statements)

References 19 publications

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“…This has already generated tangible benefits, and in BD a recent genome-wide association study (GWAS) has not only confirmed the association with know HLA-B*51 but identified further associations within MHC class I and also an association at IL-10 and IL23R-IL12RB2 loci. 96,97 This is concordant with other smaller candidate single nucleotide polymorphism (SNP) analysis studies that show in sympathetic ophthalmia an association with IL-10-1082 SNP and three haplotype-tagging SNPs(htSNPs) in the IL10 gene, rs6703630, rs2222202, and rs3024490, are significantly associated with susceptibility to non-infectious uveitis, whereas a LTA þ 252AA/ TNFhtSNP2GG haplotype (rs909253 and rs361525) is protective. 98,99 Whether this will predict the outcome on an individual basis is unknown, 100 but it highlights how further GWAS and, more importantly, genomics, RNA sequencing, and transcriptomics, will shape our future approach by identifying new genes, potential biomarkers, and new targets for therapy.…”

Section: How Do We Harness Our Approaches?supporting

confidence: 76%

Current concepts and future directions in the pathogenesis and treatment of non-infectious intraocular inflammation

Lee

Dick

2011

Eye

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The blockbuster drug paradigm is under increasing scrutiny across the biopharmaceutical industry. Intraocular inflammation poses particular challenges to this, given the heterogeneity of conditions in the uveitis spectrum, and the increasing acknowledgement of individual patient and disease variance in underlying immune responses. This need has triggered a drive towards personalised and stratified medicine, supported and enabled as a result of continued development of both experimental models and molecular biological techniques and improved clinical classification. As such we have the ability now to systematically appraise at a genomic, transcriptomic, and proteomic level individual immunophenotype, and the promise that in the eye this can be augmented by in vivo immune imaging to identify individual immunopathology. With such advances all running in parallel, we are entering an era of experimental medicine that will facilitate early diagnosis, generate biomarkers for accurate prognostication, and enable the development of individualised and targeted therapies, which can progress rapidly into clinical practice.

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Section: How Do We Harness Our Approaches?supporting

confidence: 76%

Current concepts and future directions in the pathogenesis and treatment of non-infectious intraocular inflammation

Lee

Dick

2011

Eye

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“…By comparison, B*52/MICA*009 was found in 25% of controls (8). Recently genome-wide association studies (GWASs) in different patient populations showed specific genes linked to BD in different ethnic groups; however, all the studies identified the HLA-B loci as the strongest association (9)(10)(11). However, in a recent study, deep sequencing of the HLA region identified an SNP, rs116799036, close to MICA that gave the strongest association and was independent of HLA-B*51 (12).…”

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confidence: 99%

HLA-B51* the primary risk in Behçet disease

Wallace

2014

Proc. Natl. Acad. Sci. U.S.A.

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“…However, efforts to parse the effects of MICA and HLA-B alleles definitively have been confounded by their particularly strong LD (11)(12)(13)(14). Additionally, HLA-A has been identified as a BD susceptibility locus in numerous studies (2,3,(14)(15)(16)(17), and it has been suggested that HLA-C contributes to BD risk, as well (14).…”

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confidence: 99%

“…The predominant BD susceptibility locus is the MHC on chromosome 6 (2, 3), which contains the strongest known risk factor for BD, the MHC class I (MHC-I) allele HLA-B*51 (2)(3)(4)(5). Several recent studies have expanded the list of genes or loci implicated in the pathophysiology of BD, which now includes HLA-B, IL10, IL23R, HLA-A, CCR1, STAT4, endoplasmic reticulum amino peptidase 1 (ERAP1), the killer lectinlike receptor cluster on chromosome 12, and, most recently, TLR4 and MEFV (2,3,6,7). Although these genetic studies of BD have provided new clues and insights into the pathogenesis of BD, none has provided a thorough accounting of the individual risk factors within the MHC.…”

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confidence: 99%

Behçet disease-associated MHC class I residues implicate antigen binding and regulation of cell-mediated cytotoxicity

Ombrello

Kirino

Bakker

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

121

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The HLA protein, HLA-B*51, encoded by HLA-B in MHC, is the strongest known genetic risk factor for Behçet disease (BD). Associations between BD and other factors within the MHC have been reported also, although strong regional linkage disequilibrium complicates their confident disentanglement from HLA-B*51. In the current study, we examined a combination of directly obtained and imputed MHC-region SNPs, directly obtained HLA-B locus types, and imputed classical HLA types with their corresponding polymorphic amino acid residues for association with BD in 1,190 cases and 1,257 controls. SNP mapping with logistic regression of the MHC identified the HLA-B/MICA region and the region between HLA-F and HLA-A as independently associated with BD (P < 1.7 × 10 −8 ). HLA-B*51, -A*03, -B*15, -B*27, -B*49, -B*57, and -A*26 each contributed independently to BD risk. We directly examined rs116799036, a noncoding SNP upstream of HLA-B that was recently suggested to underlie the association of HLA-B*51 with BD, but we were unable to replicate that finding in our collection. Instead, we mapped the BD association to seven MHC class I (MHC-I) amino acid residues, including anchor residues that critically define the selection and binding of peptides to MHC-I molecules, residues known to influence MHC-Ikiller immunoglobulin-like receptor interactions, and a residue located in the signal peptide of HLA-B. The locations of these variants collectively implicate MHC-I peptide binding in the pathophysiology of BD. Furthermore, several lines of evidence suggest a role for altered regulation of cellular cytotoxicity in BD pathogenesis.HLA imputation | autoinflammation | antigen presentation | killer immunoglobulin-like receptors | natural killer cells

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Genome-wide association studies identify IL23R-IL12RB2 and IL10 as Behçet's disease susceptibility loci

Cited by 470 publications

References 19 publications

Current concepts and future directions in the pathogenesis and treatment of non-infectious intraocular inflammation

Current concepts and future directions in the pathogenesis and treatment of non-infectious intraocular inflammation

HLA-B51* the primary risk in Behçet disease

Behçet disease-associated MHC class I residues implicate antigen binding and regulation of cell-mediated cytotoxicity

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Genome-wide association studies identify IL23R-IL12RB2 and IL10 as Behçet's disease susceptibility loci

Cited by 470 publications

References 19 publications

Current concepts and future directions in the pathogenesis and treatment of non-infectious intraocular inflammation

Current concepts and future directions in the pathogenesis and treatment of non-infectious intraocular inflammation

HLA-B*51 the primary risk in Behçet disease

Behçet disease-associated MHC class I residues implicate antigen binding and regulation of cell-mediated cytotoxicity

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HLA-B51* the primary risk in Behçet disease