Yogita Ghodke-Puranik1, Molly Imgruet2, Jessica M Dorschner2, Prakriti Shrestha2, Kaci McCoy2, Jennifer A Kelly3, Miranda Marion4, Joel M Guthridge3, Carl D Langefeld4, John B Harley5, Judith A James3, Kathy L Sivils3, Timothy B Niewold6. 1. Colton Center for Autoimmunity, New York University School of Medicine, New York, NY, USA. 2. Division of Rheumatology, Mayo Clinic, Rochester, MN, USA. 3. Arthritis & Clinical Immunology Program, Oklahoma Medical Research Foundation, Oklahoma City, OK, USA. 4. Department of Biostatistical Sciences, Wake Forest School of Medicine, Winston-Salem, NC, USA. 5. Cincinnati Children's Hospital Medical Center, University of Cincinnati College of Medicine and Cincinnati VA Medical Center, Cincinnati, OH, USA. 6. Colton Center for Autoimmunity, New York University School of Medicine, New York, NY, USA. Electronic address: Timothy.Niewold@nyulangone.org.
Abstract
BACKGROUND/ PURPOSE: High serum interferon alpha (IFN-α) is an important heritable phenotype in systemic lupus erythematosus (SLE) which is involved in primary disease pathogenesis. High vs. low levels of IFN-α are associated with disease severity and account for some of the biological heterogeneity between SLE patients. The aim of the study was to replicate and fine-map previously detected genetic associations with serum IFN-α in SLE. METHODS: We previously undertook a case-case genome-wide association study of SLE patients stratified by ancestry and extremes of phenotype in serum IFN-α. Single nucleotide polymorphisms (SNPs) in seven loci identified in this screen were selected for follow up in a large independent cohort of 1370 SLE patients (703 European-ancestry, 432 African ancestry, and 235 Amerindian ancestry). Each ancestral background was analyzed separately, and ancestry-informative markers were used to control for ancestry and admixture. RESULTS: We find a rare haplotype spanning the promoter region of EFNA5 that is strongly associated with serum IFN-α in both African-American and European-American SLE patients (OR = 3.0, p = 3.7 × 10-6). We also find SNPs in the PPM1H, PTPRM, and NRGN regions associated with IFN-α levels in European-American, Amerindian, and African-American SLE patients respectively. Many of these associations are within regulatory regions of the gene, suggesting an impact on transcription. CONCLUSION: This study demonstrates the power of molecular sub-phenotypes to reveal genetic factors involved in complex autoimmune disease. The distinct associations observed in different ancestral backgrounds emphasize the heterogeneity of molecular pathogenesis in SLE.
BACKGROUND/ PURPOSE: High serum interferon alpha (IFN-α) is an important heritable phenotype in systemic lupus erythematosus (SLE) which is involved in primary disease pathogenesis. High vs. low levels of IFN-α are associated with disease severity and account for some of the biological heterogeneity between SLEpatients. The aim of the study was to replicate and fine-map previously detected genetic associations with serum IFN-α in SLE. METHODS: We previously undertook a case-case genome-wide association study of SLEpatients stratified by ancestry and extremes of phenotype in serum IFN-α. Single nucleotide polymorphisms (SNPs) in seven loci identified in this screen were selected for follow up in a large independent cohort of 1370 SLEpatients (703 European-ancestry, 432 African ancestry, and 235 Amerindian ancestry). Each ancestral background was analyzed separately, and ancestry-informative markers were used to control for ancestry and admixture. RESULTS: We find a rare haplotype spanning the promoter region of EFNA5 that is strongly associated with serum IFN-α in both African-American and European-American SLEpatients (OR = 3.0, p = 3.7 × 10-6). We also find SNPs in the PPM1H, PTPRM, and NRGN regions associated with IFN-α levels in European-American, Amerindian, and African-American SLEpatients respectively. Many of these associations are within regulatory regions of the gene, suggesting an impact on transcription. CONCLUSION: This study demonstrates the power of molecular sub-phenotypes to reveal genetic factors involved in complex autoimmune disease. The distinct associations observed in different ancestral backgrounds emphasize the heterogeneity of molecular pathogenesis in SLE.
Authors: Corinna E Weckerle; Beverly S Franek; Jennifer A Kelly; Marissa Kumabe; Rachel A Mikolaitis; Stephanie L Green; Tammy O Utset; Meenakshi Jolly; Judith A James; John B Harley; Timothy B Niewold Journal: Arthritis Rheum Date: 2011-04
Authors: Timothy B Niewold; Jennifer A Kelly; Silvia N Kariuki; Beverly S Franek; Akaash A Kumar; Kenneth M Kaufman; Kenaz Thomas; Daniel Walker; Stan Kamp; Jacqueline M Frost; Andrew K Wong; Joan T Merrill; Marta E Alarcón-Riquelme; Mohammed Tikly; Rosalind Ramsey-Goldman; John D Reveille; Michelle A Petri; Jeffrey C Edberg; Robert P Kimberly; Graciela S Alarcón; Diane L Kamen; Gary S Gilkeson; Timothy J Vyse; Judith A James; Patrick M Gaffney; Kathy L Moser; Mary K Crow; John B Harley Journal: Ann Rheum Dis Date: 2011-11-16 Impact factor: 19.103
Authors: Isobel D Lawrenson; Sabine H Wimmer-Kleikamp; Peter Lock; Simone M Schoenwaelder; Michelle Down; Andrew W Boyd; Paul F Alewood; Martin Lackmann Journal: J Cell Sci Date: 2002-03-01 Impact factor: 5.285
Authors: S N Kariuki; Y Ghodke-Puranik; J M Dorschner; B S Chrabot; J A Kelly; B P Tsao; R P Kimberly; M E Alarcón-Riquelme; C O Jacob; L A Criswell; K L Sivils; C D Langefeld; J B Harley; A D Skol; T B Niewold Journal: Genes Immun Date: 2014-10-23 Impact factor: 2.676
Authors: Carl D Langefeld; Hannah C Ainsworth; Deborah S Cunninghame Graham; Jennifer A Kelly; Mary E Comeau; Miranda C Marion; Timothy D Howard; Paula S Ramos; Jennifer A Croker; David L Morris; Johanna K Sandling; Jonas Carlsson Almlöf; Eduardo M Acevedo-Vásquez; Graciela S Alarcón; Alejandra M Babini; Vicente Baca; Anders A Bengtsson; Guillermo A Berbotto; Marc Bijl; Elizabeth E Brown; Hermine I Brunner; Mario H Cardiel; Luis Catoggio; Ricard Cervera; Jorge M Cucho-Venegas; Solbritt Rantapää Dahlqvist; Sandra D'Alfonso; Berta Martins Da Silva; Iñigo de la Rúa Figueroa; Andrea Doria; Jeffrey C Edberg; Emőke Endreffy; Jorge A Esquivel-Valerio; Paul R Fortin; Barry I Freedman; Johan Frostegård; Mercedes A García; Ignacio García de la Torre; Gary S Gilkeson; Dafna D Gladman; Iva Gunnarsson; Joel M Guthridge; Jennifer L Huggins; Judith A James; Cees G M Kallenberg; Diane L Kamen; David R Karp; Kenneth M Kaufman; Leah C Kottyan; László Kovács; Helle Laustrup; Bernard R Lauwerys; Quan-Zhen Li; Marco A Maradiaga-Ceceña; Javier Martín; Joseph M McCune; David R McWilliams; Joan T Merrill; Pedro Miranda; José F Moctezuma; Swapan K Nath; Timothy B Niewold; Lorena Orozco; Norberto Ortego-Centeno; Michelle Petri; Christian A Pineau; Bernardo A Pons-Estel; Janet Pope; Prithvi Raj; Rosalind Ramsey-Goldman; John D Reveille; Laurie P Russell; José M Sabio; Carlos A Aguilar-Salinas; Hugo R Scherbarth; Raffaella Scorza; Michael F Seldin; Christopher Sjöwall; Elisabet Svenungsson; Susan D Thompson; Sergio M A Toloza; Lennart Truedsson; Teresa Tusié-Luna; Carlos Vasconcelos; Luis M Vilá; Daniel J Wallace; Michael H Weisman; Joan E Wither; Tushar Bhangale; Jorge R Oksenberg; John D Rioux; Peter K Gregersen; Ann-Christine Syvänen; Lars Rönnblom; Lindsey A Criswell; Chaim O Jacob; Kathy L Sivils; Betty P Tsao; Laura E Schanberg; Timothy W Behrens; Earl D Silverman; Marta E Alarcón-Riquelme; Robert P Kimberly; John B Harley; Edward K Wakeland; Robert R Graham; Patrick M Gaffney; Timothy J Vyse Journal: Nat Commun Date: 2017-07-17 Impact factor: 14.919