Your search keyword '"Kenneth M. Kaufman"' showing total 100 results

1. Validation of low‐coverage whole‐genome sequencing for mitochondrial DNA variants suggests mitochondrial DNA as a genetic cause of preterm birth

Author

Kenneth M. Kaufman, Jesse Slone, Yongbo Huang, Louis J. Muglia, Michael W. Pauciulo, Taosheng Huang, Xinjian Wang, Iouri Chepelev, Jack Zhan, Bahram Namjou, John B. Harley, and Zeyu Yang

Subjects

Genetics, Whole genome sequencing, Mitochondrial DNA, Whole Genome Sequencing, Mitochondrial disease, Infant, Newborn, Infant, Gestational age, Biology, medicine.disease, DNA, Mitochondrial, Haplogroup, Human genetics, Heteroplasmy, Mitochondria, Genome, Mitochondrial, Cohort, medicine, Humans, Premature Birth, Genetics (clinical)

Abstract

Preterm birth (PTB), or birth that occurs earlier than 37 weeks of gestational age, is a major contributor to infant mortality and neonatal hospitalization. Mutations in the mitochondrial genome (mtDNA) have been linked to various rare mitochondrial disorders, and may be a contributing factor in PTB given that maternal genetic factors have been strongly linked to PTB. However, to date, no study has found a conclusive connection between a particular mtDNA variant and PTB. Given the high mtDNA copy number per cell, an automated pipeline was developed for detecting mtDNA variants using low-pass whole genome sequencing (lcWGS) data. The pipeline was first validated against samples of known heteroplasmy, and then applied to 929 samples from a PTB cohort from diverse ethnic backgrounds with an average gestational age of 27.18 weeks (range: 21-30). Our new pipeline successfully identified haplogroups and a large number of mtDNA variants in this large PTB cohort, including 8 samples carrying known pathogenic variants and 47 samples carrying rare mtDNA variants. These results confirm that lcWGS can be utilized to reliably identify mtDNA variants. These mtDNA variants may make a contribution toward preterm birth in a small proportion of live births. This article is protected by copyright. All rights reserved.

Published

2021

2. Pleiotropy in the Genetic Predisposition to Rheumatoid Arthritis: A Phenome‐Wide Association Study and Inverse Variance–Weighted Meta‐Analysis

Author

Dan M. Roden, Cecilia P. Chung, Scott J. Hebbring, Mingjian Shi, Nancy J. Cox, Jonathan D. Mosley, Gail P. Jarvik, Eric B. Larson, Ge Liu, Ming T M Lee, C. Michael Stein, eMERGE Investigators, Kenneth M. Kaufman, Vivian K. Kawai, Bahram Namjou, John B. Harley, QiPing Feng, and Adam S. Gordon

Subjects

Oncology, medicine.medical_specialty, Multiple Sclerosis, Statistics as Topic, Immunology, Hyperlipidemias, Article, Autoimmune Diseases, Arthritis, Rheumatoid, PTPN22, Rheumatology, Pleiotropy, Internal medicine, medicine, Genetic predisposition, Genetic Pleiotropy, Humans, Immunology and Allergy, Genetic Predisposition to Disease, Obesity, Renal Insufficiency, Chronic, Metabolic Syndrome, Type 1 diabetes, Scleroderma, Systemic, business.industry, Thyroiditis, Autoimmune, Mendelian Randomization Analysis, Odds ratio, medicine.disease, Diabetes Mellitus, Type 1, Phenotype, Diabetes Mellitus, Type 2, Cardiovascular Diseases, Meta-analysis, business

Abstract

Objective This study was undertaken to investigate the hypothesis that a genetic predisposition toward rheumatoid arthritis (RA) increases the risk of 10 cardiometabolic and autoimmune disorders previously associated with RA in epidemiologic studies, and to define new genetic pleiotropy present in RA. Methods Two approaches were used to test our hypothesis. First, we constructed a weighted genetic risk score (wGRS) and then examined its association with 10 prespecified disorders. Additionally, a phenome-wide association study (PheWAS) was carried out to identify potential new associations. Second, inverse variance-weighted regression (IVWR) meta-analysis was used to characterize the association between genetic susceptibility to RA and the prespecified disorders, with the results expressed as odds ratios (ORs) and 95% confidence intervals (95% CIs). Results The wGRS for RA was significantly associated with type 1 diabetes mellitus (DM) (OR 1.10 [95% CI 1.04-1.16]; P = 9.82 × 10-4 ) and multiple sclerosis (OR 0.82 [95% CI 0.77-0.88]; P = 1.73 × 10-8 ), but not with other cardiometabolic phenotypes. In the PheWAS, wGRS was also associated with an increased risk of several autoimmune phenotypes including RA, thyroiditis, and systemic sclerosis, and with a decreased risk of demyelinating disorders. In the IVWR meta-analyses, RA was significantly associated with an increased risk of type 1 DM (P = 1.15 × 10-14 ), with evidence of horizontal pleiotropy (Mendelian Randomization-Egger intercept estimate P = 0.001) likely driven by rs2476601, a PTPN22 variant. The association between type 1 DM and RA remained significant (P = 9.53 × 10-9 ) after excluding rs2476601, with no evidence of horizontal pleiotropy (intercept estimate P = 0.939). RA was also significantly associated with type 2 DM and C-reactive protein levels. These associations were driven by variation in the major histocompatibility complex region. Conclusion This study presents evidence of pleiotropy between the genetic predisposition to RA and associated phenotypes found in other autoimmune and cardiometabolic disorders, including type 1 DM.

Published

2020

3. Desmoplakin and periplakin genetically and functionally contribute to eosinophilic esophagitis

Author

Vincent A. Mukkada, Marc E. Rothenberg, J. Pablo Abonia, Pathre Purnima, Nives Zimmermann, Garrett A. Osswald, Kenneth M. Kaufman, Heather Foote, Philip E. Putnam, Michael D. Eby, Jeff E. Habel, Lisa J. Martin, Tetsuo Shoda, Kira Rehn, Wenying Zhang, Adina Y. Ballaban, Leah C. Kottyan, Margaret H. Collins, Netali Ben-Baruch Morgenstern, Julie M. Caldwell, and Ting Wen

Subjects

Male, Heterozygote, medicine.medical_specialty, Esophageal Mucosa, Adolescent, Biopsy, Science, DNA Mutational Analysis, Mutation, Missense, General Physics and Astronomy, Disease, Article, General Biochemistry, Genetics and Molecular Biology, Genetic etiology, Exome Sequencing, medicine, HaCaT Cells, Humans, Missense mutation, RNA-Seq, Child, Eosinophilic esophagitis, Gene, Periplakin, Multidisciplinary, biology, Calpain, Desmoplakin, business.industry, Plakins, Medical genetics, Desmosomes, Eosinophilic Esophagitis, General Chemistry, medicine.disease, HEK293 Cells, Desmoplakins, Case-Control Studies, Proteolysis, Immunology, biology.protein, Female, Oesophagitis, Single-Cell Analysis, business

Abstract

Eosinophilic esophagitis (EoE) is a chronic allergic inflammatory disease with a complex underlying genetic etiology. Herein, we conduct whole-exome sequencing of a multigeneration EoE pedigree (discovery set) and 61 additional multiplex families with EoE (replication set). A series of rare, heterozygous, missense variants are identified in the genes encoding the desmosome-associated proteins DSP and PPL in 21% of the multiplex families. Esophageal biopsies from patients with these variants retain dilated intercellular spaces and decrease DSP and PPL expression even during disease remission. These variants affect barrier integrity, cell motility and RhoGTPase activity in esophageal epithelial cells and have increased susceptibility to calpain-14–mediated degradation. An acquired loss of esophageal DSP and PPL is present in non-familial EoE. Taken together, herein, we uncover a pathogenic role for desmosomal dysfunction in EoE, providing a deeper mechanistic understanding of tissue-specific allergic responses., Eosinophilic esophagitis (EoE) is a chronic allergic inflammatory disease with a complex underlying genetic etiology. Here, the authors identify a series of rare variants in DSP and PPL in multiplex families with EoE and uncover a pathogenic role for desmosomal dysfunction in EoE.

Published

2021

4. 1706 A model of lupus pathogenesis: anti-EBNA1 heteroantibodies initiate lupus by cross reacting with lupus autoantigens, resulting in lupus autoantibodies and clinical disease

Author

Matthew T. Weirauch, Kenneth M. Kaufman, Viktoryia Laurynenka, John B. Harley, Leah C. Kottyan, Lili Ding, and Judith A. James

Subjects

Pathogenesis, Systemic lupus erythematosus, business.industry, Immunology, Autoantibody, Medicine, Heteroantibodies, business, medicine.disease, Clinical disease

Published

2021

5. 1502 Genetic predisposition to lupus across ancestries has >300 separable genetic contributions: what we know today

Author

Leah C. Kottyan, John B. Harley, Kenneth M. Kaufman, Viktoryia Laurynenka, and Matthew T. Weirauch

Subjects

Genetics, Systemic lupus erythematosus, Genetic predisposition, medicine, Immunologic diseases. Allergy, RC581-607, Biology, medicine.disease

Published

2021

6. Complete Tracheal Ring Deformity. A Translational Genomics Approach to Pathogenesis

Author

Alessandro de Alarcon, Ravindhra G. Elluru, John B. Harley, Daniela Zgherea, Debora Sinner, Bruce C. Trapnell, Michael J. Rutter, Jeffrey A. Whitsett, Kenneth M. Kaufman, Brenna Carey, Lauren Leesman, and Robert E. Wood

Subjects

Pulmonary and Respiratory Medicine, Pathology, medicine.medical_specialty, business.industry, Cartilage, Wnt signaling pathway, respiratory system, Critical Care and Intensive Care Medicine, medicine.disease, Hedgehog signaling pathway, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, 030228 respiratory system, Tracheomalacia, Trachealis muscle, Deformity, Medicine, 030212 general & internal medicine, medicine.symptom, business, Exome sequencing

Abstract

Rationale: Complete tracheal ring deformity (CTRD) is a rare congenital abnormality of unknown etiology characterized by circumferentially continuous or nearly-continuous cartilaginous tracheal rin...

Published

2019

7. A large-scale multi-ethnic genome-wide association study of coronary artery disease

Author

Joshua C. Bis, Kari E. North, Christopher A. Haiman, Mariaelisa Graff, Charles Kooperberg, Steven Buyske, Loic Le Marchand, Saiju Pyarajan, Yingchang Lu, Huaying Fang, Yuk-Lam Ho, Ian B. Stanaway, Shefali S. Verma, Kyung Min Lee, Peter W.F. Wilson, Shining Ma, Yan V. Sun, Ozan Dikilitas, Stephen Waldo, Daniel J. Rader, Hampton L. Leonard, Sekar Kathiresan, Christopher P. O'Donnell, Fei Chen, Kaoru Ito, Xiang Zhu, Elizabeth R. Hauser, Kyong-Mi Chang, Gail P. Jarvik, Botong Shen, Luca A. Lotta, Peter D. Reaven, Rachel L. Kember, Danish Saleheen, Genevieve L. Wojcik, Yoichiro Kamatani, Jeffrey Haessler, Sridharan Raghavan, Kumardeep Chaudhary, Kenneth M. Kaufman, Marijana Vujkovic, Jennifer Lee, Scott M. Damrauer, Kazuyoshi Ishigaki, Jie Huang, Austin T. Hilliard, Ron Do, Shoa L. Clarke, Noah Tsao, Derek Klarin, Kelly Cho, Jennifer E. Huffman, Donald R. Miller, J. Michael Gaziano, Bahram Namjou, Satoshi Koyama, Leslie A. Lange, Alexander G. Bick, Valerio Napolioni, Bryan R Gorman, Pradeep Natarajan, Scott J. Hebbring, Lynne R. Wilkens, Ruth J. F. Loos, P.S. Tsao, Benjamin F. Voight, Catherine Tcheandjieu, Mary Plomondon, Aris Baras, Hua Tang, Themistocles L. Assimes, Adam S. Gordon, Marylyn D. Ritchie, Ayush Giri, Michael G. Levin, Nasa Sinnott-Armstrong, Rebecca J Song, Christy L. Avery, Thomas Maddox, Marie Verbanck, Iftikhar J. Kullo, and Julie Lynch

Subjects

Coronary artery disease, Scale (ratio), business.industry, Ethnic group, Medicine, Genome-wide association study, Computational biology, business, medicine.disease

Abstract

Coronary artery disease (CAD) is a leading cause of death, yet its genetic determinants are not fully elucidated. We report a multi-ethnic genome-wide association study of CAD involving nearly a quarter of a million cases, incorporating the largest cohorts to date of Whites, Blacks, and Hispanics from the Million Veteran Program with existing studies including CARDIoGRAMplusC4D, UK Biobank, and Biobank Japan. We verify substantial and nearly equivalent heritability of CAD across multiple ancestral groups, discover 107 novel loci including the first nine on the X-chromosome, identify the first eight genome-wide significant loci among Blacks and Hispanics, and demonstrate that two common haplotypes are largely responsible for the risk stratification at the well-known 9p21 locus in most populations except those of African origin where both haplotypes are virtually absent. We identify 15 loci for angiographically derived burden of coronary atherosclerosis, which robustly overlap with the strongest and earliest loci reported to date for clinical CAD. Phenome-wide association analyses of novel loci and externally validated polygenic risk scores (PRS) augment signals from the insulin resistance cluster of risk factors and consequences, extend previously established pleiotropic associations of loci with traditional risk factors to include smoking and family history, and confirm a substantially reduced transferability of existing PRS to Blacks. Downstream integrative genomic analyses reinforce the critical role of endothelial, fibroblast, and smooth muscle cells within the coronary vessel wall in CAD susceptibility. Our study highlights the value of a multi-ethnic design in efficiently characterizing the genetic architecture of CAD across all human populations.

Published

2021

8. Transcription factors operate across disease loci, with EBNA2 implicated in autoimmunity

Author

Carmy Forney, Matthew T. Weirauch, Masashi Yukawa, Daniel Miller, Xiaoting Chen, John B. Harley, Kashish Chetal, Albert F. Magnusen, Artem Barski, Leah C. Kottyan, Nathan Salomonis, Mario Pujato, Kenneth M. Kaufman, Arthur Lynch, and Avery Maddox

Subjects

0301 basic medicine, Regulation of gene expression, Genetics, Epstein-Barr Virus Infections, Herpesvirus 4, Human, Lupus erythematosus, Autoimmunity, Disease, Biology, medicine.disease_cause, medicine.disease, Article, Human genetics, 3. Good health, Androgen receptor, 03 medical and health sciences, 030104 developmental biology, medicine, Humans, Gene-Environment Interaction, Functional genomics, Transcription factor, Transcription Factors

Abstract

Explaining the genetics of many diseases is challenging because most associations localize to incompletely characterized regulatory regions. Using new computational methods, we show that transcription factors (TFs) occupy multiple loci associated with individual complex genetic disorders. Application to 213 phenotypes and 1,544 TF binding datasets identified 2,264 relationships between hundreds of TFs and 94 phenotypes, including androgen receptor in prostate cancer and GATA3 in breast cancer. Strikingly, nearly half of systemic lupus erythematosus risk loci are occupied by the Epstein–Barr virus EBNA2 protein and many coclustering human TFs, showing gene–environment interaction. Similar EBNA2-anchored associations exist in multiple sclerosis, rheumatoid arthritis, inflammatory bowel disease, type 1 diabetes, juvenile idiopathic arthritis and celiac disease. Instances of allele-dependent DNA binding and downstream effects on gene expression at plausibly causal variants support genetic mechanisms dependent on EBNA2. Our results nominate mechanisms that operate across risk loci within disease phenotypes, suggesting new models for disease origins.

Published

2018

9. Copb2 is essential for embryogenesis and hypomorphic mutations cause human microcephaly

Author

Kristen L. Sund, Kenneth M. Kaufman, Elizabeth K. Schorry, Cynthia A. Prows, Andrew DiStasio, Biplab Dasgupta, Beth M. Kline-Fath, Ashley M. Driver, Milene Donlin, Ranjith M. Muraleedharan, Rolf W. Stottmann, and Shabnam Pooya

Subjects

Male, 0301 basic medicine, Heterozygote, Microcephaly, WD40 Repeats, Embryonic Development, Biology, medicine.disease_cause, Coatomer Protein, Mice, 03 medical and health sciences, 0302 clinical medicine, Gene Frequency, Intellectual Disability, Exome Sequencing, Genetics, medicine, Animals, Humans, Allele, Child, Molecular Biology, Genetics (clinical), Exome sequencing, 030304 developmental biology, 0303 health sciences, Mutation, Homozygote, Articles, General Medicine, medicine.disease, Null allele, COPB2, Phenotype, Pedigree, Disease Models, Animal, Corticogenesis, 030104 developmental biology, Female, 030217 neurology & neurosurgery

Abstract

Primary microcephaly is a congenital brain malformation characterized by a head circumference less than three standard deviations below the mean for age and sex and results in moderate to severe mental deficiencies and decreased lifespan. We recently studied two children with primary microcephaly in an otherwise unaffected family. Exome sequencing identified an autosomal recessive mutation leading to an amino acid substitution in a WD40 domain of the highly conserved Coatomer Protein Complex, Subunit Beta 2 (COPB2). To study the role of Copb2 in neural development, we utilized genome editing technology to generate an allelic series in the mouse. Two independent null alleles revealed that Copb2 is essential for early stages of embryogenesis. Mice homozygous for the patient variant (Copb2R254C/R254C) appear to have a grossly normal phenotype, likely due to differences in corticogenesis between the two species. Strikingly, mice heterozygous for the patient mutation and a null allele (Copb2R254C/Znf) show a severe perinatal phenotype including low neonatal weight, significantly increased apoptosis in the brain, and death within the first week of life. Immunostaining of the Copb2R254C/Znf brain revealed a reduction in layer V (CTIP2+) neurons, while the overall cell density of the cortex is unchanged. Moreover, disruption of Copb2 in mouse neurospheres resulted in reduced proliferation. These results identify a general requirement for COPB2 in embryogenesis and a specific role in corticogenesis. We further demonstrate the utility of CRISPR-Cas9 generated mouse models in the study of potential pathogenicity of variants of potential clinical interest.

Published

2017

10. P136 EPSTEIN-BARR VIRUS TRANSCRIPTION CO-FACTORS BIND TO MANY INFLAMMATORY BOWEL DISEASE RISK LOCI

Author

Xiaoting Chen, Shruti Eswar, John B. Harley, Matthew T. Weirauch, Sreeja Parameswaran, Leah C. Kottyan, Kenneth M. Kaufman, Martha Carter, Bahram Namjou, Batool Emadi, and Viktoryia Laurynenka

Subjects

Linkage disequilibrium, Hepatology, biology, Gastroenterology, medicine.disease, medicine.disease_cause, Virology, Epstein–Barr virus, Inflammatory bowel disease, Transcription (biology), medicine, biology.protein, Immunology and Allergy, Antibody, Candidate Disease Gene, Epstein–Barr virus infection, Transcription factor

Abstract

Objective IBD is a chronic inflammatory disorder of the GI tract with complex etiology that involves both genetic variants and environmental factors. Several viruses and bacteria have been suggested as potential causes of the disease. The clinical course of IBD appears to be influenced by EBV tissue infection. With a prevalence of >90% in the adult human population, EBV infection is nearly ubiquitous. We reported that the EBV transcription co-factor EBNA2 was concentrated in the risk loci of IBD relative to the remainder of the genome (Pc=1.24E-13, (RR) = 3.33, Nature Genetics 50:699, 2018). The objective of this study was to determine whether new data and studies made available since the data used for our 2018 study further supported the possibility that EBV was related to some IBD as a potential etiologic agent. Methods Genomic approaches offer previously unavailable perspectives for understanding disease mechanisms. The previous analysis was based upon the 9 viral transcription factor and co-factor (TF) datasets available in human cells in 2015.Of the 52 now available there are 29 from EBV. The number of established IBD loci qualifying for analysis has expanded from 112 in 2015 to 324 available now. We applied simulation analysis to assess statistical significance of TF associations with IBD risk loci using RELI (Regulatory Element Locus Intersection) (Nat Genet 50:699, 2018). RELI tests the probability of the observed association by the count of intersections of the same variant from two sources. We extracted 700 SNPs in European ancestry from 93 published GWAS and 350 additional candidate gene studies for IBD. All variants with linkage disequilibrium r2>0.8 of the best variant were included, while loci with r2>0.2 with a more highly significant locus were excluded. Results Among the 52 viral TF datasets, 139 of the 324 IBD loci were occupied by EBNALP (RR=2.08793, Pc=3.7321E-23), 113 by EBNA3C (RR=2.35113, Pc=2.84678E-22), 88 loci by EBNA2 (RR=3.2, Pc=7.8E-32) and 28 loci by EBNA3ABC, which used an antibody that did not distinguish between EBNA3 subtypes. Analysis of 11,535 human TF ChIP-seq datasets produced 1578 with strong associations (p The locus intersections of the three EBV gene products optimally clustered at 150 IBD loci (46%) with a set of 26 human TFs (p The human TFs were enriched for (ChIP-seq) data obtained from EBV-infected B lymphocyte cell line (OR = 10.12425329, Chi-squared = 241.2925605) Moreover, the human TFs that participate in the super-enhancers that form in the latency III EBV infected and transformed B cell are also concentrated among the statistically significant associations (p Conclusion These preliminary findings nominate EBV for a role in the pathogenesis and etiology of IBD by mechanisms operating in transformed B cells through the latency III EBV program of viral gene expression.

Published

2020

11. Genetic architecture distinguishes systemic juvenile idiopathic arthritis from other forms of juvenile idiopathic arthritis: clinical and therapeutic implications

Author

Elaine F. Remmers, Alberto Martini, Seza Ozen, Leah C. Kottyan, Eleftheria Zeggini, Anne Hinks, Wendy Thomson, Michael J. Ombrello, Sara Signa, Elisa Docampo, Ioanna Tachmazidou, Patricia Woo, Jordi Anton, Maria Odete Esteves Hilário, Rosenberg Am, Stephen W. Scherer, Susan D. Thompson, John F. Bohnsack, Erkan Demirkaya, Alexei A. Grom, Elizabeth Baskin, Dalila Pinto, Norman T. Ilowite, Kenneth M. Kaufman, Xavier Estivill, M. Ilyas Kamboh, Claudio Arnaldo Len, Kirsten Minden, Ricardo Russo, Emily Shuldiner, J Cobb, Carl D. Langefeld, Dirk Foell, Klaus Tenbrock, Marco Gattorno, Jean-Paul Achkar, Elizabeth D. Mellins, Johannes-Peter Haas, Rae S. M. Yeung, Ahmet Gül, Richard H. Duerr, Lucy R. Wedderburn, Sampath Prahalad, Angela Rösen-Wolff, Andrew Zeft, Arthur Vl, Daniel L. Kastner, Sheila Knupp Feitosa de Oliveira, Marta E. Alarcón-Riquelme, Universitat de Barcelona, and Çocuk Sağlığı ve Hastalıkları

Subjects

0301 basic medicine, genetic structures, Childhood arthritis, Juvenile, Arthritis, Genome-wide association study, Adolescents, Systemic inflammation, Major Histocompatibility Complex, 0302 clinical medicine, Human genetics, Risk Factors, Immunology and Allergy, health care economics and organizations, Genètica humana, Adult Onset Still's Disease, Gene Polymorphism, Juvenile Idiopathic Arthritis, Arthritis, Juvenile, Case-Control Studies, Chromosomes, Human, Pair 1, Genome-Wide Association Study, Genotype, Humans, Polymorphism, Single Nucleotide, Single Nucleotide, Pair 1, medicine.symptom, Human, musculoskeletal diseases, Immunology, Single-nucleotide polymorphism, Teenagers, Chromosomes, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Rheumatology, medicine, Polymorphism, 030203 arthritis & rheumatology, Cromosomes humans, Artritis, business.industry, Case-control study, medicine.disease, Genetic architecture, 030104 developmental biology, Gene polymorphism, business, Complex major d'histocompatibilitat, Genètica

Abstract

Annals of the rheumatic diseases 76(5), 906-913 (2017). doi:10.1136/annrheumdis-2016-210324, Published by BMJ Publ. Group, London

Published

2016

12. Genome-Wide Association Study in an Amerindian Ancestry Population Reveals Novel Systemic Lupus Erythematosus Risk Loci and the Role of European Admixture

Author

Lindsey A. Criswell, Swapan K. Nath, Astrid Rasmussen, Hugo R. Scherbarth, Teresa Tusié-Luna, Alejandra Babini, José Francisco Moctezuma, Jennifer A. Kelly, Robert P. Kimberly, Adam Adler, Patricia Ortiz-Tello, Sergio Toloza, Carl D. Langefeld, Marta E. Alarcón-Riquelme, Carlos Aguilar Salinas, Andrés Moreno-Estrada, Mercedes A. García, Chaim O. Jacob, Jorge M. Cucho-Venegas, Eduardo M. Acevedo-Vázquez, Raphael Zidovetzki, Mario H. Cardiel, Lorena Orozco, Guillermo A. Berbotto, Pedro Miranda, Jorge A. Esquivel-Valerio, Betty P. Tsao, Hannah C. Ainsworth, Bernardo A. Pons-Estel, Timothy J. Vyse, Vicente Baca, Judith A. James, Julio E. Molineros, Ignacio García-De La Torre, Luis J. Catoggio, Patrick M. Gaffney, Elena Sánchez-Rodríguez, Kenneth M. Kaufman, Kathy L. Sivils, Julie T. Ziegler, John B. Harley, Mary E. Comeau, Marco A. Maradiaga-Ceceña, Timothy D. Howard, and Sang Cheol Bae

Subjects

0301 basic medicine, Genetics, education.field_of_study, Lupus erythematosus, Immunology, Haplotype, Population, Locus (genetics), Genome-wide association study, Human leukocyte antigen, Biology, medicine.disease, 03 medical and health sciences, 030104 developmental biology, Rheumatology, Expression quantitative trait loci, medicine, Immunology and Allergy, education, Imputation (genetics)

Abstract

Objective Systemic lupus erythematosus (SLE) is a chronic autoimmune disease with a strong genetic component. We undertook the present work to perform the first genome-wide association study on individuals from the Americas who are enriched for Native American heritage. Methods We analyzed 3,710 individuals from the US and 4 countries of Latin America who were diagnosed as having SLE, and healthy controls. Samples were genotyped with HumanOmni1 BeadChip. Data on out-of-study controls genotyped with HumanOmni2.5 were also included. Statistical analyses were performed using SNPtest and SNPGWA. Data were adjusted for genomic control and false discovery rate. Imputation was performed using Impute2 and, for classic HLA alleles, HiBag. Odds ratios (ORs) and 95% confidence intervals (95% CIs) were calculated. Results The IRF5–TNPO3 region showed the strongest association and largest OR for SLE (rs10488631: genomic control–adjusted P [Pgcadj] = 2.61 × 10−29, OR 2.12 [95% CI 1.88–2.39]), followed by HLA class II on the DQA2–DQB1 loci (rs9275572: Pgcadj = 1.11 × 10−16, OR 1.62 [95% CI 1.46–1.80] and rs9271366: Pgcadj = 6.46 × 10−12, OR 2.06 [95% CI 1.71–2.50]). Other known SLE loci found to be associated in this population were ITGAM, STAT4, TNIP1, NCF2, and IRAK1. We identified a novel locus on 10q24.33 (rs4917385: Pgcadj = 1.39 × 10−8) with an expression quantitative trait locus (eQTL) effect (Peqtl = 8.0 × 10−37 at USMG5/miR1307), and several new suggestive loci. SLE risk loci previously identified in Europeans and Asians were corroborated. Local ancestry estimation showed that the HLA allele risk contribution is of European ancestral origin. Imputation of HLA alleles suggested that autochthonous Native American haplotypes provide protection against development of SLE. Conclusion Our results demonstrate that studying admixed populations provides new insights in the delineation of the genetic architecture that underlies autoimmune and complex diseases.

Published

2016

13. High-density genotyping of immune-related loci identifies new SLE risk variants in individuals with Asian ancestry

Author

Xana Kim-Howard, Takayuki Sumida, Celi Sun, Hong Zhang, Bok Ghee Han, Chang Hee Suh, Yong Beom Park, So Young Bang, Swapan K. Nath, Kwangwoo Kim, Nan Shen, Young Mo Kang, Kek Heng Chua, Yukinori Okada, Jonathan D. Wren, Yuan-yuan Qi, Julio E. Molineros, Akari Suzuki, Xu-jie Zhou, Seung Cheol Shim, Loren L. Looger, Sang Cheol Bae, Michiaki Kubo, John B. Harley, Adam Adler, Jung Yoon Choe, Hye Soon Lee, Young-Jin Kim, Kazuhiko Yamamoto, Prasenjeet Motghare, Yuta Kochi, Won Tae Chung, Kenneth M. Kaufman, Mikhail G. Dozmorov, Shin-Seok Lee, Tae-Hwan Kim, Jianyang Ma, and Krishna Bhattarai

Subjects

0301 basic medicine, Male, Genotype, Genotyping Techniques, CD226, Gene Expression, Locus (genetics), Genome-wide association study, Biology, Polymorphism, Single Nucleotide, Article, White People, 03 medical and health sciences, Asian People, Genetics, medicine, Humans, Lupus Erythematosus, Systemic, Genetic Predisposition to Disease, Genotyping, Lupus erythematosus, medicine.disease, Genetic architecture, 3. Good health, 030104 developmental biology, Female, Genome-Wide Association Study

Abstract

Systemic lupus erythematosus (SLE) has a strong but incompletely understood genetic architecture. We conducted an association study with replication in 4,478 SLE cases and 12,656 controls from six East Asian cohorts to identify new SLE susceptibility loci and better localize known loci. We identified ten new loci and confirmed 20 known loci with genome-wide significance. Among the new loci, the most significant locus was GTF2IRD1-GTF2I at 7q11.23 (rs73366469, Pmeta = 3.75 × 10(-117), odds ratio (OR) = 2.38), followed by DEF6, IL12B, TCF7, TERT, CD226, PCNXL3, RASGRP1, SYNGR1 and SIGLEC6. We identified the most likely functional variants at each locus by analyzing epigenetic marks and gene expression data. Ten candidate variants are known to alter gene expression in cis or in trans. Enrichment analysis highlights the importance of these loci in B cell and T cell biology. The new loci, together with previously known loci, increase the explained heritability of SLE to 24%. The new loci share functional and ontological characteristics with previously reported loci and are possible drug targets for SLE therapeutics.

Published

2016

14. GG-09 A role for EBNA2 in mechanisms that are responsible for lupus and other autoimmune diseases

Author

Artem Barski, Leah C. Kottyan, John B. Harley, Mario Pujato, Weirauch Mt, Albert F. Magnusen, Kenneth M. Kaufman, Nathan Salomonis, Kashish Chetal, Daniel Miller, X Chen, Carmy Forney, Arthur Lynch, Masashi Yukawa, and Avery Maddox

Subjects

Genetics, Prostate cancer, Systemic lupus erythematosus, Antigen, business.industry, medicine, GATA3, Disease, medicine.disease, business, Transcription factor, Phenotype, Virus

Abstract

Background Explaining the genetics of many diseases is challenging because most associations localize to incompletely understood regulatory regions. Methods We show that transcription factors (TFs) occupy multiple loci of individual complex genetic disorders much more than expected by chance using novel computational methods. Results Application to 213 phenotypes and 1,544 TF binding datasets identifies 2,264 relationships between hundreds of TFs and 94 phenotypes, including AR in prostate cancer and GATA3 in breast cancer. Strikingly, nearly half of the systemic lupus erythematosus risk loci are occupied by the Epstein-Barr virus (EBV) Nuclear Antigen 2 (EBNA2) protein (OR=6, P Conclusions Our results nominate mechanisms that operate across risk loci within disease phenotypes; they suggest new paradigms for disease origin and strongly support a role for Epstein-Barr virus in the generation of systemic lupus erythematosus, as well as of particular other autoimmune diseases, apparently related to lupus by the genomic mechanisms that produce them.

Published

2018

15. Whole-exome sequencing uncovers oxidoreductases DHTKD1 and OGDHL as linkers between mitochondrial dysfunction and eosinophilic esophagitis

Author

John B. Harley, Bruce J. Aronow, Xinjian Wang, Marc E. Rothenberg, Joseph D. Sherrill, Margaret H. Collins, Leah C. Kottyan, Taosheng Huang, Phillip J. Dexheimer, Ting Wen, Kiran Kc, J. Pablo Abonia, Philip E. Putnam, Adam C. Chamberlin, Qiang Wu, Emily M. Stucke, Kenneth M. Kaufman, and Yanyan Peng

Subjects

Adult, Male, 0301 basic medicine, Oxidoreductases Acting on CH-CH Group Donors, T-Lymphocytes, Inflammation, Esophageal Disorder, Mitochondrion, Biology, 03 medical and health sciences, 0302 clinical medicine, Exome Sequencing, medicine, Humans, DHTKD1, Ketoglutarate Dehydrogenase Complex, RNA, Small Interfering, Child, Eosinophilic esophagitis, Gene, Exome sequencing, Interleukin-13, Proteins, Epithelial Cells, Ketone Oxidoreductases, Eosinophilic Esophagitis, General Medicine, Fibroblasts, medicine.disease, Mitochondria, Up-Regulation, 030104 developmental biology, Viperin, Mutation, Cancer research, Cytokines, Female, medicine.symptom, Oxidoreductases, Research Article, 030215 immunology

Abstract

Eosinophilic esophagitis (EoE) is an allergic inflammatory esophageal disorder with a complex underlying genetic etiology often associated with other comorbidities. Using whole-exome sequencing (WES) of 63 patients with EoE and 60 unaffected family members and family-based trio analysis, we sought to uncover rare coding variants. WES analysis identified 5 rare, damaging variants in dehydrogenase E1 and transketolase domain–containing 1 (DHTKD1). Rare variant burden analysis revealed an overabundance of putative, potentially damaging DHTKD1 mutations in EoE (P = 0.01). Interestingly, we also identified 7 variants in the DHTKD1 homolog oxoglutarate dehydrogenase-like (OGDHL). Using shRNA-transduced esophageal epithelial cells and/or patient fibroblasts, we further showed that disruption of normal DHTKD1 or OGDHL expression blunts mitochondrial function. Finally, we demonstrated that the loss of DHTKD1 expression increased ROS production and induced the expression of viperin, a gene previously shown to be involved in production of Th2 cytokines in T cells. Viperin had increased expression in esophageal biopsies of EoE patients compared with control individuals and was upregulated by IL-13 in esophageal epithelial cells. These data identify a series of rare genetic variants implicating DHTKD1 and OGDHL in the genetic etiology of EoE and underscore a potential pathogenic role for mitochondrial dysfunction in EoE.

Published

2018

16. Genetic variants at the 16p13 locus confer risk for eosinophilic esophagitis

Author

Julian R. Braxton, Avery Maddox, J. Pablo Abonia, Jennifer A. Kelly, John B. Harley, Glenn T. Furuta, Patrick M. Gaffney, Brian P. Vickery, Peter Dawson, Hugh A. Sampson, Kenneth M. Kaufman, Leah C. Kottyan, Robbie D. Pesek, Emily M. Stucke, Philip E. Putnam, Marc E. Rothenberg, Vince Mukkada, Kathy L. Sivils, Robert P. Kimberly, Robert A. Wood, Lisa J. Martin, and Mirna Chehade

Subjects

0301 basic medicine, Monosaccharide Transport Proteins, Immunology, Population, Genome-wide association study, Locus (genetics), Disease, CLEC16A, Biology, Major histocompatibility complex, Article, 03 medical and health sciences, 0302 clinical medicine, Genetics, medicine, Humans, Lectins, C-Type, Eosinophilic esophagitis, education, Genotyping, Genetics (clinical), 2. Zero hunger, education.field_of_study, Polymorphism, Genetic, Membrane Proteins, Nuclear Proteins, Eosinophilic Esophagitis, medicine.disease, 3. Good health, DNA-Binding Proteins, 030104 developmental biology, Genetic Loci, biology.protein, Trans-Activators, Chromosomes, Human, Pair 16, 030215 immunology

Abstract

Eosinophilic esophagitis (EoE) is a chronic inflammatory disease of the esophagus triggered by immune hypersensitivity to food. Herein, we tested whether genetic risk factors for known, non-allergic, immune-mediated diseases, particularly those involving autoimmunity, were associated with EoE risk. We used the high-density Immunochip platform, encoding 200,000 genetic variants for major auto-immune disease. Accordingly, 1,214 subjects with EoE of European ancestry and 3,734 population controls were genotyped and assessed using data directly generated or imputed from the previously published GWAS. We found lack of association of EoE with the genetic variants in the major histocompatibility complex (MHC) class I, II, and III genes and nearly all other loci using a highly powered study design with dense genotyping throughout the locus. Importantly, we identified an EoE risk locus at 16p13 with genome-wide significance (Pcombined = 2.05 × 10−9, odds ratio = 0.76–0.81). This region is known to encode for the genes CLEC16A, DEXI, and CIITI, which are expressed in immune cells and esophageal epithelial cells. Suggestive EoE risk were also seen 5q23 (intergenic) and 7p15 (JAZF1). Overall, we have identified an additional EoE risk locus at 16p13 and highlight a shared and unique genetic etiology of EoE with a spectrum of immune-associated diseases.

Published

2018

17. A plausibly causal functional lupus-associated risk variant in the STAT1-STAT4 locus

Author

Swapan K. Nath, Arthur Lynch, Zubin Patel, Daniel J. Wallace, Miranda C. Marion, Michael Henrickson, Hannah C. Ainsworth, Kenneth M. Kaufman, Gary S. Gilkeson, Lindsey A. Criswell, Adrienne H. Williams, Connor Schroeder, Daniel Miller, Adam Adler, Joel M. Guthridge, Kathy L. Sivils, Erin E. Zoller, Deborah S. Cunninghame Graham, So Young Bang, Joshua Lee, Julie T. Ziegler, John B. Harley, Joan T. Merrill, R. Hal Scofield, Stuart B. Glenn, Patrick M. Gaffney, Hermine I. Brunner, Anne M. Stevens, Juan-Manuel Anaya, Mary E. Comeau, Judith A. James, Marta E. Alarcón-Riquelme, Avery Maddox, John D. Reveille, Diane L. Kamen, Lois Parks, Rosalind Ramsey-Goldman, Timothy J. Vyse, Edward K. Wakeland, Elizabeth E. Brown, Robert P. Kimberly, Michael H. Weisman, Carmy Forney, Bernardo A. Pons-Estel, Albert F. Magnusen, Hye Soon Lee, Susan A. Boackle, Sang Cheol Bae, Luis M. Vilá, Jennifer A. Kelly, Carl D. Langefeld, Michelle Petri, Xiaoting Chen, Matthew T. Weirauch, Jeffrey C. Edberg, Graciela S. Alarcón, Jennifer Huggins, Earl D. Silverman, Betty P. Tsao, Nan Shen, Timothy B. Niewold, Barry I. Freedman, Leah C. Kottyan, Mario Pujato, Bahram Namjou, Javier Martin, Prithvi Raj, Xiaoming Lu, and Chaim O. Jacob

Subjects

0301 basic medicine, Male, HMGA1 protein, Unclassified drug, Protein domain, Intron, High mobility group A protein, Gene locus, immune system diseases, Risk Factors, STAT4 protein, Lupus Erythematosus, Systemic, Expression quantitative trait locus, skin and connective tissue diseases, STAT4, Genetics (clinical), Priority journal, Genetics, Allele, Systemic lupus erythematosus, Lupus vulgaris, Association Studies Articles, General Medicine, STAT4 Transcription Factor, Multicenter study, Clinical trial, STAT1 Transcription Factor, Female, Quantitative trait locus, Functional disease, Quantitative Trait Loci, Locus (genetics), Biology, Article, 03 medical and health sciences, Genetic, STAT1 protein, medicine, Humans, human, DNA binding, Polymorphism, Molecular Biology, Alleles, Lupus erythematosus, Polymorphism, Genetic, Genetic polymorphism, Lupus Erythematosus, Systemic, medicine.disease, 030104 developmental biology, Expression quantitative trait loci, Protein expression, Genetic variability, Risk factor, B-lymphocyte cell line, Controlled study

Abstract

Systemic lupus erythematosus (SLE or lupus) (OMIM: 152700) is a chronic autoimmune disease with debilitating inflammation that affects multiple organ systems. The STAT1-STAT4 locus is one of the first and most highly replicated genetic loci associated with lupus risk. We performed a fine-mapping study to identify plausible causal variants within the STAT1-STAT4 locus associated with increased lupus disease risk. Using complementary frequentist and Bayesian approaches in trans-ancestral Discovery and Replication cohorts, we found one variant whose association with lupus risk is supported across ancestries in both the Discovery and Replication cohorts: rs11889341. In B cell lines from patients with lupus and healthy controls, the lupus risk allele of rs11889341 was associated with increased STAT1 expression. We demonstrated that the transcription factor HMGA1, a member of the HMG transcription factor family with an AT-hook DNA-binding domain, has enriched binding to the risk allele compared with the non-risk allele of rs11889341.We identified a genotype-dependent repressive element in the DNA within the intron of STAT4 surrounding rs11889341. Consistent with expression quantitative trait locus (eQTL) analysis, the lupus risk allele of rs11889341 decreased the activity of this putative repressor. Altogether, we present a plausible molecular mechanism for increased lupus risk at the STAT1-STAT4 locus in which the risk allele of rs11889341, the most probable causal variant, leads to elevated STAT1 expression in B cells due to decreased repressor activity mediated by increased binding of HMGA1. © The Author(s) 2018. Published by Oxford University Press. All rights reserved.

Published

2018

18. Identification of a Sjögren's syndrome susceptibility locus at OAS1 that influences isoform switching, protein expression, and responsiveness to type I interferons

Author

He Li, Tove Ragna Reksten, John A Ice, Jennifer A Kelly, Indra Adrianto, Astrid Rasmussen, Shaofeng Wang, Bo He, Kiely M Grundahl, Stuart B Glenn, Corinne Miceli-Richard, Simon Bowman, Sue Lester, Per Eriksson, Maija-Leena Eloranta, Johan G Brun, Lasse G Gøransson, Erna Harboe, Joel M Guthridge, Kenneth M Kaufman, Marika Kvarnström, Deborah S Cunninghame Graham, Ketan Patel, Adam J Adler, A Darise Farris, Michael T Brennan, James Chodosh, Rajaram Gopalakrishnan, Michael H Weisman, Swamy Venuturupalli, Daniel J Wallace, Kimberly S Hefner, Glen D Houston, Andrew J W Huang, Pamela J Hughes, David M Lewis, Lida Radfar, Evan S Vista, Contessa E Edgar, Michael D Rohrer, Donald U Stone, Timothy J Vyse, John B Harley, Patrick M Gaffney, Judith A James, Sean Turner, Ilias Alevizos, Juan-Manuel Anaya, Nelson L Rhodus, Barbara M Segal, Courtney G Montgomery, R Hal Scofield, Susan Kovats, Xavier Mariette, Lars Rönnblom, Torsten Witte, Maureen Rischmueller, Marie Wahren-Herlenius, Roald Omdal, Roland Jonsson, Wan-Fai Ng, for UK Primary Sjögren's Syndrome Registry, Gunnel Nordmark, Christopher J Lessard, and Kathy L Sivils

Subjects

0301 basic medicine, Male, Cancer Research, Medicin och hälsovetenskap, Microarrays, Physiology, Protein Expression, Gene Expression, Biochemistry, Medical and Health Sciences, 0302 clinical medicine, Silicone oil, Interferon, Immune Physiology, Vitrectomy, Medicine and Health Sciences, 2',5'-Oligoadenylate Synthetase, Genetics (clinical), Immune System Proteins, Neuronal apoptosis, 3. Good health, Body Fluids, Nucleic acids, Bioassays and Physiological Analysis, Blood, Sjogren's Syndrome, Virus Diseases, Interferon Type I, Medical genetics, Female, Anatomy, Medical Genetics, medicine.drug, Research Article, musculoskeletal diseases, Gene isoform, medicine.medical_specialty, lcsh:QH426-470, Immunology, Quantitative Trait Loci, Biology, Research and Analysis Methods, Antibodies, Article, 03 medical and health sciences, stomatognathic system, medicine, Genetic predisposition, Genetics, Gene Expression and Vector Techniques, Humans, Genetic Predisposition to Disease, Allele, Molecular Biology Techniques, Molecular Biology, Ecology, Evolution, Behavior and Systematics, Alleles, Genetic Association Studies, Medicinsk genetik, Autoantibodies, Un-explained visual loss, 030203 arthritis & rheumatology, Müller cells, Molecular Biology Assays and Analysis Techniques, Autoantibody, Biology and Life Sciences, Proteins, medicine.disease, eye diseases, Lymphoma, stomatognathic diseases, Alternative Splicing, lcsh:Genetics, 030104 developmental biology, RNA processing, Gene Expression Regulation, Retinal detachment, Genetics of Disease, Potassium, RNA, Interferons, Interferon type I

Abstract

Sjögren’s syndrome (SS) is a common, autoimmune exocrinopathy distinguished by keratoconjunctivitis sicca and xerostomia. Patients frequently develop serious complications including lymphoma, pulmonary dysfunction, neuropathy, vasculitis, and debilitating fatigue. Dysregulation of type I interferon (IFN) pathway is a prominent feature of SS and is correlated with increased autoantibody titers and disease severity. To identify genetic determinants of IFN pathway dysregulation in SS, we performed cis-expression quantitative trait locus (eQTL) analyses focusing on differentially expressed type I IFN-inducible transcripts identified through a transcriptome profiling study. Multiple cis-eQTLs were associated with transcript levels of 2'-5'-oligoadenylate synthetase 1 (OAS1) peaking at rs10774671 (PeQTL = 6.05 × 10−14). Association of rs10774671 with SS susceptibility was identified and confirmed through meta-analysis of two independent cohorts (Pmeta = 2.59 × 10−9; odds ratio = 0.75; 95% confidence interval = 0.66–0.86). The risk allele of rs10774671 shifts splicing of OAS1 from production of the p46 isoform to multiple alternative transcripts, including p42, p48, and p44. We found that the isoforms were differentially expressed within each genotype in controls and patients with and without autoantibodies. Furthermore, our results showed that the three alternatively spliced isoforms lacked translational response to type I IFN stimulation. The p48 and p44 isoforms also had impaired protein expression governed by the 3' end of the transcripts. The SS risk allele of rs10774671 has been shown by others to be associated with reduced OAS1 enzymatic activity and ability to clear viral infections, as well as reduced responsiveness to IFN treatment. Our results establish OAS1 as a risk locus for SS and support a potential role for defective viral clearance due to altered IFN response as a genetic pathophysiological basis of this complex autoimmune disease., Author summary Sjögren’s syndrome (SS) is a common autoimmune condition where immune cells infiltrate moisture-producing glands, leading to dryness typically in the eyes and mouth. SS patients also manifest debilitating fatigue as well as other diseases in liver, lung, kidney, and skin. The cause of this complex disease is still not fully understood; however, an environmental trigger, such as viral infections, in individuals with genetic risk factor(s) is thought to contribute to the development of SS. Type 1 interferons (IFNs) are one of the first defenders after viral infection and induce the expression of various virus-responding genes. Perpetual elevation of type 1 IFN signaling has been observed in SS patients. Here, we first replicated previously identified RNA transcripts contributing to the abnormal type 1 IFN signaling in SS patients. We then identified a disease-associated genetic variant in an IFN-inducible gene, OAS1. This variant governs splicing of OAS1, altering the transcript into multiple isoforms that lack protein expression and responsiveness to IFNs. The results of this study may provide insight into the genetic basis of SS, as well as other autoimmune disease with similar dysregulation in the type 1 IFN system.

Published

2017

19. Transancestral mapping and genetic load in systemic lupus erythematosus

Author

László Kovács, Helle Laustrup, Michael F. Seldin, Jeffrey C. Edberg, Swapan K. Nath, John D. Reveille, Diane L. Kamen, Quan Zhen Li, Guillermo A. Berbotto, Betty P. Tsao, Lennart Truedsson, Dafna D. Gladman, Mario H. Cardiel, Robert R. Graham, Chaim O. Jacob, Carlos Vasconcelos, Iñigo de la Rúa Figueroa, Mary E. Comeau, Deborah S. Cunninghame Graham, Iva Gunnarsson, Rosalind Ramsey-Goldman, Ignacio García-De La Torre, Luis J. Catoggio, Miranda C. Marion, Pedro Miranda, John D. Rioux, Laura E. Schanberg, Jorge R. Oksenberg, Earl D. Silverman, David R. McWilliams, Solbritt Rantapää Dahlqvist, Jennifer A. Croker, Raffaella Scorza, Carl D. Langefeld, Susan D. Thompson, Edward K. Wakeland, Elizabeth E. Brown, Berta Martins da Silva, Christopher Sjöwall, Kenneth M. Kaufman, Jennifer Huggins, Johan Frostegård, Lars Rönnblom, Joan E. Wither, Joseph M. McCune, Laurie P Russell, Sandra D'Alfonso, Johanna K. Sandling, Timothy W. Behrens, Mercedes A. García, Andrea Doria, Vicente Baca, Joel M. Guthridge, Bernardo A. Pons-Estel, José Francisco Moctezuma, Bernard Lauwerys, Sergio Toloza, Timothy D. Howard, Kathy L. Sivils, Hannah C. Ainsworth, Patrick M. Gaffney, David L. Morris, Jorge A. Esquivel-Valerio, Christian A. Pineau, Michelle Petri, Elisabet Svenungsson, Daniel J. Wallace, Norberto Ortego-Centeno, Robert P. Kimberly, Jonas Carlsson Almlöf, Gary S. Gilkeson, Lorena Orozco, Peter K. Gregersen, Judith A. James, Teresa Tusié-Luna, Paul R. Fortin, Marc Bijl, Jennifer A. Kelly, Timothy B. Niewold, Ricard Cervera, Timothy J. Vyse, Javier Martín, Prithvi Raj, Barry I. Freedman, Eduardo Acevedo-Vásquez, Carlos A. Aguilar-Salinas, Paula S. Ramos, Emőke Endreffy, Michael H. Weisman, Leah C. Kottyan, Janet E. Pope, Ann-Christine Syvänen, Joan T. Merrill, Hermine I. Brunner, Luis M. Vilá, Anders A. Bengtsson, Graciela S. Alarcón, Marta E. Alarcón-Riquelme, Jorge M. Cucho-Venegas, John B. Harley, Cees G. M. Kallenberg, Marco A. Maradiaga-Ceceña, David R. Karp, Lindsey A. Criswell, José Mario Sabio, Tushar Bhangale, Hugo R. Scherbarth, Alejandra Babini, UCL - SSS/IREC/RUMA - Pôle de Pathologies rhumatismales, UCL - (SLuc) Service de rhumatologie, Universitat de Barcelona, and Translational Immunology Groningen (TRIGR)

Subjects

0301 basic medicine, Genetics and Molecular Biology (all), Medicin och hälsovetenskap, Multifactorial Inheritance, Autoimmune diseases, General Physics and Astronomy, Genome-wide association study, VARIANTS, Medical and Health Sciences, Biochemistry, DISEASE, 0302 clinical medicine, Human genetics, HLA Antigens, immune system diseases, Genotype, Lupus Erythematosus, Systemic, 03.02. Klinikai orvostan, Age of Onset, skin and connective tissue diseases, Sequence Deletion, Genetics, REVISED CRITERIA, Genètica humana, Multidisciplinary, Malalties autoimmunitàries, Chemistry (all), Hispanic or Latino, 3. Good health, Genetic load, SHARED EPITOPE HYPOTHESIS, HLA, Estudi de casos, CAUCASIAN POPULATIONS, Medical genetics, Genetic Load, Medical Genetics, medicine.medical_specialty, SUSCEPTIBILITY LOCI, Science, Black People, Human leukocyte antigen, Biology, Polymorphism, Single Nucleotide, Article, White People, General Biochemistry, Genetics and Molecular Biology, PHYLOGENETIC TREES, 03 medical and health sciences, Physics and Astronomy (all), Journal Article, medicine, Humans, GENOME-WIDE ASSOCIATION, American Indian or Alaska Native, Medicinsk genetik, 030203 arthritis & rheumatology, Lupus erythematosus, Case-control study, General Chemistry, medicine.disease, RHEUMATOID-ARTHRITIS, Mutagenesis, Insertional, Logistic Models, 030104 developmental biology, Lupus eritematós, Case-Control Studies, Immunology, Case studies, Biochemistry, Genetics and Molecular Biology (all), Anti-SSA/Ro autoantibodies

Abstract

Systemic lupus erythematosus (SLE) is an autoimmune disease with marked gender and ethnic disparities. We report a large transancestral association study of SLE using Immunochip genotype data from 27,574 individuals of European (EA), African (AA) and Hispanic Amerindian (HA) ancestry. We identify 58 distinct non-HLA regions in EA, 9 in AA and 16 in HA (∼50% of these regions have multiple independent associations); these include 24 novel SLE regions (P, Systemic lupus erythematosus (SLE) is an autoimmune disease with a strong ethnic and gender bias. In a transancestral genetic association study, Langefeld et al. identify 24 novel regions associated with risk to lupus and propose a cumulative hits hypothesis for loci conferring risk to SLE.

Published

2017

20. Whole-Exome Sequencing Reveals Overlap Between Macrophage Activation Syndrome in Systemic Juvenile Idiopathic Arthritis and Familial Hemophagocytic Lymphohistiocytosis

Author

Joseph D. Szustakowski, Kenneth M. Kaufman, N. R. Nirmala, Alexandra H. Filipovich, Fan Yang, Alexei A. Grom, Ammar Husami, Ndate Fall, John B. Harley, Bolan Linghu, and Kejian Zhang

Subjects

musculoskeletal diseases, Genetics, Candidate gene, genetic structures, Sequence analysis, Immunology, Familial Hemophagocytic Lymphohistiocytosis, Biology, Compound heterozygosity, medicine.disease, Rheumatology, Macrophage activation syndrome, medicine, Immunology and Allergy, Gene, Exome, Exome sequencing

Abstract

Objective Macrophage activation syndrome (MAS), a life-threatening complication of systemic juvenile idiopathic arthritis (JIA), resembles familial hemophagocytic lymphohistiocytosis (HLH), a constellation of autosomal-recessive immune disorders resulting from deficiency in cytolytic pathway proteins. We undertook this study to test our hypothesis that MAS predisposition in systemic JIA could be attributed to rare gene sequence variants affecting the cytotolytic pathway. Methods Whole-exome sequencing was used in 14 patients with systemic JIA and MAS and in their parents to identify protein-altering single-nucleotide polymorphisms/indels in known HLH-associated genes. To discover new candidate genes, the entire whole-exome sequencing data were filtered to identify protein-altering, rare recessive homozygous, compound heterozygous, and de novo variants with the potential to affect the cytolytic pathway. Results Heterozygous protein-altering rare variants in the known genes (LYST,MUNC13-4, and STXBP2) were found in 5 of 14 patients with systemic JIA and MAS (35.7%). This was in contrast to only 4 variants in 4 of 29 patients with systemic JIA without MAS (13.8%). Homozygosity and compound heterozygosity analysis applied to the entire whole-exome sequencing data in systemic JIA/MAS revealed 3 recessive pairs in 3 genes and compound heterozygotes in 73 genes. We also identified 20 heterozygous rare protein-altering variants that occurred in at least 2 patients. Many of the identified genes encoded proteins with a role in actin and microtubule reorganization and vesicle-mediated transport. "Cellular assembly and organization" was the top cellular function category based on Ingenuity Pathways Analysis (P < 3.10 × 10-5). Conclusion Whole-exome sequencing performed in patients with systemic JIA and MAS identified rare protein-altering variants in known HLH-associated genes as well as in new candidate genes.

Published

2014

21. ABIN1 Dysfunction as a Genetic Basis for Lupus Nephritis

Author

Carl D. Langefeld, Gary S. Gilkeson, John B. Harley, Ryan M. Sheehan, Chaim O. Jacob, Susan A. Boackle, Timothy B. Niewold, Anne M. Stevens, John D. Reveille, Betty P. Tsao, Jeffrey C. Edberg, Rachel T. G'Sell, Erik A. Korte, Barry I. Freedman, K R McLeish, Rebecca K. Oliver, Darrell W. Freeman, Judith A. James, Juan-Manuel Anaya, Diane L. Kamen, Marta E. Alarcón-Riquelme, Susan Coventry, Patrick M. Gaffney, Lindsey A. Criswell, Indra Adrianto, Rosalind Ramsey-Goldman, Sang Cheol Bae, Bernardo A. Pons-Estel, Dawn J. Caster, Jennifer A. Kelly, Michelle Petri, Sambit K. Nanda, Javier Martin, David W. Powell, Kenneth M. Kaufman, Joel M. Guthridge, Kathy L. Sivils, Robert P. Kimberly, Elizabeth E. Brown, Luis M. Vilá, Graciela S. Alarcón, Timothy J. Vyse, Joan T. Merrill, R. Hal Scofield, and Philip Cohen

Subjects

single nucleotide, Mouse, Lupus nephritis, Fluorescent Antibody Technique, knockout, Disease, Mitogen activated protein kinase, Kidney, Toll like receptor, Gene, Pathogenesis, Mice, immune system diseases, skin and connective tissue diseases, Priority journal, Mice, Knockout, Systemic lupus erythematosus, NF-kappa B, General Medicine, Lupus Nephritis, DNA-Binding Proteins, Fluorescent antibody technique, Nephrology, inbred c57bl, A20 binding inhibitor of immunoglobulin enhancer binding protein 1 gene, Nephritis, Genotype, Biology, Polymorphism, Single Nucleotide, Pathophysiology, Article, European american, Immune system, medicine, Animals, Humans, Animal model, Animal experiment, African american, Polymorphism, Autoimmune disease, Immunocompetent cell, Nonhuman, medicine.disease, Dna-binding proteins, Single nucleotide polymorphism, Mice, Inbred C57BL, Basic Research, Immunoglobulin enhancer binding protein, Nf-kappa b, Lupus erythematosus nephritis, Immunology, Controlled study, Anti-SSA/Ro autoantibodies

Abstract

The genetic factors underlying the pathogenesis of lupus nephritis associated with systemic lupus erythematosus are largely unknown, although animal studies indicate that nuclear factor (NF)-?B is involved. We reported previously that aknockin mouse expressinganin active form of ABIN1 (ABIN1[D485N]) develops lupus-like autoimmune disease and demonstrates enhanced activation of NF-?B and mitogen-activated protein kinases in immune cells after toll-like receptor stimulation. In the current study, we show that ABIN1[D485N] mice develop progressive GN similar to class III and IV lupus nephritis in humans. To investigate the clinical relevance of ABIN1 dysfunction, we genotyped five single-nucleotide polymorphisms in the gene encoding ABIN1, TNIP1, in samples from European-American, African American, Asian, Gullah, and Hispanic participants in the Large Lupus Association Study 2. Comparing cases of systemic lupus erythematosus with nephritis and cases ofsystemic lupus erythematosus without nephritis revealed strong associations with lupus nephritis at rs7708392 in European Americans and rs4958881 in African Americans. Comparing cases of systemic lupus erythematosus with nephritis and healthy controls revealed a stronger association at rs7708392 in European Americans but not at rs4958881 in African Americans. Our data suggest that variants in the TNIP1 gene are associated with the risk for lupus nephritis and could be mechanistically involved in disease development via aberrant regulation of NF-?B and mitogen-activated protein kinase activity. Copyright © 2013 by the American Society of Nephrology.

Published

2013

22. Profound loss of esophageal tissue differentiation in patients with eosinophilic esophagitis

Author

Mary C. Bedard, Bruce J. Aronow, Jeffrey K. Rymer, Mark Rochman, Kiran Kc, Kenneth M. Kaufman, Cora E. Miracle, Jared Travers, Benjamin P. Davis, Julie M. Caldwell, Ting Wen, Marc E. Rothenberg, Joseph D. Sherrill, and Nurit P. Azouz

Subjects

0301 basic medicine, Male, Pathology, medicine.medical_specialty, Adolescent, Immunology, Biology, Article, Transcriptome, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, Esophagus, Biopsy, medicine, Immunology and Allergy, Humans, Eosinophilic esophagitis, Child, Exome sequencing, Interleukin-13, medicine.diagnostic_test, Cell Differentiation, Epithelial Cells, Eosinophilic Esophagitis, medicine.disease, Esophageal Tissue, 030104 developmental biology, Keratin 4, 030220 oncology & carcinogenesis, Interleukin 13, Mutation, biology.protein, Female

Abstract

Background A key question in the allergy field is to understand how tissue-specific disease is manifested. Eosinophilic esophagitis (EoE) is an emerging tissue-specific allergic disease with an unclear pathogenesis. Objective Herein we tested the hypothesis that a defect in tissue-specific esophageal genes is an integral part of EoE pathogenesis. Methods We interrogated the pattern of expression of esophagus-specific signature genes derived from the Human Protein Atlas in the EoE transcriptome and in EPC2 esophageal epithelial cells. Western blotting and immunofluorescence were used for evaluating expression of esophageal proteins in biopsy specimens from control subjects and patients with active EoE. Whole-exome sequencing was performed to identify mutations in esophagus-specific genes. Results We found that approximately 39% of the esophagus-specific transcripts were altered in patients with EoE, with approximately 90% being downregulated. The majority of transcriptional changes observed in esophagus-specific genes were reproduced in vitro in esophageal epithelial cells differentiated in the presence of IL-13. Functional enrichment analysis revealed keratinization and differentiation as the most affected biological processes and identified IL-1 cytokines and serine peptidase inhibitors as the most dysregulated esophagus-specific protein families in patients with EoE. Accordingly, biopsy specimens from patients with EoE evidenced a profound loss of tissue differentiation, decreased expression of keratin 4 (KRT4) and cornulin (CRNN) , and increased expression of KRT5 and KRT14 . Whole-exome sequencing of 33 unrelated patients with EoE revealed 39 rare mutations in 18 esophagus-specific differentially expressed genes. Conclusions A tissue-centered analysis has revealed a profound loss of esophageal tissue differentiation (identity) as an integral and specific part of the pathophysiology of EoE and implicated protease- and IL-1–related activities as putative central pathways in disease pathogenesis.

Published

2016

23. Decreased SMG7 expression associates with lupus-risk variants and elevated antinuclear antibody production

Author

Betty P. Tsao, Jennifer A. Kelly, Michelle Petri, Bevra H. Hahn, Marta E. Alarcón-Riquelme, John B. Harley, Patrick M. Gaffney, Anne M. Stevens, Vadim Osadchiy, Robert P. Kimberly, Yun Deng, Luis M. Vilá, Elizabeth E. Brown, Kenneth M. Kaufman, Susan A. Boackle, Juan-Manuel Anaya, Graciela S. Alarcón, I. I.Woong Sohn, Chaim O. Jacob, Daisuke Sakurai, Jian Zhao, Carl D. Langefeld, John D. Reveille, Deh Ming Chang, Seung Ro Lee, Kathy Moser Sivils, Yeong Wook Song, Judith A. James, Diane L. Kamen, Jennifer M. Grossman, Joan T. Merrill, R. Hal Scofield, Timothy B. Niewold, Timothy J. Vyse, Andrea L. Sestak, Barry I. Freedman, Rita M. Cantor, Rosalind Ramsey-Goldman, Gary S. Gilkeson, Jeffrey C. Edberg, Sang Cheol Bae, and Lindsey A. Criswell

Subjects

Nmnat2 gene, Male, Anti-nuclear antibody, Genotyping Techniques, Ribonucleoprotein antibody, Messenger rna, Genome-wide association study, Real time polymerase chain reaction, Gene, Linkage Disequilibrium, Raji cell line, Immunoglobulin g, antinuclear, American native continental ancestry group, education.field_of_study, Gene knockdown, Systemic lupus erythematosus, Genetic transcription, Gene silencing, Gene linkage disequilibrium, Hispanic or Latino, Raji cell, Pedigree, Correlational study, Nmnat2 protein, American indian, Human, Genotype, Immunology, Case control study, mononuclear, Major clinical study, Hek293 cell line, Hek293 cells, General Biochemistry, Genetics and Molecular Biology, White People, Article, 03 medical and health sciences, Smg7 gene, Rheumatology, Genetics, Humans, RNA, Messenger, education, Alleles, Autoantibodies, Lupus erythematosus, Genetic predisposition, Hispanic americans, Peripheral blood mononuclear cell, systemic, medicine.disease, Multicenter study (topic), messenger, 030104 developmental biology, Human cell, Risk factors, Leukocytes, Mononuclear, Gene polymorphism, Gene expression, Risk factor, Carrier Proteins, 0301 basic medicine, Carrier proteins, Luciferase assay, Carrier protein, Hispanic, Antibody production, Real-time polymerase chain reaction, Smg7 protein, Risk Factors, Sm antibody, Leukocytes, Immunology and Allergy, Lupus Erythematosus, Systemic, Regulatory mechanism, Nicotinamide-Nucleotide Adenylyltransferase, Priority journal, Allele, Antibody titer, Promoter region, Ethnic difference, Genotyping technique, Embryo, Antibodies, Antinuclear, Female, Nicotinamide-nucleotide adenylyltransferase, Quantitative trait locus, Risk, Nicotinamide nucleotide adenylyltransferase, Population, Genetic predisposition to disease, Mononuclear cell, Biology, Small interfering rna, Caucasian, Real-Time Polymerase Chain Reaction, Antibodies, Antinuclear antibody, Genotyping techniques, medicine, Linkage disequilibrium, Genetic Predisposition to Disease, American Indian or Alaska Native, Autoantibody, Molecular biology, Single nucleotide polymorphism, HEK293 Cells, Metabolism, Genetic association, Rna, Genetic variability, Cell culture, Controlled study, Gene function, Genome-Wide Association Study, European continental ancestry group

Abstract

ObjectivesFollowing up the systemic lupus erythematosus (SLE) genome-wide association studies (GWAS) identification of NMNAT2 at rs2022013, we fine-mapped its 150 kb flanking regions containing NMNAT2 and SMG7 in a 15 292 case–control multi-ancestry population and tested functions of identified variants.MethodsWe performed genotyping using custom array, imputation by IMPUTE 2.1.2 and allele specific functions using quantitative real-time PCR and luciferase reporter transfections. SLE peripheral blood mononuclear cells (PBMCs) were cultured with small interfering RNAs to measure antinuclear antibody (ANA) and cyto/chemokine levels in supernatants using ELISA.ResultsWe confirmed association at NMNAT2 in European American (EA) and Amerindian/Hispanic ancestries, and identified independent signal at SMG7 tagged by rs2702178 in EA only (p=2.4×10−8, OR=1.23 (95% CI 1.14 to 1.32)). In complete linkage disequilibrium with rs2702178, rs2275675 in the promoter region robustly associated with SMG7 mRNA levels in multiple expression quantitative trait locus (eQTL) datasets. Its risk allele was dose-dependently associated with decreased SMG7 mRNA levels in PBMCs of 86 patients with SLE and 119 controls (p=1.1×10−3 and 6.8×10−8, respectively) and conferred reduced transcription activity in transfected HEK-293 (human embryonic kidney cell line) and Raji cells (p=0.0035 and 0.0037, respectively). As a critical component in the nonsense-mediated mRNA decay pathway, SMG7 could regulate autoantigens including ribonucleoprotein (RNP) and Smith (Sm). We showed SMG7 mRNA levels in PBMCs correlated inversely with ANA titres of patients with SLE (r=−0.31, p=0.01), and SMG7 knockdown increased levels of ANA IgG and chemokine (C-C motif) ligand 19 in SLE PBMCs (p=2.0×10−5 and 2.0×10−4, respectively).ConclusionWe confirmed NMNAT2 and identified independent SMG7 association with SLE. The inverse relationship between levels of the risk allele-associated SMG7 mRNAs and ANA suggested the novel contribution of mRNA surveillance pathway to SLE pathogenesis.

Published

2016

24. Impact of genetic ancestry and sociodemographic status on the clinical expression of systemic lupus erythematosus in American Indian-European populations

Author

Carlos E. Perandones, Ignacio García-De La Torre, Adrianne H. Williams, Luis M. Vilá, Kathy L. Moser, Vicente Baca, Jennifer A. Kelly, Michelle Petri, Graciela S. Alarcón, Rosalind Ramsey-Goldman, Timothy J. Vyse, Astrid Rasmussen, Mary E. Comeau, I. Annelise Goecke, Teresa Tusié-Luna, Elizabeth E. Brown, José Francisco Moctezuma, Jorge L. Musuruana, Chaim O. Jacob, Kenneth M. Kaufman, Robert P. Kimberly, Cecilia Castel, Juan-Manuel Anaya, Timothy B. Niewold, Marco A. Maradiaga-Ceceña, Gary S. Gilkeson, Julie T. Ziegler, Marta E. Alarcón-Riquelme, John D. Reveille, Hugo A. Laborde, Laura Riba, Eduardo Acevedo-Vásquez, Mario H. Cardiel, P Alba, Adam Adler, Bernardo A. Pons-Estel, Stuart B. Glenn, Javier Martin, John B. Harley, Patrick M. Gaffney, Judith A. James, Pedro Miranda, Jacqueline Rodriguez-Amado, Carl D. Langefeld, Joan T. Merrill, R. Hal Scofield, Elena Sánchez, Jeffrey C. Edberg, Jorge A. Esquivel-Valerio, Susan A. Boackle, Betty P. Tsao, Lorena Orozco, Lindsey A. Criswell, and Miranda C. Marion

Subjects

Male, Neurologic disease, Heredity, Population genetics, Lupus nephritis, Skin disease, Logistic regression, Indians, Photosensitivity, Risk Factors, Prevalence, Malar rash, South American, Lupus Erythematosus, Systemic, Immunology and Allergy, Pharmacology (medical), Mouth ulcer, Young adult, Child, Priority journal, Risk assessment, Genetic analysis, Kidney disease, Middle Aged, Lupus Nephritis, Genotyping technique, Europe, American Indian, Public Health and Health Services, Female, medicine.symptom, Serositis, North American, Human, Adult, medicine.medical_specialty, Adolescent, Genotype, Genetic genealogy, Clinical Sciences, European Continental Ancestry Group, Immunology, Lupus, Major clinical study, Autoimmune Disease, White People, Article, Hematologic disease, Young Adult, Systemic lupus erythematosus, Rheumatology, Clinical Research, Internal medicine, Genetic screening, Genetics, medicine, Humans, Genetic Predisposition to Disease, American Indian or Alaska Native, Demography, Genetic risk, Inflammation, Lupus erythematosus, Asian, Lupus Erythematosus, business.industry, Inflammatory and immune system, Arthritis, Indians, South American, Systemic, Discoid rash, Odds ratio, medicine.disease, Arthritis & Rheumatology, Onset age, Socioeconomic Factors, Africa, Genetic association, Indians, North American, Morbidity, business

Abstract

Objective American Indian-Europeans, Asians, and African Americans have an excess morbidity from systemic lupus erythematosus (SLE) and a higher prevalence of lupus nephritis than do Caucasians. The aim of this study was to analyze the relationship between genetic ancestry and sociodemographic characteristics and clinical features in a large cohort of American Indian-European SLE patients. Methods A total of 2,116 SLE patients of American Indian-European origin and 4,001 SLE patients of European descent for whom we had clinical data were included in the study. Genotyping of 253 continental ancestry-informative markers was performed on the Illumina platform. Structure and Admixture software were used to determine genetic ancestry proportions of each individual. Logistic regression was used to test the association between genetic ancestry and sociodemographic and clinical characteristics. Odds ratios (ORs) were calculated with 95% confidence intervals (95% CIs). Results The average American Indian genetic ancestry of 2,116 SLE patients was 40.7%. American Indian genetic ancestry conferred increased risks of renal involvement (P less than 0.0001, OR 3.50 [95% CI 2.63- 4.63]) and early age at onset (P less than 0.0001). American Indian ancestry protected against photosensitivity (P less than 0.0001, OR 0.58 [95% CI 0.44-0.76]), oral ulcers (P less than 0.0001, OR 0.55 [95% CI 0.42-0.72]), and serositis (P less than 0.0001, OR 0.56 [95% CI 0.41-0.75]) after adjustment for age, sex, and age at onset. However, age and sex had stronger effects than genetic ancestry on malar rash, discoid rash, arthritis, and neurologic involvement. Conclusion In general, American Indian genetic ancestry correlates with lower sociodemographic status and increases the risk of developing renal involvement and SLE at an earlier age. Copyright © 2012 by the American College of Rheumatology.

Published

2012

25. Analysis of autosomal genes reveals gene–sex interactions and higher total genetic risk in men with systemic lupus erythematosus

Author

Berta Martins da Silva, Anne M. Stevens, Kenneth M. Kaufman, Timothy B. Niewold, Robert P. Kimberly, Javier Martín, Carl D. Langefeld, Gian Domenico Sebastiani, Jeffrey C. Edberg, Mauro Galeazzi, Amr H. Sawalha, Gary S. Gilkeson, Luis M. Vilá, Patrick M. Gaffney, Joan T. Merrill, R. Hal Scofield, Susan A. Boackle, Bruce C. Richardson, Graciela S. Alarcón, Michelle Petri, Rosalind Ramsey-Goldman, Norberto Ortego-Centeno, Carlos Vasconcelos, John D. Reveille, Bernard Lauwerys, Lindsey A. Criswell, Enrique de Ramón, Adam Adler, José Mario Sabio, Timothy J. Vyse, Kathy L. Moser, Elizabeth E. Brown, Torsten Witte, Elena Sánchez, Adrienne H. Williams, Judith A. James, Jennifer A. Kelly, Lennart Truedsson, Travis K. Hughes, José Luis Callejas, Sandra D'Alfonso, Emoke Endreffy, Julio Sánchez-Román, Chaim O. Jacob, María Francisca González-Escribano, Betty P. Tsao, Johan Frostegård, László Kovács, Marta E. Alarcón-Riquelme, Sergio Migliarese, and John B. Harley

Subjects

Male, Genetics and Molecular Biology (all), Genotype, Genetic Linkage, Quantitative Trait Loci, Immunology, Human leukocyte antigen, Polymorphism, Single Nucleotide, Biochemistry, Article, General Biochemistry, Genetics and Molecular Biology, Sex Factors, Rheumatology, Risk Factors, immune system diseases, Genetic linkage, Genetic predisposition, medicine, Lupus Erythematosus, Systemic, Humans, Immunology and Allergy, Genetic Predisposition to Disease, Polymorphism, skin and connective tissue diseases, Genetic association, Lupus erythematosus, Lupus Erythematosus, business.industry, Medicine (all), Systemic, Case-control study, Single Nucleotide, Case-Control Studies, Female, Biochemistry, Genetics and Molecular Biology (all), medicine.disease, Genetic load, business

Abstract

Objectives: Systemic lupus erythematosus (SLE) is a sexually dimorphic autoimmune disease which is more common in women, but affected men often experience a more severe disease. The genetic basis of sexual dimorphism in SLE is not clearly defined. A study was undertaken to examine sex-specific genetic effects among SLE susceptibility loci. Methods: A total of 18 autosomal genetic susceptibility loci for SLE were genotyped in a large set of patients with SLE and controls of European descent, consisting of 5932 female and 1495 male samples. Sex-specific genetic association analyses were performed. The sex-gene interaction was further validated using parametric and non-parametric methods. Aggregate differences in sex-specific genetic risk were examined by calculating a cumulative genetic risk score for SLE in each individual and comparing the average genetic risk between male and female patients. Results: A significantly higher cumulative genetic risk for SLE was observed in men than in women. (P=4.52x10 -8) A significant sex-gene interaction was seen primarily in the human leucocyte antigen (HLA) region but also in IRF5, whereby men with SLE possess a significantly higher frequency of risk alleles than women. The genetic effect observed in KIAA1542 is specific to women with SLE and does not seem to have a role in men. Conclusions: The data indicate that men require a higher cumulative genetic load than women to develop SLE. These observations suggest that sex bias in autoimmunity could be influenced by autosomal genetic susceptibility loci.

Published

2011

26. Identification of novel genetic susceptibility loci in African American lupus patients in a candidate gene association study

Author

Carl D. Langefeld, Luis M. Vilá, Amr H. Sawalha, Gary S. Gilkeson, Michelle Petri, Diane L. Kamen, Joan T. Merrill, Graciela S. Alarcón, Jeffrey C. Edberg, Patrick M. Gaffney, Jennifer A. Kelly, Timothy J. Vyse, Mary E. Comeau, Timothy B. Niewold, Betty P. Tsao, Barry I. Freedman, Elizabeth E. Brown, Robert P. Kimberly, John B. Harley, Kenneth M. Kaufman, Bruce C. Richardson, Elena Sánchez, Marta E. Alarcón-Riquelme, Rosalind Ramsey-Goldman, Chaim O. Jacob, John D. Reveille, and Judith A. James

Subjects

Candidate gene, Genotype, Immunology, Human leukocyte antigen, Biology, FCGR2A, Polymorphism, Single Nucleotide, Article, PTPN22, Rheumatology, immune system diseases, Genetic predisposition, medicine, Humans, Lupus Erythematosus, Systemic, Immunology and Allergy, Genetic Predisposition to Disease, Pharmacology (medical), Allele, skin and connective tissue diseases, Alleles, Genetic Association Studies, Genetic association, Genetics, Systemic lupus erythematosus, medicine.disease, Black or African American, Genetic Loci

Abstract

Objective Candidate gene and genome-wide association studies have identified several disease susceptibility loci in lupus patients. These studies have largely been performed in lupus patients who are Asian or of European ancestry. This study was undertaken to examine whether some of these same susceptibility loci increase lupus risk in African American individuals. Methods Single-nucleotide polymorphisms tagging 15 independent lupus susceptibility loci were genotyped in a set of 1,724 lupus patients and 2,024 healthy controls of African American descent. The loci examined included PTPN22, FCGR2A, TNFSF4, STAT4, CTLA4, PDCD1, PXK, BANK1, MSH5 (HLA region), CFB (HLA region), C8orf13-BLK region, MBL2, KIAA1542, ITGAM, and MECP2/IRAK1. Results We found the first evidence of genetic association between lupus in African American patients and 5 susceptibility loci (C8orf13-BLK, BANK1, TNFSF4, KIAA1542, and CTLA4; P = 8.0 × 10−6, P = 1.9 × 10−5, P = 5.7 × 10−5, P = 0.00099, and P = 0.0045, respectively). Further, we confirmed the genetic association between lupus and 5 additional lupus susceptibility loci (ITGAM, MSH5, CFB, STAT4, and FCGR2A; P = 7.5 × 10−11, P = 5.2 × 10−8, P = 8.7 × 10−7, P = 0.0058, and P = 0.0070, respectively), and provided evidence, for the first time, of genome-wide significance for the association between lupus in African American patients and ITGAM and MSH5 (HLA region). Conclusion These findings provide evidence of novel genetic susceptibility loci for lupus in African Americans and demonstrate that the majority of lupus susceptibility loci examined confer lupus risk across multiple ethnicities.

Published

2011

27. Association of a functional IRF7 variant with systemic lupus erythematosus

Author

Jonathan L. Wong, Jian Zhao, Betty P. Tsao, Xiaoxia Qian, Soo-Kyung Cho, Sang Cheol Bae, Nan Shen, Frank C. Arnett, Joel M Guthridge, Mo Yin Mok, Bevra H. Hahn, Yeong Wook Song, Hwee Siew Howe, C. Yung Yu, Jennifer M. Grossman, Kenneth M. Kaufman, John B. Harley, and Qiong Fu

Subjects

Adult, Male, Genotype, Interferon Regulatory Factor-7, Molecular Sequence Data, Immunology, Population, Genome-wide association study, Biology, Polymorphism, Single Nucleotide, Article, White People, Asian People, Rheumatology, Risk Factors, Polymorphism (computer science), Ethnicity, medicine, Humans, Lupus Erythematosus, Systemic, Immunology and Allergy, SNP, Genetic Predisposition to Disease, Pharmacology (medical), Amino Acid Sequence, Allele, education, education.field_of_study, Lupus erythematosus, Genetic Variation, Odds ratio, medicine.disease, Black or African American, Female, Genome-Wide Association Study

Abstract

Objective A previous genome-wide association study conducted in a population of European ancestry identified rs4963128, a KIAA1542 single-nucleotide polymorphism (SNP) 23 kb telomeric to IRF7 (the gene for interferon regulatory factor 7 [IRF-7]), to be strongly associated with systemic lupus erythematosus (SLE). This study was undertaken to investigate whether genetic polymorphism within IRF7 is a risk factor for the development of SLE. Methods We genotyped one KIAA1542 SNP (rs4963128) and one IRF7 SNP (rs1131665 [Q412R]) in an Asian population (1,302 cases, 1,479 controls), to assess their association with SLE. Subsequently, rs1131665 was further genotyped in independent panels of Chinese subjects (528 cases, 527 controls), European American subjects (446 cases, 461 controls), and African American subjects (159 cases, 115 controls) by TaqMan genotyping assay, to seek confirmation of association in various ethnic groups. A luciferase reporter assay was used to assess the effect of Q412R polymorphism on the activation of IRF-7. Results Consistent association of rs1131665 (Q412R) with SLE was identified in Asian, European American, and African American populations (total 2,435 cases and 2,582 controls) (Pmeta = 6.18 × 10−6, odds ratio 1.42 [95% confidence interval 1.22–1.65]). Expression of the IRF7 412Q risk allele resulted in a 2-fold increase in interferon-stimulated response element transcriptional activity compared with expression of IRF7 412R (P = 0.0003), suggesting that IRF7 412Q confers elevated IRF-7 activity and may therefore affect a downstream interferon pathway. Conclusion These findings show that the major allele of a nonsynonymous SNP, rs1131665 (412Q) in IRF7, confers elevated activation of IRF-7 and predisposes to the development of SLE in multiple ethnic groups. This result provides direct genetic evidence that IRF7 may be a risk gene for human SLE.

Published

2011

28. Identification of a Systemic Lupus Erythematosus Susceptibility Locus at 11p13 between PDHX and CD44 in a Multiethnic Study

Author

Yeong Wook Song, So-Yeon Park, Chaim O. Jacob, John B. Harley, Patrick M. Gaffney, Betty P. Tsao, John D. Reveille, Gary S. Gilkeson, Elizabeth E. Brown, Juan-Manuel Anaya, Indra Adrianto, Lindsey A. Criswell, Diane L. Kamen, Caroline J. Gallant, Adrienne H. Williams, Carl D. Langefeld, Susan A. Boackle, Rosalind Ramsey-Goldman, Kenneth M. Kaufman, Anne M. Stevens, Kiely Grundahl, Joan T. Merrill, R. Hal Scofield, Deh Ming Chang, Kathy L. Moser, Gail R. Bruner, Judith A. James, Luis M. Vilá, Timothy J. Vyse, Bernardo A. Pons-Estel, Timothy B. Niewold, Christopher J. Lessard, Barry I. Freedman, Javier Martin, Chack-Yung Yu, Jeffrey C. Edberg, Adam Adler, Sang Cheol Bae, Joel M. Guthridge, Peter K. Gregersen, Courtney G. Montgomery, Jennifer A. Kelly, Michelle Petri, and Robert P. Kimberly

Subjects

Male, Linkage disequilibrium, Pyruvate Dehydrogenase Complex, Locus (genetics), Single-nucleotide polymorphism, Biology, Polymorphism, Single Nucleotide, Linkage Disequilibrium, White People, Genetic determinism, Cohort Studies, Asian People, Report, medicine, Genetic predisposition, Genetics, Humans, Lupus Erythematosus, Systemic, Genetic Predisposition to Disease, Genetics(clinical), American Indian or Alaska Native, Genetics (clinical), Genetic association, Lupus erythematosus, Chromosomes, Human, Pair 11, Haplotype, Hispanic or Latino, medicine.disease, Black or African American, Hyaluronan Receptors, Haplotypes, Genetic Loci, Immunology, Female

Abstract

Systemic lupus erythematosus (SLE) is considered to be the prototypic autoimmune disease, with a complex genetic architecture influenced by environmental factors. We sought to replicate a putative association at 11p13 not yet exceeding genome-wide significance (p < 5 × 10-8) identified in a genome-wide association study (GWAS). Our GWA scan identified two intergenic SNPs located between PDHX and CD44 showing suggestive evidence of association with SLE in cases of European descent (rs2732552, p = 0.004, odds ratio [OR] = 0.78; rs387619, p = 0.003, OR = 0.78). The replication cohort consisted of >15,000 subjects, including 3562 SLE cases and 3491 controls of European ancestry, 1527 cases and 1811 controls of African American (AA) descent, and 1265 cases and 1260 controls of Asian origin. We observed robust association at both rs2732552 (p = 9.03 × 10-8, OR = 0.83) and rs387619 (p = 7.7 × 10-7, OR = 0.83) in the European samples with pmeta = 1.82 × 10-9 for rs2732552. The AA and Asian SLE cases also demonstrated association at rs2732552 (p = 5 × 10-3, OR = 0.81 and p = 4.3 × 10-4, OR = 0.80, respectively). A meta-analysis of rs2732552 for all racial and ethnic groups studied produced pmeta = 2.36 × 10-13. This locus contains multiple regulatory sites that could potentially affect expression and functions of CD44, a cell-surface glycoprotein influencing immunologic, inflammatory, and oncologic phenotypes, or PDHX, a subunit of the pyruvate dehydrogenase complex. © 2011 The American Society of Human Genetics.

Published

2011

29. Genetically determined Amerindian ancestry correlates with increased frequency of risk alleles for systemic lupus erythematosus

Author

Ignacio García-De La Torre, Mercedes A. García, Carlos Vasconcelos, Ryan Webb, Elena Sánchez, John B. Harley, Kenneth M. Kaufman, Mario H. Cardiel-Rios, Laura Riba, Bruce Richardson, Bernardo A. Pons-Estel, José Francisco Moctezuma, Jennifer A. Kelly, Amr H. Sawalha, Marco A. Maradiaga-Ceceña, Marta E. Alarcón-Riquelme, Eduardo Acevedo, Susana Gamron, Mariano Cucho-Venegas, Astrid Rasmussen, Teresa Tusié-Luna, and Javier Martín

Subjects

Genetics, Systemic lupus erythematosus, Lupus erythematosus, Immunology, Case-control study, Single-nucleotide polymorphism, Biology, medicine.disease, Rheumatology, immune system diseases, Polymorphism (computer science), Genetic predisposition, medicine, Immunology and Allergy, Pharmacology (medical), skin and connective tissue diseases, Allele frequency, Genetic association

Abstract

Objective To assess whether genetically determined Amerindian ancestry predicts increased presence of risk alleles of known susceptibility genes for systemic lupus erythematosus (SLE). Methods Single-nucleotide polymorphisms (SNPs) within 16 confirmed genetic susceptibility loci for SLE were genotyped in a set of 804 Mestizo lupus patients and 667 Mestizo healthy controls. In addition, 347 admixture informative markers were genotyped. Individual ancestry proportions were determined using STRUCTURE. Association analysis was performed using PLINK, and correlation between ancestry and the presence of risk alleles was analyzed using linear regression. Results A meta-analysis of the genetic association of the 16 SNPs across populations showed that TNFSF4, STAT4, ITGAM, and IRF5 were associated with lupus in a Hispanic Mestizo cohort enriched for European and Amerindian ancestry. In addition, 2 SNPs within the major histocompatibility complex region, previously shown to be associated in a genome-wide association study in Europeans, were also associated in Mestizos. Using linear regression, we predicted an average increase of 2.34 risk alleles when comparing an SLE patient with 100% Amerindian ancestry versus an SLE patient with 0% Amerindian ancestry (P < 0.0001). SLE patients with 43% more Amerindian ancestry were predicted to carry 1 additional risk allele. Conclusion Our results demonstrate that Amerindian ancestry is associated with an increased number of risk alleles for SLE.

Published

2010

30. Early disease onset is predicted by a higher genetic risk for lupus and is associated with a more severe phenotype in lupus patients

Author

Elena Sánchez, Amr H. Sawalha, Swapan K. Nath, Marta E. Alarcón-Riquelme, Kenneth M. Kaufman, Ryan Webb, Diane L. Kamen, Travis K. Hughes, Gail R. Bruner, Gary S. Gilkeson, Bruce C. Richardson, Jennifer A. Kelly, John B. Harley, and Emily C. Somers

Subjects

Adult, Male, Adolescent, Genotype, Immunology, Disease, Polymorphism, Single Nucleotide, Article, General Biochemistry, Genetics and Molecular Biology, Young Adult, Rheumatology, immune system diseases, Genetic predisposition, Humans, Lupus Erythematosus, Systemic, Immunology and Allergy, Medicine, Genetic Predisposition to Disease, Age of Onset, Risk factor, Child, skin and connective tissue diseases, Lupus erythematosus, Systemic lupus erythematosus, business.industry, Oklahoma, Middle Aged, Prognosis, medicine.disease, Connective tissue disease, Phenotype, Female, medicine.symptom, Age of onset, Epidemiologic Methods, business, Malar rash

Abstract

Systemic lupus erythematosus (SLE) is a chronic, multiorgan, autoimmune disease that affects people of all ages and ethnicities.To explore the relationship between age at disease onset and many of the diverse manifestations of SLE. Additionally, to determine the relationship between age of disease onset and genetic risk in patients with SLE.The relationship between the age at disease onset and SLE manifestations were explored in a multi-racial cohort of 1317 patients. Patients with SLE were genotyped across 19 confirmed genetic susceptibility loci for SLE. Logistic regression was used to determine the relationships between the number of risk alleles present and age of disease onset.Childhood-onset SLE had higher odds of proteinuria, malar rash, anti-dsDNA antibody, haemolytic anaemia, arthritis and leucopenia (OR=3.03, 2.13, 2.08, 2.50, 1.89, 1.53, respectively; p values0.0001, 0.0004, 0.0005, 0.0024, 0.0114, 0.045, respectively). In female subjects, the odds of having cellular casts were 2.18 times higher in childhood-onset than in adult-onset SLE (p=0.0027). With age of onset ≥50, the odds of having proteinuria, cellular casts, anti-nRNP antibody, anti-Sm antibody, anti-dsDNA antibody and seizures were reduced. However, late adult-onset patients with SLE have higher odds of developing photosensitivity than early adult-onset patients. Each SLE-susceptibility risk allele carried within the genome of patients with SLE increased the odds of having a childhood-onset disease in a race-specific manner: by an average of 48% in Gullah and 25% in African-Americans, but this was not significant in Hispanic and European-American lupus patients.The genetic contribution towards predicting early-onset disease in patients with SLE is quantified for the first time. A more severe SLE phenotype is found in patients with early-onset disease in a large multi-racial cohort, independent of gender, race and disease duration.

Published

2010

31. X chromosomal linkage to eosinophilic esophagitis susceptibility

Author

Ting Wen, Avery Maddox, Robert M. Genta, Simon P. Hogan, Phillip J. Dexheimer, Carmey Forney, Pablo Abonia, Kenneth M. Kaufman, Philip E. Putnam, Kate Hoffman, Michael D. Eby, Tetsuo Shoda, Mark Rochman, Vincent A. Mukkada, Marc E. Rothenberg, Evan S. Dellon, Nina Lukac, Leanne Ray, Melissa K. Mingler, Leah C. Kottyan, Justin C. Wheeler, Julie M. Caldwell, and Lisa J. Martin

Subjects

Linkage (software), Genetics, Immunology, medicine, Immunology and Allergy, Biology, Eosinophilic esophagitis, medicine.disease

Published

2018

32. Regulatory Variants of ATF3, CDH17 and FAM71A are Risk Factors for Diisocyanate Induced Occupational Asthma (DA)

Author

María Jesús Cruz, Jianbo Yao, Daniel Miller, Kenneth M. Kaufman, Joaquín Sastre, Susan M. Tarlo, David I. Bernstein, Xavier Muñoz, André Cartier, Catherine Lemière, Santiago Quirce, Banu Kesavalu, Matthew T. Weirauch, Zana L. Lummus, and Leah C. Kottyan

Subjects

business.industry, Immunology, Immunology and Allergy, Medicine, business, medicine.disease, Occupational asthma

Published

2018

33. Reactivity with dichotomous determinants of Ro 60 stratifies autoantibody responses in lupus and primary Sjögren's syndrome

Author

Anthony W. Purcell, Shannon E. Osborne, Nadine L. Dudek, Joanne H. Reed, Tom P. Gordon, Kenneth M. Kaufman, and Michael W. Jackson

Subjects

Immunology, Cross Reactions, Autoantigens, Protein Structure, Secondary, Epitope, Immune tolerance, Flow cytometry, Jurkat Cells, Rheumatology, RNA, Small Cytoplasmic, medicine, Humans, Lupus Erythematosus, Systemic, Immunology and Allergy, Pharmacology (medical), B cell, Autoantibodies, Lupus erythematosus, Systemic lupus erythematosus, medicine.diagnostic_test, Immunodominant Epitopes, Chemistry, Autoantibody, Flow Cytometry, medicine.disease, Molecular biology, Protein Structure, Tertiary, Sjogren's Syndrome, medicine.anatomical_structure, Epitope mapping, Ribonucleoproteins, Immunoglobulin G, Epitope Mapping

Abstract

Objective Analysis of B cell determinants of Ro 60 exposed on the surface of apoptotic cells (apotopes) or intracellular epitopes provides insight into the structural forms of the autoantigen that break immune tolerance. This study was initiated to compare anti–Ro 60 responses in systemic lupus erythematosus (SLE) and primary Sjogren's syndrome (SS) against membrane-bound and intracellular forms of Ro 60. Methods The reactivity of autoantibodies from patients with SLE and primary SS to Ro 60 apotopes and epitopes was assessed by multiparameter flow cytometry and solid-phase immunoassay. Anti–Ro 60 IgG was eluted from early apoptotic cells or recombinant Ro 60 immobilized on nitrocellulose, and binding to membrane-bound and intracellular forms of Ro 60 was quantitated by flow cytometry. Results An immunodominant apotope, which was recognized by IgG from a subset of SLE patients with anti-Ro, but not anti-La, autoantibodies, was mapped to a region forming a helix-loop-helix at the apical tip of the Ro 60 molecule. Immobilization of this region to the solid phase exposed an epitope that was recognized by IgG from primary SS and SLE patients whose sera had both anti-Ro and anti-La autoantibodies. Autoantibodies eluted from either the surface of apoptotic cells or the Ro 60 epitope on the solid phase were non–cross-reactive and specifically recognized membrane-bound or cytoplasmic forms of Ro 60. Conclusion This is the first example of a dichotomy of human autoantibody responses against mutually exclusive determinants linked to a single domain of a systemic autoantigen and supports a model in which tolerance is broken by different immunogenic forms of Ro 60.

Published

2010

34. A polymorphism withinIL21Rconfers risk for systemic lupus erythematosus

Author

Rosalind Ramsey-Goldman, Marta E. Alarcón-Riquelme, Robert P. Kimberly, Judith A. James, Amr H. Sawalha, Peter E. Lipsky, Swapan K. Nath, Joan T. Merrill, Carl D. Langefeld, TJ Vyse, Kathy L. Moser, Gary S. Gilkeson, Luis M. Vilá, Ryan Webb, Graciela S. Alarcón, Jennifer A. Kelly, Michelle Petri, Jeffrey C. Edberg, Kenneth M. Kaufman, Julie T. Ziegler, John B. Harley, John D. Reveille, Andrea L. Sestak, Chaim O. Jacob, and Patrick M. Gaffney

Subjects

Male, Immunology, Single-nucleotide polymorphism, Polymorphism, Single Nucleotide, Linkage Disequilibrium, White People, Article, Rheumatology, Risk Factors, immune system diseases, Immunopathology, Plasma cell differentiation, medicine, Humans, Lupus Erythematosus, Systemic, Immunology and Allergy, Genetic Predisposition to Disease, Pharmacology (medical), skin and connective tissue diseases, Systemic lupus erythematosus, Lupus erythematosus, biology, business.industry, Interleukin-21 Receptor alpha Subunit, Hispanic or Latino, Odds ratio, medicine.disease, Interleukin-21 receptor, biology.protein, Female, Antibody, business

Abstract

OBJECTIVE: Interleukin-21 (IL-21) is a member of the type I cytokine superfamily that has a variety of effects on the immune system, including B cell activation, plasma cell differentiation, and immunoglobulin production. The expression of IL-21 receptor (IL-21R) is reduced in the B cells of patients with systemic lupus erythematosus (SLE), while serum IL-21 levels are increased both in lupus patients and in some murine lupus models. We recently reported that polymorphisms within the IL21 gene are associated with increased susceptibility to SLE. The aim of this study was to examine the genetic association between single-nucleotide polymorphisms (SNPs) within IL21R and SLE. METHODS: We genotyped 17 SNPs in the IL21R gene in 2 large cohorts of lupus patients (a European-derived cohort and a Hispanic cohort) and in ethnically matched healthy controls. RESULTS: We identified and confirmed the association between rs3093301 within the IL21R gene and SLE in the 2 cohorts (meta-analysis odds ratio 1.16 [95% confidence interval 1.08-1.25], P=1.0x10(-4)). CONCLUSION: Our findings indicate that IL21R is a novel susceptibility gene for SLE.

Published

2009

35. Evaluation of C1q genomic region in minority racial groups of lupus

Author

Joan T. Merrill, Jasmin Divers, Andrea L. Sestak, Chaim O. Jacob, Gary S. Gilkeson, Courtney Gray-McGuire, Judith A. James, John B. Harley, Carl D. Langefeld, Edward K. Wakeland, Bahram Namjou, Jennifer A. Kelly, Kenneth M. Kaufman, Julie T. Ziegler, Kathy L. Moser, and Quan Zhen Li

Subjects

Immunology, Single-nucleotide polymorphism, Biology, Polymorphism, Single Nucleotide, Article, immune system diseases, Genetics, medicine, Humans, Lupus Erythematosus, Systemic, SNP, Genetic Predisposition to Disease, skin and connective tissue diseases, Gene, Genetics (clinical), Systemic lupus erythematosus, Complement C1q, Oklahoma, Hispanic or Latino, medicine.disease, Lupus Nephritis, Phenotype, Complement system, Black or African American, Cohort, Nephritis

Abstract

Complement cascade plasma proteins play a complex role in the etiopathogenesis of systemic lupus erythematosus (SLE). Hereditary C1q deficiency has been strongly related to SLE; however, there are very few published SLE studies that evaluate the polymorphisms of genes encoding for C1q (A, B and C). In this study, we evaluated 17 single nucleotide polymorphisms (SNPs) across 37 kb of C1QA, C1QB and C1QC in a lupus cohort of individuals of the African-American and Hispanic origin. In a case-only analysis, a significant association at multiple SNPs in the C1QA gene was detected in African Americans with kidney nephritis (best P=4.91 x 10(-6)). In addition, C1QA was associated with SLE in African Americans with a lack of nephritis and accompanying photosensitivity when compared with that in normal controls (P=6.80 x 10(-6)). A similar trend was observed in the Hispanic subjects (P=0.003). Quantitative analysis showed that some SNPs in C1q genes might be correlated with C3 complement levels in an additive model among African Americans (best P=0.0001). The C1QA gene is associated with subphenotypes of lupus in the African-American and Hispanic subjects. Further studies with higher SNP densities in this region and other complement components are necessary to elucidate the complex genetics and phenotypic interactions between complement components and SLE.

Published

2009

36. Meta-analysis and imputation identifies a 109 kb risk haplotype spanning TNFAIP3 associated with lupus nephritis and hematologic manifestations

Author

Patrick M. Gaffney, Mary Beth Humphrey, Judith A. James, Courtney Gray-McGuire, Justin Rodgers, Jennifer A. Kelly, Gary S. Gilkeson, Laura J. Battiest, Jared S. Bates, Kathy L. Moser, Kenneth M. Kaufman, Christopher J. Lessard, Thuan Nguyen, John B. Harley, and Joanlise M. Leon

Subjects

Immunology, Lupus nephritis, imputation, Single-nucleotide polymorphism, Genome-wide association study, Biology, Polymorphism, Single Nucleotide, Article, 03 medical and health sciences, 0302 clinical medicine, systemic lupus erythematosus, Genotype, Genetics, medicine, International HapMap Project, skin and connective tissue diseases, TNFAIP3, Tumor Necrosis Factor alpha-Induced Protein 3, Genetics (clinical), 030304 developmental biology, 0303 health sciences, Haplotype, Intracellular Signaling Peptides and Proteins, Nuclear Proteins, Odds ratio, medicine.disease, Lupus Nephritis, 3. Good health, meta-analysis, DNA-Binding Proteins, Haplotypes, Imputation (genetics), Genome-Wide Association Study, 030215 immunology

Abstract

TNFAIP3 encodes the ubiquitin-modifying enzyme, A20, a key regulator of inflammatory signaling pathways. We previously reported association between TNFAIP3 variants and systemic lupus erythematosus (SLE). To further localize the risk variant(s), we performed a meta-analysis using genetic data available from two Caucasian case-control datasets (1453 total cases, 3381 total control subjects) and 713 SLE trio families. The best result was found at rs5029939 (P=1.67 x 10(-14), odds ratio=2.09, 95% confidence interval 1.68-2.60). We then imputed single nucleotide polymorphisms (SNPs) from the CEU Phase II HapMap using genotypes from 431 SLE cases and 2155 control subjects. Imputation identified 11 SNPs in addition to three observed SNPs, which together, defined a 109 kb SLE risk segment surrounding TNFAIP3. When evaluating whether the rs5029939 risk allele was associated with SLE clinical manifestations, we observed that heterozygous carriers of the TNFAIP3 risk allele at rs5029939 have a twofold increased risk of developing renal or hematologic manifestations compared to homozygous non-risk subjects. In summary, our study strengthens the genetic evidence that variants in the region of TNFAIP3 influence risk for SLE, particularly in patients with renal and hematologic manifestations, and narrows the risk effect to a 109 kb DNA segment that spans the TNFAIP3 gene.

Published

2009

37. Variants withinMECP2, a key transcription regulator, are associated with increased susceptibility to lupus and differential gene expression in patients with systemic lupus erythematosus

Author

Rosalind Ramsey-Goldman, Judith A. James, Jonathan D. Wren, Gary S. Gilkeson, Jennifer A. Kelly, Michelle Petri, Jeffrey C. Edberg, Amr H. Sawalha, Luis M. Vilá, Patrick M. Gaffney, John B. Harley, Ryan Webb, Kenneth M. Kaufman, Graciela S. Alarcón, Yuhong Tang, Robert P. Kimberly, Kathy L. Moser, Timothy J. Vyse, Marta E. Alarcón-Riquelme, John D. Reveille, Mark Barton Frank, Matlock A. Jeffries, and Joan T. Merrill

Subjects

Genetics, congenital, hereditary, and neonatal diseases and abnormalities, Systemic lupus erythematosus, Immunology, Haplotype, Single-nucleotide polymorphism, Promoter, Locus (genetics), Biology, medicine.disease, nervous system diseases, MECP2, Rheumatology, mental disorders, biology.protein, medicine, Immunology and Allergy, Pharmacology (medical), CREB1, Gene

Abstract

Objective Both genetic and epigenetic factors play an important role in the pathogenesis of lupus. The aim of this study was to examine methyl-CpG–binding protein 2 gene (MECP2) polymorphisms in a large cohort of patients with lupus and control subjects, and to determine the functional consequences of the lupus-associated MECP2 haplotype. Methods We genotyped 18 single-nucleotide polymorphisms within MECP2, located on chromosome Xq28, in a large cohort of patients with lupus and control subjects of European descent. We studied the functional effects of the lupus-associated MECP2 haplotype by determining gene expression profiles in B cell lines in female lupus patients with and those without the lupus-associated MECP2 risk haplotype. Results We confirmed, replicated, and extended the genetic association between lupus and genetic markers within MECP2 in a large independent cohort of lupus patients and control subjects of European descent (odds ratio 1.35, P = 6.65 × 10−11). MECP2 is a dichotomous transcription regulator that either activates or represses gene expression. We identified 128 genes that are differentially expressed in lupus patients with the disease-associated MECP2 haplotype; most (∼81%) were up-regulated. Genes that were up-regulated had significantly more CpG islands in their promoter regions compared with genes that were down-regulated. Gene ontology analysis using the differentially expressed genes revealed significant association with epigenetic regulatory mechanisms, suggesting that these genes are targets for MECP2 regulation in B cells. Furthermore, at least 13 of the 104 up-regulated genes are regulated by interferon. The disease-risk MECP2 haplotype was associated with increased expression of the MECP2 transcription coactivator CREB1 and decreased expression of the corepressor histone deacetylase 1. Conclusion Polymorphism in the MECP2 locus is associated with lupus and, at least in part, contributes to the interferon signature observed in lupus patients.

Published

2009

38. Genetic association of interleukin-21 polymorphisms with systemic lupus erythematosus

Author

Amy E. Wandstrat, Edward K. Wakeland, Kenneth M. Kaufman, David S Karp, Adam Adler, Jeff Kilpatrick, Judith A. James, Quan Zhen Li, Jennifer A. Kelly, Amr H. Sawalha, John B. Harley, Teresa Aberle, Joan T. Merrill, and Peter E. Lipsky

Subjects

Male, Candidate gene, Genotype, Immunology, Population, Single-nucleotide polymorphism, Polymorphism, Single Nucleotide, White People, General Biochemistry, Genetics and Molecular Biology, Gene Frequency, Rheumatology, medicine, Humans, Lupus Erythematosus, Systemic, Immunology and Allergy, Genetic Predisposition to Disease, Allele, education, Genetic association, Genetics, education.field_of_study, Lupus erythematosus, business.industry, Interleukins, Haplotype, medicine.disease, Black or African American, Haplotypes, Case-Control Studies, Female, business

Abstract

Objective:The aetiology of systemic lupus erythematosus (SLE) is incompletely understood. Both genetic and environmental factors are implicated in the pathogenesis of the disease. Herein, we describe genetic association between SLE and polymorphisms in the interleukin (IL)-21 gene. The reported effect of IL-21 on B-cell differentiation into plasma cells and its effect on dendritic cell maturation and T-cell responses make IL-21 an attractive candidate gene for SLE.Methods:Three single nucleotide polymorphisms (SNPs) in the IL-21 gene were genotyped in a total of 2636 individuals (1318 cases and 1318 controls matched for age, sex and race). Population-based case–control association analyses were performed.Results:We found a genetic association with SLE and two SNPs located within the IL-21 gene (rs907715: χ2 = 11.55, p2 = 5.49, p = 0.019). Furthermore, genotypes homozygous for the risk alleles were more frequent than genotypes homozygous for the non-risk alleles in European–American patients as compared to controls (rs907715 (GG versus AA): odds ratio (OR) = 1.66, p = 0.0049; rs2221903 (GG versus AA): OR = 1.60, p = 0.025).Conclusion:Our findings indicate that IL-21 polymorphism is a candidate association with SLE. The functional effects of this association, when revealed, might improve our understanding of the disease and provide new therapeutic targets.

Published

2007

39. X Chromosome Dose and Sex Bias in Autoimmune Diseases: Increased 47,XXX in Systemic Lupus Erythematosus and Sjögren's Syndrome

Author

Daniel J. Wallace, Wan-Fai Ng, Carrie A. Weaver, Maureen Rischmueller, Marie Wahren-Herlenius, Michael T. Brennan, Gideon M. Hirschfield, Christopher I. Amos, James Chodosh, Michael D. Rohrer, Susan D. Thompson, Katherine A. Siminovitch, Jeffrey C. Edberg, Torsten Witte, Timothy J. Vyse, Barbara M. Segal, Courtney G. Montgomery, Gunnel Nordmark, Valerie M. Harris, Jacen S. Maier-Moore, Judith A. James, Gabor G. Illei, Juan-Manuel Anaya, Tammy O. Utset, Lida Radfar, Ke Liu, Marta E. Alarcón-Riquelme, Diane L. Kamen, W. Joseph McCune, Roald Omdal, Pamela J. Hughes, Kristi A. Koelsch, Corinne Miceli-Richard, Patrick M. Gaffney, Vivian P. Bykerk, Per Eriksson, James A. Lessard, Edward C. Keystone, John B. Harley, Biji T. Kurien, Rajaram Gopalakrishnan, Jennifer A. Kelly, Robert P. Kimberly, Xianglan Lu, Adam Adler, Leah C. Kottyan, Erwin P. Bottinger, Graciela S. Alarcón, Betty P. Tsao, Sara Lazaro, Kenneth M. Kaufman, Joel M. Guthridge, Kathy L. Sivils, C. Langefeld, Michael H. Weisman, Diana H. Taft, Jay Kumar, Joan T. Merrill, R. Hal Scofield, Shibo Li, Nelson L. Rhodus, Xavier Mariette, Jacques-Eric Gottenberg, Gang Xie, Mitali Talsania, Ann Igoe, Christopher J. Lessard, Sarah L. Zimmerman, Bernardo A. Pons-Estel, Gary S. Gilkeson, Roland Jonsson, John A. Ice, Donald U. Stone, Deborah S. Cunninghame-Graham, Jane E. Salmon, Andrew J.W. Huang, David M Lewis, and Astrid Rasmussen

Subjects

medicine.medical_specialty, Sarcoidosis, Sex Chromosome Disorders of Sex Development, Immunology, Gene Dosage, Trisomy, medicine.disease_cause, Gastroenterology, Article, Autoimmune Diseases, Autoimmunity, Arthritis, Rheumatoid, Primary biliary cirrhosis, Rheumatology, Internal medicine, Prevalence, medicine, Humans, Lupus Erythematosus, Systemic, Immunology and Allergy, Sex Distribution, In Situ Hybridization, Fluorescence, Sex Chromosome Aberrations, Chromosomes, Human, X, Lupus erythematosus, Liver Cirrhosis, Biliary, business.industry, Case-control study, Odds ratio, medicine.disease, 3. Good health, Sjogren's Syndrome, Case-Control Studies, Rheumatoid arthritis, Female, business, Anti-SSA/Ro autoantibodies

Abstract

Objective More than 80% of autoimmune disease predominantly affects females, but the mechanism for this female bias is poorly understood. We suspected that an X chromosome dose effect accounts for this, and we undertook this study to test our hypothesis that trisomy X (47,XXX; occurring in ∼1 in 1,000 live female births) would be increased in patients with female-predominant diseases (systemic lupus erythematosus [SLE], primary Sjogren's syndrome [SS], primary biliary cirrhosis, and rheumatoid arthritis [RA]) compared to patients with diseases without female predominance (sarcoidosis) and compared to controls. Methods All subjects in this study were female. We identified subjects with 47,XXX using aggregate data from single-nucleotide polymorphism arrays, and, when possible, we confirmed the presence of 47,XXX using fluorescence in situ hybridization or quantitative polymerase chain reaction. Results We found 47,XXX in 7 of 2,826 SLE patients and in 3 of 1,033 SS patients, but in only 2 of 7,074 controls (odds ratio in the SLE and primary SS groups 8.78 [95% confidence interval 1.67–86.79], P = 0.003 and odds ratio 10.29 [95% confidence interval 1.18–123.47], P = 0.02, respectively). One in 404 women with SLE and 1 in 344 women with SS had 47,XXX. There was an excess of 47,XXX among SLE and SS patients. Conclusion The estimated prevalence of SLE and SS in women with 47,XXX was ∼2.5 and ∼2.9 times higher, respectively, than that in women with 46,XX and ∼25 and ∼41 times higher, respectively, than that in men with 46,XY. No statistically significant increase of 47,XXX was observed in other female-biased diseases (primary biliary cirrhosis or RA), supporting the idea of multiple pathways to sex bias in autoimmunity.

Published

2015

40. Unraveling the genetics of systemic lupus erythematosus

Author

Kenneth M. Kaufman, John B. Harley, and Jennifer A. Kelly

Subjects

Genetic Markers, Genetics, Polymorphism, Genetic, Systemic lupus erythematosus, Lupus erythematosus, Genetic Linkage, Genome, Human, Immunology, Family aggregation, General Medicine, Biology, medicine.disease, Twin study, immune system diseases, Genetic linkage, Genetic marker, medicine, Animals, Humans, Lupus Erythematosus, Systemic, Genetic Predisposition to Disease, Human genome, skin and connective tissue diseases, Genetic association

Abstract

The capacity to locate polymorphisms on a virtually complete map of the human genome coupled with the ability to accurately evaluate large numbers (by historical standards) of genetic markers has led to gene identification in complex diseases, such as systemic lupus erythematosus (SLE or lupus). While this is a phenotype with enormous clinical variation, the twin studies and the observed familial aggregation, along with the genetic effects now known, suggest a strong genetic component. Unlike type 1 diabetes, lupus genetics is not dominated by the powerful effect of a single locus. Instead, there are at least six known genetic association effects in lupus of smaller magnitude (odds ratio2), and at least 17 robust linkages (established and arguably confirmed independently) defining potentially responsible genes that largely remain to be discovered. The more convincing genetic associations include the human leukocyte antigen region (with multiple genes), C1q, PTPN22, PDCD1, Fc receptor-like 3, FcgammaRIIA, FcgammaRIIIA, interferon regulatory factor 5, and others. How they contribute to disease risk remains yet to be clarified, beyond the obvious speculation derived from what has previously been learned about these genes. Certainly, they are expected to contribute to lupus risk independently and in combination with each other, with genes not yet identified, and with the environment. A substantial number of genes (10) are expected to be identified to contribute to lupus or in its many subsets defined by clinical and laboratory features.

Published

2006

41. Proteasome degradation of GRK2 during ischemia and ventricular tachyarrhythmias in a canine model of myocardial infarction

Author

David C. Kem, Kenneth M. Kaufman, Xichun Yu, Eugene Patterson, Samuel T. Dunn, Jordan P. Metcalf, Meili Zhu, Shijun Huang, and Marion W. Garrett

Subjects

G-Protein-Coupled Receptor Kinase 5, Male, Tachycardia, Proteasome Endopeptidase Complex, medicine.medical_specialty, Physiology, Immunoblotting, Myocardial Infarction, Myocardial Ischemia, Ischemia, Protein Serine-Threonine Kinases, Sudden death, Sudden cardiac death, Bortezomib, Electrocardiography, Dogs, Physiology (medical), Internal medicine, Animals, Medicine, Myocardial infarction, Ligation, Cardioprotection, Microscopy, Confocal, medicine.diagnostic_test, Reverse Transcriptase Polymerase Chain Reaction, business.industry, Myocardium, medicine.disease, Boronic Acids, Death, Sudden, Cardiac, Endocrinology, Microscopy, Fluorescence, Pyrazines, Circulatory system, Tachycardia, Ventricular, medicine.symptom, Cardiology and Cardiovascular Medicine, business, Pericardium

Abstract

Arrhythmia-prone subepicardial border zone (EBZ) tissue demonstrates decreased G protein receptor kinase 2 (GRK2) activity and increased sensitivity to isoproterenol 6–24 h after coronary artery ligation (CAL) in the dog. With the use of a semiquantitative immunofluorescence technique, the relative fluorescence intensity (RF) of GRK2 in EBZ decreased to 24% of that in a remote site (RS) ( P < 0.01, n = 30 cells from 3 dogs), whereas GRK5 RF did not change. Confocal studies of cardiac tissue from transgenic mice overexpressing GRK2 validated the use of a semilogarithmic relationship between RF and GRK2 activity. As shown with the use of quantitative real-time RT-PCR, both GRK2 and GRK5 mRNA were not decreased at 24 h in EBZ ( n = 6 dogs) relative to RS control, indicating that the decrease of GRK2 in the EBZ is likely due to posttranscriptional degradation following CAL. Pretreatment of six dogs with the selective proteasome inhibitor bortezomib provided 100% (EBZ) and 50% (infarct) protection against loss of GRK2 at 24 h. There was an absence of rapid (>300 beats/min) and very rapid (>360 beats/min) ventricular triplets that are highly predictive of sudden cardiac death during ECG monitoring in the bortezomib-pretreated animals in contrast to nonpretreated infarcted animals. We have demonstrated that the dramatic decrease in GRK2 in cardiac ischemic tissue can be largely blocked by prior proteasome blockade and that this is associated with significant cardioprotection against malignant ventricular tachyarrhythmias.

Published

2005

42. Structural availability influences the capacity of autoantigenic epitopes to induce a widespread lupus-like autoimmune response

Author

Micah T. McClain, Carol S. Lutz, Kenneth M. Kaufman, Judith A. James, Timothy Gross, and Ofer Z. Faig

Subjects

Molecular Sequence Data, Autoimmunity, Biology, Autoantigens, snRNP Core Proteins, Epitope, Ribonucleoprotein, U1 Small Nuclear, Epitopes, Species Specificity, Antigen, medicine, Animals, Humans, Lupus Erythematosus, Systemic, Amino Acid Sequence, skin and connective tissue diseases, Peptide sequence, Autoantibodies, Multidisciplinary, Lupus erythematosus, Systemic lupus erythematosus, Sequence Homology, Amino Acid, SnRNP Core Proteins, RNA-Binding Proteins, biochemical phenomena, metabolism, and nutrition, Biological Sciences, medicine.disease, Virology, stomatognathic diseases, Immunology, Spliceosomes, biology.protein, Immunization, Rabbits, Antibody, Small nuclear ribonucleoprotein

Abstract

A subset of lupus patients with severe nephritis and anti-nRNP reactivity produces autoantibodies primarily against two major epitopes of the nRNP A (also known as U1A) protein. These sequences span amino acids 44-56 (A3) and amino acids 103-115 (A6). These two epitopes represent structurally different regions of the protein, as both epitopes are located on the surface, but the A6 epitope is functionally maskedin vivoby binding between nRNP A and the U1 RNA. Rabbits were immunized with either the A3 or A6 peptides constructed on a branching polylysine backbone. Rabbits immunized with each of these peptides first developed antibodies directed against the peptide of immunization. With boosting, the immune response of rabbits immunized with the A3 peptide spread to other common antigenic regions of nRNP A. These regions of nRNP A bound by A3 immunized rabbits are very similar to common epitopes in human systemic lupus erythematosus. These A3 immunized rabbits also develop antibodies to common antigenic regions of nRNP 70K, nRNP C, Sm B/B′, and Sm D1 proteins, as well as clinical symptoms of systemic lupus erythematosus such as leukopenia and renal insufficiency. On the other hand, rabbits immunized with the A6 peptide only develop antibodies to the peptide of immunization. Anti-A3, but not anti-A6, antibodies are capable of immunoprecipitating native small nuclear ribonucleoprotein complexes. Immunization with the A3 peptide of nRNP A (a surface epitope), but not the A6 peptide (masked), induces an extensive, varied immune response against multiple small nuclear ribonucleoprotein autoantigens similar to that seen in human systemic lupus erythematosus.

Published

2004

43. Genetic Ancestry, Serum Interferon-α Activity, and Autoantibodies in Systemic Lupus Erythematosus

Author

Timothy B. Niewold, Kenneth M. Kaufman, John B. Harley, Beverly S. Franek, Carl D. Langefeld, Miranda C. Marion, and Kichul Ko

Subjects

Male, Genetic genealogy, Immunology, Black People, Alpha interferon, Article, Rheumatology, Interferon, Interferon α, medicine, Humans, Lupus Erythematosus, Systemic, Immunology and Allergy, Genetic Predisposition to Disease, Ohio, Ribonucleoprotein, Principal Component Analysis, Lupus erythematosus, biology, Autoantibody, Interferon-alpha, Middle Aged, medicine.disease, Ribonucleoproteins, Antibodies, Antinuclear, biology.protein, Female, Antibody, medicine.drug

Abstract

Objective.To investigate and refine the relationships among systemic lupus erythematosus (SLE) and related autoantibodies, interferon-α (IFN-α), and various ancestral backgrounds.Methods.We investigated quantitatively defined genetic ancestry through principal component analysis in place of self-reported ancestry.Results.African ancestry was found to be associated with presence of anti-RNP antibody (p = 0.0026), and anti-RNP was correlated with high levels of IFN-α (p = 2.8 × 10−5).Conclusion.Our data support a model in which African ancestry increases the likelihood of SLE-associated autoantibody formation, which subsequently results in higher levels of serum IFN-α.

Published

2012

44. Anti-Sm Autoantibodies in Systemic Lupus Target Highly Basic Surface Structures of Complexed Spliceosomal Autoantigens

Author

Kenneth M. Kaufman, Micah T. McClain, Judith A. James, and Paul A. Ramsland

Subjects

Adult, Male, Models, Molecular, Adolescent, Macromolecular Substances, Molecular Sequence Data, Immunology, Biology, Crystallography, X-Ray, medicine.disease_cause, Autoantigens, Binding, Competitive, Epitope, Autoimmunity, Antigen, medicine, Humans, Lupus Erythematosus, Systemic, Immunology and Allergy, Amino Acid Sequence, Isoelectric Point, Peptide sequence, Autoantibodies, Ribonucleoprotein, Spliceosomal complex, Lupus erythematosus, Amino Acids, Basic, Ribonucleoproteins, Small Nuclear, medicine.disease, Molecular biology, Epitope mapping, Biochemistry, Spliceosomes, Epitopes, B-Lymphocyte, Female, Epitope Mapping

Abstract

Autoantibodies directed against spliceosomal proteins are a common and specific feature of systemic lupus erythematosus. These autoantibodies target a collection of proteins, including Sm B, B′, D1, D2, and D3. We define the common antigenic targets of Sm D2 and D3 and examine their role in spliceosomal autoimmunity. Our results define nine major common epitopes, five on Sm D2 and four on Sm D3. These epitopes have significantly higher (more basic) isoelectric points than do nonantigenic regions. In fact, this association is of sufficient power to make isoelectric point an excellent predictor of spliceosomal antigenicity. The crystallographic structure of Sm D2 and D3 is now partially described. The anti-Sm D2 and D3 antigenic targets are located on the surface of the respective three-dimensional complexed proteins, thereby suggesting that these epitopes are accessible in the native configuration. All but one of these nine epitopes conspicuously avoid the specific regions involved in intermolecular interactions within the spliceosomal complex. One of the D3 epitopes (RGRGRGMGR) has significant sequence homology with a major antigenic region of Sm D1 (containing a carboxyl-terminal glycine-arginine repeat), and anti-D3 Abs cross-react with this epitope of Sm D1. These results demonstrate that spliceosomal targets of autoimmunity are accessible on native structure surfaces and that cross-reactive epitopes, as well as structural associations of various spliceosomal Ags, may be involved in the induction of autoimmunity in systemic lupus.

Published

2002

45. Next Generation DNA Sequencing of Novel Loci in Workers with Diisocyanate Asthma (DA)

Author

Banu Kesavalu, Xavier Muñoz, Santiago Quirce, Matthew T. Weirauch, David I. Bernstein, Ignacio Pérez-Camo, Zana L. Lummus, Berran Yucesoy, Kenneth M. Kaufman, María Jesús Cruz, Joaquín Sastre, André Cartier, and Catherine Lemière

Subjects

Genetics, Immunology, medicine, Immunology and Allergy, Biology, medicine.disease, DNA sequencing, Asthma

Published

2017

46. Whole exome sequencing for familial bicuspid aortic valve identifies putative variants

Author

Phillip J. Dexheimer, D. Woodrow Benson, Linda H. Cripe, Kenneth M. Kaufman, Leah C. Kottyan, Valentina Pilipenko, Mehdi Keddache, Lisa J. Martin, and Matthew T. Weirauch

Subjects

Aortic valve, Adult, Male, Genotype, Genetic Linkage, Heart Valve Diseases, Biology, Bicuspid aortic valve, Bicuspid Aortic Valve Disease, Genetics, medicine, Humans, Exome, Genetic Predisposition to Disease, Genetics (clinical), Exome sequencing, Family Health, Models, Genetic, Computational Biology, Genetic Variation, Reproducibility of Results, medicine.disease, Pedigree, medicine.anatomical_structure, Phenotype, Aortic Valve, Female, Cardiology and Cardiovascular Medicine

Abstract

Background— Bicuspid aortic valve (BAV) is the most common congenital cardiovascular malformation. Although highly heritable, few causal variants have been identified. The purpose of this study was to identify genetic variants underlying BAV by whole exome sequencing a multiplex BAV kindred. Methods and Results— Whole exome sequencing was performed on 17 individuals from a single family (BAV=3; other cardiovascular malformation, 3). Postvariant calling error control metrics were established after examining the relationship between Mendelian inheritance error rate and coverage, quality score, and call rate. To determine the most effective approach to identifying susceptibility variants from among 54 674 variants passing error control metrics, we evaluated 3 variant selection strategies frequently used in whole exome sequencing studies plus extended family linkage. No putative rare, high-effect variants were identified in all affected but no unaffected individuals. Eight high-effect variants were identified by ≥2 of the commonly used selection strategies; however, these were either common in the general population (>10%) or present in the majority of the unaffected family members. However, using extended family linkage, 3 synonymous variants were identified; all 3 variants were identified by at least one other strategy. Conclusions— These results suggest that traditional whole exome sequencing approaches, which assume causal variants alter coding sense, may be insufficient for BAV and other complex traits. Identification of disease-associated variants is facilitated by the use of segregation within families.

Published

2014

47. Two Functional Lupus-Associated BLK Promoter Variants Control Cell-Type- and Developmental-Stage-Specific Transcription

Author

Joan T. Merrill, R. Hal Scofield, Anne M. Stevens, Diane L. Kamen, Nan Shen, Jennifer A. Kelly, Michelle Petri, Gary S. Gilkeson, Edward K. Wakeland, Carl D. Langefeld, Hye Soon Lee, Kenneth M. Kaufman, Chaim O. Jacob, Robert P. Kimberly, Carol F. Webb, Graham B. Wiley, Xana Kim-Howard, Joel M. Guthridge, Swapan K. Nath, Kathy L. Sivils, Jeffery Edberg, Betty P. Tsao, Harry Sun, Robert R. Graham, Susan A. Boackle, John B. Harley, Elizabeth E. Brown, Xiaoxia Qian, Marta E. Alarcón-Riquelme, Rosalind Ramsey-Goldman, Timothy J. Vyse, Lindsey A. Criswell, Luis M. Vilá, Isaac T.W. Harley, Beth L. Cobb, Judith A. James, John D. Reveille, Timothy W. Behrens, Young Bin Joo, Susan R. Macwana, Celi Sun, Patrick M. Gaffney, So Young Bang, Christopher J. Lessard, Timothy B. Niewold, Jiyoung Choi, Barry I. Freedman, Nicolas Dominguez, Adam Adler, Sang Cheol Bae, and Rufei Lu

Subjects

Male, Transcription, Genetic, Electrophoretic Mobility Shift Assay, Medical and Health Sciences, Transcription (biology), 2.1 Biological and endogenous factors, Lupus Erythematosus, Systemic, Genetics(clinical), Aetiology, Promoter Regions, Genetic, Genetics (clinical), Genetics, Genetics & Heredity, Systemic lupus erythematosus, Single Nucleotide, Biological Sciences, src-Family Kinases, Pair 8, Female, Transcription, Human, Chromosomes, Human, Pair 8, Lupus, Locus (genetics), Biology, Autoimmune Disease, Polymorphism, Single Nucleotide, Chromosomes, Article, Promoter Regions, Genetic, Clinical Research, medicine, Humans, Electrophoretic mobility shift assay, Genetic Predisposition to Disease, Allele, Progenitor cell, Polymorphism, Alleles, Lupus erythematosus, Lupus Erythematosus, Inflammatory and immune system, Haplotype, Systemic, medicine.disease, Stem Cell Research, Molecular biology, Haplotypes

Abstract

Efforts to identify lupus-associated causal variants in the FAM167A/BLK locus on 8p21 are hampered by highly associated noncausal variants. In this report, we used a trans-population mapping and sequencing strategy to identify a common variant (rs922483) in the proximal BLK promoter and a tri-allelic variant (rs1382568) in the upstream alternative BLK promoter as putative causal variants for association with systemic lupus erythematosus. The risk allele (T) at rs922483 reduced proximal promoter activity and modulated alternative promoter usage. Allelic differences at rs1382568 resulted in altered promoter activity in B progenitor cell lines. Thus, our results demonstrated that both lupus-associated functional variants contribute to the autoimmune disease association by modulating transcription of BLK in B cells and thus potentially altering immune responses.

Published

2014

48. Genome-wide association analysis of eosinophilic esophagitis provides insight into the tissue specificity of this allergic disease

Author

Sara Lazaro, Matthew T. Weirauch, Joseph D. Sherrill, Samuel E. Vaughn, Hua He, Hugh A. Sampson, Vincent A. Mukkada, Mark Rochman, Andrew M. Rupert, Katherine A. Kemme, J. Pablo Abonia, Brian P. Vickery, Kan Liu, Mirna Chehade, Phil E. Putnam, Benjamin P. Davis, Leah C. Kottyan, Kenneth M. Kaufman, Robbie D. Pesek, Lisa J. Martin, Emily M. Stucke, Albert F. Magnusen, Mojtaba Kohram, Marc E. Rothenberg, Robert Lindbad, John B. Harley, Phillip Dexheimer, Robert A. Wood, and David Fleischer

Subjects

Adult, Male, Adolescent, Genotype, Genome-wide association study, Disease, Biology, Article, Young Adult, Esophagus, Meta-Analysis as Topic, Genetics, medicine, Humans, Genetic Predisposition to Disease, Eosinophilic esophagitis, Child, Interleukin-13, Models, Genetic, Calpain, Haplotype, Genetic Variation, Epithelial Cells, Eosinophilic Esophagitis, Middle Aged, medicine.disease, Up-Regulation, medicine.anatomical_structure, Haplotypes, Organ Specificity, Child, Preschool, Interleukin 13, Immunology, Female, Genome-Wide Association Study

Abstract

Eosinophilic esophagitis (EoE) is a chronic inflammatory disorder associated with allergic hypersensitivity to food. We interrogated1.5 million genetic variants in EoE cases of European ancestry and subsequently in a multi-site cohort with local and out-of-study control subjects. In addition to replicating association of the 5q22 locus (meta-analysis P=1.9×10(-16)), we identified an association at 2p23 spanning CAPN14 (P=2.5×10(-10)). CAPN14 was specifically expressed in the esophagus, was dynamically upregulated as a function of disease activity and genetic haplotype and after exposure of epithelial cells to interleukin (IL)-13, and was located in an epigenetic hotspot modified by IL-13. Genes neighboring the top 208 EoE-associated sequence variants were enriched for esophageal expression, and multiple loci for allergic sensitization were associated with EoE susceptibility (4.8×10(-2)P5.1×10(-11)). We propose a model to explain the tissue-specific nature of EoE that involves the interplay of allergic sensitization with an EoE-specific, IL-13-inducible esophageal response involving CAPN14.

Published

2014

49. The effect of inversion at 8p23 on BLK association with lupus in Caucasian population

Author

John B. Harley, Iouri Chepelev, Leah C. Kottyan, Bahram Namjou, Patrick M. Gaffney, Kenneth M. Kaufman, Joel M. Guthridge, Isaac T.W. Harley, Yizhao Ni, and Beth L. Cobb

Subjects

Male, Linkage disequilibrium, lcsh:Medicine, Locus (genetics), Biology, Research and Analysis Methods, Polymorphism, Single Nucleotide, White People, Database and Informatics Methods, Rheumatology, Genetics, Medicine and Health Sciences, medicine, Humans, Lupus Erythematosus, Systemic, International HapMap Project, Allele, lcsh:Science, Genotyping, Sequence Inversion, Clinical Genetics, Multidisciplinary, Systemic lupus erythematosus, Homozygote, Haplotype, lcsh:R, Biology and Life Sciences, medicine.disease, United States, src-Family Kinases, Haplotypes, Genetic Loci, Case-Control Studies, Female, lcsh:Q, Chromosomes, Human, Pair 8, Research Article

Abstract

UNLABELLED:To explore the potential influence of the polymorphic 8p23.1 inversion on known autoimmune susceptibility risk at or near BLK locus, we validated a new bioinformatics method that utilizes SNP data to enable accurate, high-throughput genotyping of the 8p23.1 inversion in a Caucasian population. METHODS:Principal components analysis (PCA) was performed using markers inside the inversion territory followed by k-means cluster analyses on 7416 European derived and 267 HapMaP CEU and TSI samples. A logistic regression conditional analysis was performed. RESULTS:Three subgroups have been identified; inversion homozygous, heterozygous and non-inversion homozygous. The status of inversion was further validated using HapMap samples that had previously undergone Fluorescence in situ hybridization (FISH) assays with a concordance rate of above 98%. Conditional analyses based on the status of inversion were performed. We found that overall association signals in the BLK region remain significant after controlling for inversion status. The proportion of lupus cases and controls (cases/controls) in each subgroup was determined to be 0.97 for the inverted homozygous group (1067 cases and 1095 controls), 1.12 for the inverted heterozygous group (1935 cases 1717 controls) and 1.36 for non-inverted subgroups (924 cases and 678 controls). After calculating the linkage disequilibrium between inversion status and lupus risk haplotype we found that the lupus risk haplotype tends to reside on non-inversion background. As a result, a new association effect between non-inversion status and lupus phenotype has been identified ((p = 8.18×10(-7), OR = 1.18, 95%CI = 1.10-1.26). CONCLUSION:Our results demonstrate that both known lupus risk haplotype and inversion status act additively in the pathogenesis of lupus. Since inversion regulates expression of many genes in its territory, altered expression of other genes might also be involved in the development of lupus.

Published

2014

50. Linkage analysis of angiotensin-converting enzyme (ACE) insertion/deletion polymorphism and systemic lupus erythematosus

Author

David Hutchings, R. Hal Scofield, John B. Harley, Tiffany Baird, Kathy L. Moser, Jeff Reid, Gail R. Bruner, Neeraj Asundi, Jennifer A. Kelly, Kenneth M. Kaufman, Hua Yu, and Courtney Gray-McGuire

Subjects

Genotype, Genetic Linkage, Alu element, Peptidyl-Dipeptidase A, Biology, Biochemistry, Endocrinology, Gene Frequency, immune system diseases, Genetic linkage, medicine, Humans, Lupus Erythematosus, Systemic, Genetic Testing, skin and connective tissue diseases, Molecular Biology, Allele frequency, Sequence Deletion, Genetic association, Family Health, Enzyme Gene, Genetics, Polymorphism, Genetic, Systemic lupus erythematosus, Racial Groups, Angiotensin-converting enzyme, medicine.disease, Molecular biology, biology.protein

Abstract

Previous studies have suggested an association between systemic lupus erythematosus (SLE) and an insertion/deletion polymorphism in the angiotensin-converting enzyme gene (ACE). This polymorphism consists of a 250-bp insertion/deletion of an alu repeat in the 16th intron of the ACE gene. Individuals homozygous for the deletion have a higher level of circulating enzyme. Due to the important role of this enzyme in regulating the renin--angiotensin and kallikrein--kininogen systems, it is possible that the ACE insertion/deletion may play a role in SLE, which can include vasculitis and vascular changes. Using primers flanking the insertion/deletion site, we have examined the ACE gene in lupus patients and family members using genomic DNA obtained from the Lupus Multiplex Registry and Repository (LMRR). We were unable to detect significant linkage or genetic association between the ACE gene and SLE.

Published

2001