Fine-mapping and functional studies highlight potential causal variants for rheumatoid arthritis and type 1 diabetes

被引:0
|
作者
Harm-Jan Westra
Marta Martínez-Bonet
Suna Onengut-Gumuscu
Annette Lee
Yang Luo
Nikola Teslovich
Jane Worthington
Javier Martin
Tom Huizinga
Lars Klareskog
Solbritt Rantapaa-Dahlqvist
Wei-Min Chen
Aaron Quinlan
John A. Todd
Steve Eyre
Peter A. Nigrovic
Peter K. Gregersen
Stephen S. Rich
Soumya Raychaudhuri
机构
[1] Harvard Medical School,Center for Data Sciences, Brigham and Women’s Hospital
[2] Harvard Medical School,Division of Genetics, Brigham and Women’s Hospital
[3] Broad Institute of Harvard and MIT,Program in Medical and Population Genetics
[4] Harvard Medical School,Division of Rheumatology, Immunology, and Allergy, Brigham and Women’s Hospital
[5] University Medical Center Groningen,Department of Genetics, University of Groningen
[6] University of Virginia,Department of Public Health Sciences
[7] University of Virginia,Center for Public Health Genomics
[8] Northwell Health,The Feinstein Institute for Medical Research
[9] The University of Manchester,Arthritis Research UK Centre for Genetics and Genomics, Centre for Musculoskeletal Research, Manchester Academic Health Science Centre
[10] Manchester University NHS Foundation Trust,NIHR Manchester Biomedical Research Centre
[11] Consejo Superior de Investigaciones Científicas,Instituto de Parasitología y Biomedicina López
[12] Leiden University Medical Centre,Neyra
[13] Karolinska Institutet and Karolinska University Hospital,Department of Rheumatology
[14] Umeå University,Rheumatology Unit, Department of Medicine
[15] University of Utah,Department of Public Health and Clinical Medicine, Division of Rheumatology
[16] University of Utah,Department of Human Genetics
[17] University of Oxford,Department of Biomedical Informatics
[18] Boston Children’s Hospital,JDRF/Wellcome Diabetes and Inflammation Laboratory, Wellcome Centre for Human Genetics, Nuffield Department of Medicine
[19] Harvard Medical School,Division of Immunology
来源
Nature Genetics | 2018年 / 50卷
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摘要
To define potentially causal variants for autoimmune disease, we fine-mapped1,2 76 rheumatoid arthritis (11,475 cases, 15,870 controls)3 and type 1 diabetes loci (9,334 cases, 11,111 controls)4. After sequencing 799 1-kilobase regulatory (H3K4me3) regions within these loci in 568 individuals, we observed accurate imputation for 89% of common variants. We defined credible sets of ≤5 causal variants at 5 rheumatoid arthritis and 10 type 1 diabetes loci. We identified potentially causal missense variants at DNASE1L3, PTPN22, SH2B3, and TYK2, and noncoding variants at MEG3, CD28–CTLA4, and IL2RA. We also identified potential candidate causal variants at SIRPG and TNFAIP3. Using functional assays, we confirmed allele-specific protein binding and differential enhancer activity for three variants: the CD28–CTLA4 rs117701653 SNP, MEG3 rs34552516 indel, and TNFAIP3 rs35926684 indel.
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页码:1366 / 1374
页数:8
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