Your search keyword '"Timothy J Vyse"' showing total 291 results

101. 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

102. Dissection of Genetic Mechanisms Governing the Expression of Serum Retroviral gp70 Implicated in Murine Lupus Nephritis

Author

Trine N. Jørgensen, Naoki Morito, Liliane Fossati-Jimack, Lucie Clementine Baudino, Leonard H. Evans, Bernard J Morley, Shuichi Kikuchi, Timothy J. Vyse, Kumiko Yoshinobu, Sachiko Hirose, Brian L. Kotzin, Christina L. Roark, Rebecca M. Tucker, and Shozo Izui

Subjects

Mice, Inbred MRL lpr, Molecular Chaperones/biosynthesis/genetics, viruses, Immunology, Congenic, Lupus nephritis, Endogenous retrovirus, Endogeny, ddc:616.07, Biology, Autoantigens, Article, Virus, Mice, Mice, Congenic, Lupus Nephritis/blood/genetics/pathology, hemic and lymphatic diseases, medicine, Animals, Immunology and Allergy, Glycoproteins, Regulator gene, chemistry.chemical_classification, Mice, Inbred NZB, Endogenous Retroviruses, RNA, medicine.disease, Lupus Nephritis, Virology, Molecular biology, Mice, Inbred C57BL, carbohydrates (lipids), Inflammation Mediators/blood/physiology, chemistry, Endogenous Retroviruses/genetics/immunology, Glycoproteins/biosynthesis/blood/genetics, Autoantigens/biosynthesis/genetics/immunology, Inflammation Mediators, Glycoprotein, Molecular Chaperones

Abstract

The endogenous retroviral envelope glycoprotein, gp70, implicated in murine lupus nephritis is secreted by hepatocytes as an acute phase protein, and it has been thought to be a product of an endogenous xenotropic virus, NZB-X1. However, since endogenous polytropic (PT) and modified polytropic (mPT) viruses encode gp70s that are closely related to xenotropic gp70, these viruses can be additional sources of serum gp70. To better understand the genetic basis of the expression of serum gp70, we analyzed the abundance of xenotropic, PT, or mPT gp70 RNAs in livers and the genomic composition of corresponding proviruses in various strains of mice, including two different Sgp (serum gp70 production) congenic mice. Our results demonstrated that the expression of different viral gp70 RNAs was remarkably heterogeneous among various mouse strains and that the level of serum gp70 production was regulated by multiple structural and regulatory genes. Additionally, a significant contribution of PT and mPT gp70s to serum gp70 was revealed by the detection of PT and mPT, but not xenotropic transcripts in 129 mice, and by a closer correlation of serum levels of gp70 with the abundance of PT and mPT gp70 RNAs than with that of xenotropic gp70 RNA in Sgp3 congenic mice. Furthermore, the injection of lipopolysaccharides selectively up-regulated the expression of xenotropic and mPT gp70 RNAs, but not PT gp70 RNA. Our data indicate that the genetic origin of serum gp70 is more heterogeneous than previously thought, and that distinct retroviral gp70s are differentially regulated in physiological vs inflammatory conditions.

Published

2008

103. The genetics of SLE: an update in the light of genome-wide association studies

Author

Timothy J. Vyse and Benjamin Rhodes

Subjects

Genetic Markers, Genetics, Candidate gene, Polymorphism, Genetic, Models, Genetic, Genome-wide association study, Genomics, Disease, Biology, Acquired immune system, Genome, Rheumatology, Animals, Humans, Lupus Erythematosus, Systemic, Genetic Predisposition to Disease, Pharmacology (medical), Candidate Disease Gene, Gene, Genome-Wide Association Study

Abstract

Understanding the pathogenesis of SLE remains a considerable challenge. Multiple abnormalities of both the innate and adaptive immune system have been described and, furthermore, immunological dysfunction precedes clinical presentation by many years. There is a strong genetic basis to SLE, which means that genetic studies can play a key role in furthering our understanding of this disease. Since susceptibility variants are present from birth and are unaffected by the course of the disease, or by its treatment, genetic analysis is, perhaps uniquely, capable of identifying fundamental, causative, disease mechanisms. Over the last 12 months, there has been a staggering increase in our understanding of SLE genetics. We have seen the identification of new and important SLE susceptibility genes through candidate gene studies, and we have seen the publication of two whole-genome association analyses. The 'hypothesis free' whole-genome studies have provided additional evidence in support of a number of existing susceptibility genes and have identified novel gene candidates. In this article, we review the current SLE genetics literature in the light of these recent advances and we discuss our current understanding of the functional role of the key susceptibility genes. By considering how these genes fall into clusters with shared function we can begin to understand how dysregulation at a number of key immunological steps may predispose to the development of SLE.

Published

2008

104. Systemic lupus erythematosus genetics: what’s new?

Author

Timothy J. Vyse and Benjamin Rhodes

Subjects

medicine.medical_specialty, Rheumatology, business.industry, Molecular genetics, education, medicine, Susceptibility gene, business, Genealogy

Abstract

Benjamin Rhodes & Timothy J Vyse† †Author for correspondence Imperial College London, Section of Molecular Genetics and Rheumatology, Faculty of Medicine, Du Cane Road, London, W12 0NN, UK Tel.: +44 208 383 2339; Fax: +44 208 383 2379; t.vyse@imperial.ac.uk ‘Identifying SLE susceptibility genes is important because they will highlight pathways fundamental to the development of SLE, and may, in turn, become targets for therapeutic intervention.’

Published

2008

105. Association of LY9 in UK and Canadian SLE families

Author

Timothy J. Vyse, Thomas J. Hudson, Benjamin Rhodes, Joan E. Wither, S. Lim, CaNIOS GenES Investigators, Arlene H. Sharpe, Tamara McKenzie, Lauren Chad, John D. Rioux, Celia M. T. Greenwood, Alexandre Montpetit, L. Farwell, Y-C Cai, D S Cunninghame Graham, Cox Terhorst, and Paul R. Fortin

Subjects

Nonsynonymous substitution, Canada, Genetic Linkage, Immunology, Population, Locus (genetics), Biology, Polymorphism, Single Nucleotide, Antigen, Antigens, CD, Signaling Lymphocytic Activation Molecule Family, Genetic linkage, Genetics, medicine, Humans, Lupus Erythematosus, Systemic, Genetic Predisposition to Disease, Allele, education, Alleles, Genetics (clinical), education.field_of_study, Membrane Glycoproteins, Lupus erythematosus, medicine.disease, United Kingdom, Pedigree, CD8

Abstract

Systemic lupus erythematosus (SLE) is a complex disease trait of unknown aetiology. Genome-wide linkage studies in human SLE identified several linkage regions, including one at 1q23, which contains multiple susceptibility genes, including the members of the signalling lymphocyte activation molecule (SLAM) locus. In mice there is a syntenic linkage region, Sle1. The SLAM genes are functionally related cell-surface receptors, which regulate signal transduction of cells in the immune system. Family-based association study in UK and Canadian SLE families identified variants in the promoter and coding region of SLAMF7 and LY9 contributing to SLE disease susceptibility. The strongest association was from rs509749, in exon 8 of LY9 (P=0.00209). rs509749 encodes a Val/Met nonsynonymous change in amino acid 602 in the cytoplasmic domain of LY9. In the parents and affected individuals from the Canadian SLE families, the risk allele of rs509049 skews the T-cell population by increasing the number of CD8+ memory T cells, while decreasing the proportion of CD4+ naïve T cells and activated T cells. Since rs509749 lies within the consensus binding site for SAP/SH2D1a, which influences downstream signalling events from LY9, the mechanism for increased CD8+ memory T cells may include differential binding SAP/SH2D1a to the cytoplasmic domain of LY9.

Published

2008

106. Copy number variation of Fc gamma receptor genes and disease predisposition

Author

M. Fanciulli, Timothy J. Aitman, and Timothy J. Vyse

Subjects

Genetics, Polymorphism, Genetic, Receptors, IgG, Gene Dosage, Disease, Biology, Phenotype, Gene dosage, Evolution, Molecular, Immune system, Immunity, Multigene Family, Animals, Humans, Fc-Gamma Receptor, Genetic Predisposition to Disease, Copy-number variation, Molecular Biology, Gene, Genetics (clinical)

Abstract

Naturally occurring variation in gene copy number is increasingly recognized as a major source of inter-individual differences in phenotype and is an important susceptibility factor for genetically complex diseases. Several studies provide evidence of copy number variation at genes involved in inflammation and immunity highlighting their possible contribution to the inter-individual variation observed in immune responses. This review will explore copy number variation at the Fc gamma receptor cluster and its relevance in the pathogenesis of common human diseases.

Published

2008

107. Polymorphism at the TNF superfamily gene TNFSF4 confers susceptibility to systemic lupus erythematosus

Author

Timothy W. Behrens, Kathy L. Moser, Deborah S. Cunninghame Graham, Timothy J. Vyse, Patrick M. Gaffney, Andrew Wong, Harinder Manku, Robert R. Graham, David Altshuler, John C. Whittaker, and John D. Rioux

Subjects

medicine.medical_treatment, T cell, OX40 Ligand, Biology, Polymorphism, Single Nucleotide, Article, Genetics, medicine, Lupus Erythematosus, Systemic, Genetic Predisposition to Disease, Promoter Regions, Genetic, skin and connective tissue diseases, Receptor, Cells, Cultured, Autoimmune disease, Polymorphism, Genetic, Haplotype, FCGR3B, medicine.disease, United Kingdom, Cytokine, medicine.anatomical_structure, Haplotypes, Immunology, Tumor necrosis factor alpha, IRF5

Abstract

Systemic lupus erythematosus (SLE) is a multisystem complex autoimmune disease of uncertain etiology (OMIM 152700). Over recent years a genetic component to SLE susceptibility has been established1–3. Recent successes with association studies in SLE have identified genes including IRF5 (refs. 4,5) and FCGR3B6. Two tumor necrosis factor (TNF) superfamily members located within intervals showing genetic linkage with SLE are TNFSF4 (also known as OX40L; 1q25), which is expressed on activated antigen-presenting cells (APCs)7,8 and vascular endothelial cells9, and also its unique receptor, TNFRSF4 (also known as OX40; 1p36), which is primarily expressed on activated CD4+ T cells10. TNFSF4 produces a potent co-stimulatory signal for activated CD4+ T cells after engagement of TNFRSF4 (ref. 11). Using both a family-based and a case-control study design, we show that the upstream region of TNFSF4 contains a single risk haplotype for SLE, which is correlated with increased expression of both cell-surface TNFSF4 and the TNFSF4 transcript. We hypothesize that increased expression of TNFSF4 predisposes to SLE either by quantitatively augmenting T cell–APC interaction or by influencing the functional consequences of T cell activation via TNFRSF4.

Published

2007

108. Genetic Dissection of Spontaneous Autoimmunity Driven by 129-Derived Chromosome 1 Loci When Expressed on C57BL/6 Mice

Author

Francesco Carlucci, Liliane Fossati-Jimack, Marina Botto, Josefina Cortes-Hernandez, H. Terence Cook, Timothy J. Vyse, Anne E. Bygrave, and Mark Walport

Subjects

C57BL/6, Quantitative Trait Loci, Immunology, Congenic, Autoimmunity, Bone Marrow Cells, Mice, Transgenic, Biology, medicine.disease_cause, Autoantigens, T-Lymphocytes, Regulatory, Chromosomes, Mice, Immune Tolerance, medicine, Genetic predisposition, Animals, Lupus Erythematosus, Systemic, Immunology and Allergy, Genetic Predisposition to Disease, IL-2 receptor, Central element, Lupus erythematosus, Macrophages, Autoantibody, medicine.disease, biology.organism_classification, Gene Expression Regulation, Antibodies, Antinuclear, Antibody Formation

Abstract

Extensive evidence indicates that genetic predisposition is a central element in susceptibility to systemic lupus erythematosus both in humans and animals. We have previously shown that a congenic line carrying a 129-derived chromosome 1 interval on the C57BL/6 background developed humoral autoimmunity. To further dissect the contribution to autoimmunity of this 129 interval, we have created six subcongenic strains carrying fractions of the original 129 region and analyzed their serological and cellular phenotypes. At 1 year of age the congenic strain carrying a 129 interval between the microsatellites D1Mit15 (87.9 cM) and D1Mit115 (99.7 cM) (B6.129chr1b) had high levels of autoantibodies, while all the other congenic lines were not significantly different from the C57BL/6 controls. The B6.129chr1b strain displayed only mild proliferative glomerulonephritis despite high levels of IgG and C3 deposited in the kidneys. FACS analysis of the spleens revealed that the B6.129chr1b mice had a marked increase in the percentage of activated T cells associated with a significant reduction in the proportion of CD4+CD25high regulatory T cells. Moreover, this analysis showed a significantly reduced percentage of marginal zone B cells that preceded autoantibody production. Interestingly the 129chr1b-expressing bone marrow-derived macrophages displayed an impaired uptake of apoptotic cells in vitro. Collectively, our data indicate that the 129chr1b segment when recombined on the C57BL/6 genomic background is sufficient to induce loss of tolerance to nuclear Ags. These findings have important implication for the interpretation of the autoimmune phenotype associated with gene-targeted models.

Published

2007

109. General aspects of the genetics of SLE

Author

Benjamin Rhodes and Timothy J. Vyse

Subjects

Genetics, Candidate gene, Lupus erythematosus, Genetic Linkage, Immunology, Environment, Biology, medicine.disease, Disease Models, Animal, Mice, immune system diseases, medicine, Animals, Humans, Lupus Erythematosus, Systemic, Immunology and Allergy, Genetic Predisposition to Disease, skin and connective tissue diseases, Genetic association

Abstract

The application of genetic techniques to the study of systemic lupus erythematosus (SLE) has identified candidate genes with diverse immunological function. There is a growing understanding that susceptibility to SLE is due to a complex interaction of multiple genes and environmental factors, and that many of these may be shared with other autoimmune diseases. In this first of a series of review articles we outline our current understanding of SLE genetics, in particular summarising the results of recent association studies.

Published

2007

110. Identification of a systemic lupus erythematosus risk locus spanningATG16L2, FCHSD2,andP2RY2in Koreans

Author

Astrid Rasmussen, Bok Ghee Han, Kathy L. Sivils, Hannah C. Ainsworth, Quan Zhen Li, Jennifer A. Kelly, Seung Cheol Shim, Lindsey A. Criswell, Timothy J. Vyse, Soo Kon Lee, Edward K. Wakeland, Yeong Wook Song, So Young Bang, John A. Ice, Kwangwoo Kim, Betty P. Tsao, Patrick M. Gaffney, Robert P. Kimberly, Young Bin Joo, Jian Zhao, Christopher J. Lessard, Satria Sajuthi, Hye Soon Lee, Marta E. Alarcón-Riquelme, Young Mo Kang, John B. Harley, Jeongim Choi, Young-Jin Kim, He Li, Chaim O. Jacob, Chang Hee Suh, Miranda C. Marion, Ji Hee Oh, Jung Yoon Choe, Nan Shen, Hwee Siew Howe, Sang Cheol Bae, Carl D. Langefeld, and Won Tae Chung

Subjects

Genetics, Public health genomics, Extramural, Immunology, Library science, Biobank, Disease control, Rheumatology, Control data, Susceptibility locus, Immunology and Allergy, Christian ministry, Sociology, Sample collection

Abstract

Supported by grants from the NIH (5P01-AI-083194 to Drs. Lessard, Rasmussen, Gaffney, Alarcon-Riquelme, Criswell, Jacob, Kimberly, Vyse, Harley, Sivils, Langefeld, and Tsao; 5P01-AR-049084 to Drs. Kimberly and Langefeld; and R01-AR-043814 and R21-AR-065626 to Dr. Tsao), the Oklahoma Medical Research Foundation (to Drs. Lessard, Gaffney, and Sivils), the Alliance for Lupus Research (to Drs. Criswell and Tsao), and the Wake Forest School of Medicine Center for Public Health Genomics (to Dr. Langefeld). Dr. Criswell is recipient of a Kirkland Scholar Award. Sample collection and phenotyping of the subjects utilized in this study was funded by the Ministry for Health and Welfare, Republic of Korea (Korea Healthcare Technology R&D Project grant HI13C2124 to Dr. Bae, and HI13C1754 to Dr. Song). The out-of-study Korean control data were provided by the Korean Biobank Project, which is supported by the Korea Centers for Disease Control and Prevention at the Korea National Institute of Health.

Published

2015

111. 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

112. Genetic association analyses implicate aberrant regulation of innate and adaptive immunity genes in the pathogenesis of systemic lupus erythematosus

Author

David L. Morris, Timothy W. Behrens, Javier Martin, Robert R. Graham, Benjamin P. Fairfax, Christopher L. Pinder, Joan E. Wither, James Bentham, Joseph M. Replogle, John D. Rioux, Timothy J. Vyse, Julian C. Knight, Marta E. Alarcón-Riquelme, Lars Rönnblom, Philip Tombleson, Deborah S. Cunninghame Graham, Ann-Christine Syvänen, Lingyan Chen, Chen, Lingyan [0000-0003-3750-6761], and Apollo - University of Cambridge Repository

Subjects

Genetic Markers, Genome-wide association study, Adaptive Immunity, Biology, Polymorphism, Single Nucleotide, Article, Immune tolerance, Immune system, Meta-Analysis as Topic, Risk Factors, Genetics, medicine, Humans, Lupus Erythematosus, Systemic, Genetic Predisposition to Disease, QA276, QH426, Genetic Association Studies, Genetic association, Autoimmune disease, Lupus erythematosus, 11 Medical And Health Sciences, 06 Biological Sciences, medicine.disease, Acquired immune system, Immunity, Innate, 3. Good health, Gene Expression Regulation, Genetic Loci, Case-Control Studies, Immunology, Expression quantitative trait loci, Developmental Biology

Abstract

© 2015 Nature America, Inc. All rights reserved.Systemic lupus erythematosus (SLE) is a genetically complex autoimmune disease characterized by loss of immune tolerance to nuclear and cell surface antigens. Previous genome-wide association studies (GWAS) had modest sample sizes, reducing their scope and reliability. Our study comprised 7,219 cases and 15,991 controls of European ancestry, constituting a new GWAS, a meta-analysis with a published GWAS and a replication study. We have mapped 43 susceptibility loci, including ten new associations. Assisted by dense genome coverage, imputation provided evidence for missense variants underpinning associations in eight genes. Other likely causal genes were established by examining associated alleles for cis-acting eQTL effects in a range of ex vivo immune cells. We found an over-representation (n = 16) of transcription factors among SLE susceptibility genes. This finding supports the view that aberrantly regulated gene expression networks in multiple cell types in both the innate and adaptive immune response contribute to the risk of developing SLE.

Published

2015

113. Osteoclast Differentiation Is Impaired in a Subgroup of SLE Patients and Correlates Inversely with Mycophenolate Mofetil Treatment

Author

Katrin M. Weiß, Barbara G. Fürnrohr, Luis E. Muñoz, Benjamin Rhodes, Georg Schett, and Timothy J. Vyse

Subjects

Male, Osteoporosis, Osteoclasts, Cell Count, lcsh:Chemistry, IMP Dehydrogenase, systemic lupus erythematosus, Adrenal Cortex Hormones, immune system diseases, Lupus Erythematosus, Systemic, interferon alpha, skin and connective tissue diseases, lcsh:QH301-705.5, Spectroscopy, biology, Receptor Activator of Nuclear Factor-kappa B, Anti-Inflammatory Agents, Non-Steroidal, RANKL, Cell Differentiation, General Medicine, Computer Science Applications, medicine.anatomical_structure, Treatment Outcome, Female, medicine.symptom, medicine.drug, Alpha interferon, Inflammation, Catalysis, Mycophenolic acid, Article, Inorganic Chemistry, Osteoclast, medicine, Humans, Physical and Theoretical Chemistry, Molecular Biology, osteoclastogenesis, business.industry, Organic Chemistry, Case-control study, mycophenolate mofetil, Interferon-alpha, Mycophenolic Acid, medicine.disease, Blood Cell Count, lcsh:Biology (General), lcsh:QD1-999, Gene Expression Regulation, Case-Control Studies, Immunology, biology.protein, business, Ex vivo

Abstract

Osteoporosis can arise in systemic lupus erythematosus (SLE) patients secondary to medication and/or chronic inflammation. To analyze if patients with SLE have phenotypically-impaired osteoclastogenesis, we differentiated ex vivo monocytes from 72 SLE patients and 15 healthy individuals into osteoclasts followed by TRAP staining and counting. We identified a subgroup of SLE patients (45%) with a significantly impaired osteoclast differentiation, relative to the other SLE patients or healthy individuals (OR 11.2, 95% CI 1.4–89.9). A review of medication indicated that patients with osteoclast counts equal to healthy donors were significantly more likely to be treated with mycophenolate mofetil (MMF) compared to patients with impaired osteoclastogenesis. We analyzed expression of RANKL and the MMF target genes IMPDH1 and IMPDH2 in osteoclasts by qPCR, but detected no difference. Since MMF might influence interferon-α (IFNα) and -γ (IFNγ) we measured serum IFNα and IFNγ levels. Patients with very low osteoclast counts also had comparably higher IFNα serum levels than patients with normal osteoclast counts. We conclude that in vitro osteoclastogenesis is impaired in a subgroup of SLE patients. This correlates inversely with MMF treatment and high IFNα serum levels. Further observational study will be required to determine whether this translates into a clinically meaningful effect.

Published

2015

114. O37. The Autoimmune Risk Gene UBE2L3 is Highly Expressed During B Cell Proliferation and is Correlated with Plasmablast and Plasma Cell Expansion in SLE

Author

Paul H. Lehner, Myles Lewis, Timothy D. Spector, Adrian M. Shields, Henning Walczak, Timothy J. Vyse, Costantino Pitzalis, and Simon Vyse

Subjects

medicine.medical_specialty, business.industry, Risk gene, Plasma cell, medicine.disease_cause, Rheumatology, B-cell proliferation, Autoimmunity, medicine.anatomical_structure, Internal medicine, Immunology, medicine, business, Gene

Published

2015

115. Defective removal of ribonucleotides from DNA promotes systemic autoimmunity

Author

Sophia Blum, Manuel Martínez-Bueno, Christine Wolf, Timothy J. Vyse, John D. Isaacs, Annette Bley, Marta E. Alarcón-Riquelme, Louise S. Bicknell, Markus M. Nöthen, L. Unger, Stuart H. Ralston, Inga Melchers, Axel Roers, Claudia Krug, Osvaldo Chara, Franziska Schmidt, Andrea Leitch, K. Lüthke, Elisabeth Mangold, Min Ae Lee-Kirsch, Norbert Hubner, Claudia Günther, Alice Lorenzi, Young-Ae Lee, Nicole Berndt, Torsten Witte, Deborah S. Cunninghame Graham, Katy R. Astell, Martin Aringer, Andrew P. Jackson, Barbara Kind, Karsten Conrad, Victoria Tüngler, Doryen Bubeck, M. Gahr, Andreas Dahl, Anja Bauerfeind, Stefanie Kretschmer, Sarah Koss, Elizabeth A. Blackburn, Georgia Ramantani, David L. Morris, Dimitra Alexopoulou, Martin A M Reijns, and Annegret Kuhn

Subjects

Heterozygote, DNA Repair, RNase P, DNA repair, DNA damage, Biología, Ribonucleotide excision repair, DNA Mutational Analysis, Ribonuclease H, Gene Expression, purl.org/becyt/ford/3.5 [https], genetics [Lupus Erythematosus, Systemic], Autoimmunity, Biology, metabolism [Pyrimidine Dimers], medicine.disease_cause, genetics [Pyrimidine Dimers], chemistry.chemical_compound, Rnase H2, metabolism [Interferon Type I], medicine, Humans, ddc:610, RNase H, Aicardi-Goutieres Syndrome, Gene, Cells, Cultured, genetics [Ribonuclease H], Cell Proliferation, Syndrome AGS, Mutation, ribonuclease HII, Lupus Erythematosus, genetics [Autoimmunity], genetics [Interferon Type I], General Medicine, Molecular biology, Aicardi Syndrome, chemistry, Pyrimidine Dimers, Cardiovascular and Metabolic Diseases, Interferon Type I, biology.protein, purl.org/becyt/ford/3 [https], DNA

Abstract

Genome integrity is continuously challenged by the DNA damage that arises during normal cell metabolism. Biallelic mutations in the genes encoding the genome surveillance enzyme ribonuclease H2 (RNase H2) cause Aicardi-Goutières syndrome (AGS), a pediatric disorder that shares features with the autoimmune disease systemic lupus erythematosus (SLE). Here we determined that heterozygous parents of AGS patients exhibit an intermediate autoimmune phenotype and demonstrated a genetic association between rare RNASEH2 sequence variants and SLE. Evaluation of patient cells revealed that SLE- and AGS-associated mutations impair RNase H2 function and result in accumulation of ribonucleotides in genomic DNA. The ensuing chronic low level of DNA damage triggered a DNA damage response characterized by constitutive p53 phosphorylation and senescence. Patient fibroblasts exhibited constitutive upregulation of IFN-stimulated genes and an enhanced type I IFN response to the immunostimulatory nucleic acid polyinosinic:polycytidylic acid and UV light irradiation, linking RNase H2 deficiency to potentiation of innate immune signaling. Moreover, UV-induced cyclobutane pyrimidine dimer formation was markedly enhanced in ribonucleotide-containing DNA, providing a mechanism for photosensitivity in RNase H2-associated SLE. Collectively, our findings implicate RNase H2 in the pathogenesis of SLE and suggest a role of DNA damage-associated pathways in the initiation of autoimmunity., La lista completa de autores que integran el documento puede consultarse en el archivo, Instituto de Física de Líquidos y Sistemas Biológicos

Published

2015

116. Association of IRF5 in UK SLE families identifies a variant involved in polyadenylation

Author

Kirsten Timms, Harinder Manku, Susanne Wagner, Timothy J. Vyse, Julia Reid, Alexander Gutin, Jerry S. Lanchbury, and Deborah S. Cunninghame Graham

Subjects

Male, Parents, Single-nucleotide polymorphism, Biology, Polyadenylation, Polymorphism, Single Nucleotide, Article, Nuclear Family, Genotype, Genetics, Humans, Lupus Erythematosus, Systemic, Allele, 3' Untranslated Regions, Molecular Biology, Gene, Genetics (clinical), Genetic association, Regulation of gene expression, Polymorphism, Genetic, Haplotype, General Medicine, Molecular biology, United Kingdom, Gene Expression Regulation, Haplotypes, Interferon Regulatory Factors, Female, IRF5

Abstract

Results from two studies have implicated the interferon regulatory gene IRF5 as a susceptibility gene in systemic lupus erythematosus (SLE). In this study, we conducted a family-based association analysis in 380 UK SLE nuclear families. Using a higher density of markers than has hitherto been screened, we show that there is association with two SNPs in the first intron, rs2004640 (P = 3.4 x 10(-4)) and rs3807306 (P = 4.9 x 10(-4)), and the association extends into the 3'-untranslated region (UTR). There is a single haplotype block encompassing IRF5 and we show for the first time that the gene comprises two over-transmitted haplotypes and a single under-transmitted haplotype. The strongest association is with a TCTAACT haplotype (T:U = 1.92, P = 5.8 x 10(-5)), which carries all the over-transmitted alleles from this study. Haplotypes carrying the T alleles of rs2004640 and rs2280714 and the A allele of rs10954213 are over-transmitted in SLE families. The TAT haplotype shows a dose-dependent relationship with mRNA expression. A differential expression pattern was seen between two expression probes located each side of rs10954213 in the 3'-UTR. rs10954213 shows the strongest association with RNA expression levels (P = 1 x 10(-14)). The A allele of rs10954213 creates a functional polyadenylation site and the A genotype correlates with increased expression of a transcript variant containing a shorter 3'-UTR. Expression levels of transcript variants with the shorter or longer 3'-UTRs are inversely correlated. Our data support a new mechanism by which an IRF5 polymorphism controls the expression of alternate transcript variants which may have different effects on interferon signalling.

Published

2006

117. Evidence for unique association signals in SLE at the CD28–CTLA4–ICOS locus in a family-based study

Author

Andrew Wong, D S Cunninghame Graham, N.J. McHugh, John C. Whittaker, and Timothy J. Vyse

Subjects

Antigens, Differentiation, T-Lymphocyte, Genetic Markers, Male, Candidate gene, T cell, Molecular Sequence Data, chemical and pharmacologic phenomena, Single-nucleotide polymorphism, Locus (genetics), Biology, Polymorphism, Single Nucleotide, Inducible T-Cell Co-Stimulator Protein, CD28 Antigens, Gene Frequency, Antigens, CD, Genetics, medicine, Humans, Lupus Erythematosus, Systemic, Cytotoxic T cell, CTLA-4 Antigen, Family, 3' Flanking Region, Allele, Molecular Biology, Genetics (clinical), Base Sequence, Haplotype, Chromosome Mapping, General Medicine, Antigens, Differentiation, medicine.anatomical_structure, Haplotypes, Multigene Family, Female, CD8

Abstract

CD28, CTLA4 (cytotoxic T lymphocyte-associated protein 4) and ICOS (inducible T cell co-stimulator) are good candidate genes for systemic lupus erythematosus (SLE) because of their role in regulating T cell activation. CTLA4 inhibits CD28-mediated T cell activation. CTLA4 is expressed on CD4+ and CD8+ activated T cells, and also B cells, but CD28 and ICOS are largely restricted to T cells. An interval encompassing the CD28-CTLA4-ICOS locus on chromosome 2q33 was linked to lupus in two genome-wide linkage scans. This large family-based association study in 532 UK SLE families represents the first high-density genetic screen of 80 SNPs at this locus. There are seven haplotype blocks across the locus. In CTLA4, the strongest signal comes from two variants, located 2.1 kb downstream from the 3'-UTR. These polymorphisms, rs231726 (SNP 43) and rs231726 (SNP 44), are in complete linkage disequilibrium (LD) (r(2)=1) and are associated with SLE P=0.0008 (GH) and P=0.01 (family-based association test). There is also a signal in the distal 3' flanking region of CTLA4/ICOS promoter (P=0.003). There was no confirmation of published associations for SLE in the promoter or coding region of CTLA4. These SLE risk alleles are more distal than those identified in Graves' disease and are in LD with Graves' disease protective alleles identified in both of these regions of CTLA4 (Ueda et al. 2003). These factors suggest an SLE-specific pattern of association. The functional consequences of the associated polymorphisms are likely to influence CTLA4 expression, although it is possible that genetically modulated ICOS expression is involved in SLE susceptibility.

Published

2006

118. A high-resolution HLA and SNP haplotype map for disease association studies in the extended human MHC

Author

John Hart, John A. Todd, Xiaojiang Gao, Paul I.W. de Bakker, Alienke J. Monsuur, Marcos Mateo Miretti, Mark J. Daly, Pardis C. Sabeti, Jonathan Marchini, Luana Galver, Cisca Wijmenga, Xiayi Ke, Mary Carrington, John Trowsdale, Panos Deloukas, David A. Hafler, Jonathan Morrison, Sarah S. Murray, Margaret A. Pericak-Vance, Simon G. Gregory, Emily C. Walsh, Timothy J. Vyse, Pamela Whittaker, Todd Green, Marcos Delgado, Stephan Beck, Gil McVean, Angela Richardson, and John D. Rioux

Subjects

Genetics, Linkage disequilibrium, education.field_of_study, Polymorphism, Genetic, Genetics, Medical, Racial Groups, Haplotype, Population, Single-nucleotide polymorphism, Human leukocyte antigen, Biology, Major histocompatibility complex, Polymorphism, Single Nucleotide, Article, Histocompatibility, Haplotypes, HLA Antigens, Histocompatibility Antigens, biology.protein, Humans, SNP, Genetic Predisposition to Disease, education

Abstract

The proteins encoded by the classical HLA class I and class II genes in the major histocompatibility complex (MHC) are highly polymorphic and play an essential role in self/non-self immune recognition. HLA variation is a crucial determinant of transplant rejection and susceptibility to a large number of infectious and autoimmune disease1. Yet identification of causal variants is problematic due to linkage disequilibrium (LD) that extends across multiple HLA and non-HLA genes in the MHC2,3. We therefore set out to characterize the LD patterns between the highly polymorphic HLA genes and background variation by typing the classical HLA genes and >7,500 common single nucleotide polymorphisms (SNPs) and deletion/insertion polymorphisms (DIPs) across four population samples. The analysis provides informative tag SNPs that capture some of the variation in the MHC region and that could be used in initial disease association studies, and provides new insight into the evolutionary dynamics and ancestral origins of the HLA loci and their haplotypes.

Published

2006

119. Identification of chromosome intervals from 129 and C57BL/6 mouse strains linked to the development of systemic lupus erythematosus

Author

Marina Botto, Mark Walport, Y Heidari, Timothy J. Vyse, Anne E. Bygrave, Kirsten L. Rose, RJ Rigby, and H.T. Cook

Subjects

Quantitative Trait Loci, Immunology, Locus (genetics), Biology, Mice, Species Specificity, Genetics, medicine, Animals, Lupus Erythematosus, Systemic, Gene, Genetics (clinical), Chromosome 13, Mice, Knockout, Autoimmune disease, Chromosome 7 (human), Complement C1q, Chromosome Mapping, C57BL/6 Mouse, medicine.disease, Phenotype, Mice, Inbred C57BL, Chromosome 3, Antibodies, Antinuclear, Female

Abstract

Systemic lupus erythematosus is an autoimmune disease in which complex interactions between genes and environmental factors determine the disease phenotype. We have shown that genes from the non-autoimmune strains 129 and C57BL/6 (B6), commonly used for generating gene-targeted animals, can induce a lupus-like disease. Here, we conducted a genome-wide scan analysis of a cohort of (129 x B6)F2 C1q-deficient mice to identify loci outside the C1qa locus contributing to the autoimmune phenotype described in these mice. The results were then confirmed in a larger dataset obtained by combining the data from the C1q-deficient mice with data from previously reported wild-type mice. Both analyses showed that a 129-derived interval on distal chromosome 1 is strongly linked to autoantibody production. The B6 genome contributed to anti-nuclear autoantibody production with an interval on chromosome 3. Two regions were linked to glomerulonephritis: a 129 interval on proximal chromosome 7 and a B6 interval on chromosome 13. These findings demonstrate that interacting loci between 129 and B6 mice can cause the expression of an autoimmune phenotype in gene-targeted animals in the absence of any disrupted gene. They also indicate that some susceptibility genes can be inherited from the genome of non-autoimmune parental strains.

Published

2006

120. Mice, humans and haplotypes—the hunt for disease genes in SLE

Author

R. J. Rigby, Maria Michelle Fernando, and Timothy J. Vyse

Subjects

Genetics, Candidate gene, education.field_of_study, Genome, Polymorphism, Genetic, Mice, Inbred NZB, Haplotype, Population, Biology, Mice, Haplotypes, Species Specificity, Rheumatology, Models, Animal, Genetic variation, Animals, Humans, Lupus Erythematosus, Systemic, Genetic Predisposition to Disease, Pharmacology (medical), Human genome, education, Candidate Disease Gene, Genetic association

Abstract

Defining the polymorphisms that contribute to the development of complex genetic disease traits is a challenging, although increasingly tractable problem. Historically, the technical difficulties in conducting association studies across the entire human genome are such that murine models have been used to generate candidate genes for analysis in human complex diseases, such as SLE. In this article we discuss the advantages and disadvantages of this approach and specifically address some assumptions made in the transition from studying one species to another, using lupus as an example. These issues include differences in genetic structure and genetic organisation which are a reflection on the population history. Clearly there are major differences in the histories of the human population and inbred laboratory strains of mice. Both human and murine genomes do exhibit structure at the genetic level. That is to say, they comprise haplotypes which are genomic regions that carry runs of polymorphisms that are not independently inherited. Haplotypes therefore reduce the number of combinations of the polymorphisms in the DNA in that region and facilitate the identification of disease susceptibility genes in both mice and humans. There are now novel means of generating candidate genes in SLE using mutagenesis (with ENU) in mice and identifying mice that generate antinuclear autoimmunity. In addition, murine models still provide a valuable means of exploring the functional consequences of genetic variation. However, advances in technology are such that human geneticists can now screen large fractions of the human genome for disease associations using microchip technologies that provide information on upwards of 100,000 different polymorphisms. These approaches are aimed at identifying haplotypes that carry disease susceptibility mutations and rely less on the generation of candidate genes.

Published

2006

121. The role of inflammatory bowel disease susceptibility loci in multiple sclerosis and systemic lupus erythematosus

Author

Lisa Farwell, Angela Richardson, P. L. De Jager, Timothy J. Vyse, Timothy W. Behrens, John D. Rioux, Juha Kere, Alastair Compston, David A. Hafler, Robert R. Graham, and Stephen Sawcer

Subjects

Multiple Sclerosis, Immunology, Nod2 Signaling Adaptor Protein, Lupus nephritis, Locus (genetics), Biology, Polymorphism, Single Nucleotide, Inflammatory bowel disease, 03 medical and health sciences, 0302 clinical medicine, Polymorphism (computer science), Genetics, medicine, Humans, Lupus Erythematosus, Systemic, Genetic Predisposition to Disease, skin and connective tissue diseases, Gene, Genetics (clinical), 030304 developmental biology, 0303 health sciences, Lupus erythematosus, Tumor Suppressor Proteins, Multiple sclerosis, Haplotype, Intracellular Signaling Peptides and Proteins, Membrane Proteins, Exons, Inflammatory Bowel Diseases, medicine.disease, digestive system diseases, 3. Good health, Chromosomes, Human, Pair 5, 030217 neurology & neurosurgery

Abstract

To date, three loci have been validated to confer susceptibility to inflammatory bowel disease (IBD): the CARD15/NOD2 gene, the discs large homolog 5 gene (DLG5), and the IBD5 locus on 5q31 (IBD5). We have explored the possibility that these loci may also be associated with susceptibility to two other chronic inflammatory diseases, multiple sclerosis (MS) and systemic lupus erythematosus (SLE). As the CARD15 risk alleles had previously been assessed in our collection of 496 MS trios, we focused our efforts on the DLG5 risk allele and the IBD5(risk) haplotype (IBD5(risk)) for MS. While there is no evidence of association within our MS sample with either of these polymorphisms, screening of 1027 subjects with SLE suggests that IBD5(risk) may have a modest contribution to disease risk in the subset of SLE subjects without lupus nephritis. In addition, a pooled analysis of existing published and unpublished data in 1305 cases of SLE genotyped for the CARD15 risk alleles suggests that only the CARD15(908R) IBD risk allele may have a strong effect on risk of SLE. Our data, therefore, suggest that both the CARD15 gene and the IBD5 locus may have a role as general susceptibility loci for certain common, genetically complex inflammatory diseases.

Published

2006

122. Copy number polymorphism in Fcgr3 predisposes to glomerulonephritis in rats and humans

Author

Joseph J. Boyle, Jennifer A. Smith, Paul R. Cook, Matthew D. Hodges, Rong Dong, Jan Domin, Gurjeet Bhangal, Amy J. Marshall, Penny J. Norsworthy, David J. Evans, Charles D. Pusey, H. Terence Cook, Timothy J. Aitman, Kelly Sheehan-Rooney, Timothy J. Vyse, Cheri Roberton-Lowe, Mark A Duda, Michelle D. Johnson, Jonathan Flint, Sheetal Patel, Jonathan Mangion, and Enrico Petretto

Subjects

Genome evolution, Positional cloning, Molecular Sequence Data, Gene Dosage, Biology, GPI-Linked Proteins, Rats, Inbred WKY, Antigens, CD, Gene Duplication, medicine, Animals, Humans, Genetic Predisposition to Disease, Copy-number variation, Gene, Sequence Deletion, Genetics, Polymorphism, Genetic, Multidisciplinary, Systemic lupus erythematosus, Base Sequence, Receptors, IgG, Glomerulonephritis, Exons, FCGR3B, medicine.disease, Lupus Nephritis, Rats, Haplotypes, Immunology, Low copy number

Abstract

Glomerulonephritis is a kidney inflammation that occurs alone or as part of other conditions, including the autoimmune disorder lupus. A novel mutation has now been identified as the cause of the disease in a rat model. The mutation affects the Fcgr3 immunoglobulin receptor, but it does not produce a defective receptor. Rather, too many copies of an otherwise normal gene are produced. A similar gene-number defect was then detected in a subset of human systemic lupus erythematosus patients with a kidney inflammation. In these patients an equivalent receptor gene, FCGR3B, is present at a low copy number. Disease seems to result when copy number is altered in either direction, so receptor levels must need to be very finely tuned. Identification of the genes underlying complex phenotypes and the definition of the evolutionary forces that have shaped eukaryotic genomes are among the current challenges in molecular genetics1,2,3. Variation in gene copy number is increasingly recognized as a source of inter-individual differences in genome sequence and has been proposed as a driving force for genome evolution and phenotypic variation3,4,5. Here we show that copy number variation of the orthologous rat and human Fcgr3 genes is a determinant of susceptibility to immunologically mediated glomerulonephritis. Positional cloning identified loss of the newly described, rat-specific Fcgr3 paralogue, Fcgr3-related sequence (Fcgr3-rs), as a determinant of macrophage overactivity and glomerulonephritis in Wistar Kyoto rats. In humans, low copy number of FCGR3B, an orthologue of rat Fcgr3, was associated with glomerulonephritis in the autoimmune disease systemic lupus erythematosus. The finding that gene copy number polymorphism predisposes to immunologically mediated renal disease in two mammalian species provides direct evidence for the importance of genome plasticity in the evolution of genetically complex phenotypes, including susceptibility to common human disease.

Published

2006

123. Genetic variation in toll-like receptor 9 and susceptibility to systemic lupus erythematosus

Author

John D. Rioux, Angela Richardson, Philip L. De Jager, and Timothy J. Vyse

Subjects

Immunology, Population, Lupus nephritis, Single-nucleotide polymorphism, Biology, Rheumatology, Genetic variation, medicine, Humans, Lupus Erythematosus, Systemic, Immunology and Allergy, Genetic Predisposition to Disease, Pharmacology (medical), Allele, skin and connective tissue diseases, education, B cell, Genetics, education.field_of_study, Lupus erythematosus, Genetic Variation, Transmission disequilibrium test, medicine.disease, medicine.anatomical_structure, Toll-Like Receptor 9

Abstract

Objective Autoantibodies produced by differentiated B cells play an important role in the pathogenesis of systemic lupus erythematosus (SLE). The Toll-like receptor 9 (TLR-9) gene has recently emerged as an important costimulatory molecule for both B cells and dendritic cells that respond to chromatin immune complexes. Genetic variation affecting the function of TLR-9 may therefore increase or decrease the threshold of B cell or dendritic cell activation. This variability in activation threshold may, in turn, affect an individual's susceptibility to SLE. This study assessed the role of genetic variation within the TLR-9 gene in susceptibility to SLE. Methods We genotyped 362 SLE-affected subject/parent trios for 10 single-nucleotide polymorphisms (SNPs) covering a 68,742-bp genomic segment that contains the TLR-9 gene and ∼60 kb of flanking sequence. We analyzed the data using the transmission disequilibrium test. Results There was no association of susceptibility to SLE with any of the 9 SNPs that generated usable data or the 8 haplotypes found at a frequency of >0.05 in this population. When analyzing the subset of 143 subjects with lupus nephritis, there was also no evidence of association between disease susceptibility and any SNP or haplotype. Conclusion These results indicate that there is no evidence that common (frequency higher than 5%) alleles of the TLR-9 gene contribute significantly to the genetic risk involved in susceptibility to SLE or lupus nephritis.

Published

2006

124. No association between E- and L-selectin genes and SLE: soluble L-selectin levels do correlate with genotype and a subset in SLE

Author

CA Roberton, Sapna Chadha, D S Cunninghame Graham, David D'Cruz, Dorothea Nitsch, B Griffiths, Timothy J. Vyse, Andrew Russell, Tim J. Fernandez-Hart, and John C. Whittaker

Subjects

Adult, Male, Quantitative Trait Loci, Immunology, Biology, Polymorphism, Single Nucleotide, Risk Factors, Genotype, Genetics, medicine, Humans, Lupus Erythematosus, Systemic, SNP, Genetic Predisposition to Disease, L-Selectin, skin and connective tissue diseases, Genetics (clinical), Systemic lupus erythematosus, Haplotype, Autoantibody, Middle Aged, medicine.disease, Phenotype, Chromosomes, Human, Pair 1, Antibodies, Antiphospholipid, biology.protein, Female, L-selectin, E-Selectin, Selectin

Abstract

Altered function of selectin glycoprotein adhesion molecules may modulate severity and organ-specific manifestations of autoimmune and inflammatory disease via changes in leukocyte trafficking. Serum concentrations of selectin molecules have been suggested as useful biomarkers in systemic lupus erythematosus (SLE). We identified increased levels of soluble L-selectin (sL-selectin), but not soluble E-selectin (sE-selectin) in 278 European-Caucasian lupus patients compared to 230 healthy siblings (P=0.002). sL-selectin levels were markedly elevated in patients with IgG antiphospholipid autoantibodies (P=0.002), suggesting that perhaps sL-selectin defines a subgroup of lupus with vasculopathy. sL-selectin level was also influenced by two L-selectin polymorphisms: 665C>T, F206L in the epidermal growth factor-like domain (P=0.015) and rs12938 in the 3'-untranslated region (P=0.06). Having shown increased sL-selectin levels in lupus patients, we used genetics to investigate whether this was a secondary phenomena or the result of an underlying genetic mechanism. The inheritance of nine single-nucleotide polymorphisms (SNP) spanning the selectin locus was tested in 523 UK simplex SLE families. No association with SLE, or related phenotypes, was evident with any single SNP, or haplotype in family-based tests of association. Selectin polymorphisms are, therefore, unlikely to be independent factors in SLE susceptibility.

Published

2005

125. Haplotype structure of TNFRSF5-TNFSF5 (CD40–CD40L) and association analysis in systemic lupus erythematosus

Author

Lisa Farwell, Timothy J. Vyse, John D. Rioux, Sapna Chadha, Liz Lightstone, Mark J. Daly, and Katie Miller

Subjects

Male, Linkage disequilibrium, CD40 Ligand, Single-nucleotide polymorphism, Biology, Polymorphism, Single Nucleotide, Linkage Disequilibrium, White People, Nuclear Family, Cohort Studies, Gene Frequency, immune system diseases, Genetics, medicine, Humans, Lupus Erythematosus, Systemic, SNP, CD40 Antigens, skin and connective tissue diseases, Allele frequency, Genetics (clinical), Genetic association, Autoimmune disease, Haplotype, hemic and immune systems, medicine.disease, Connective tissue disease, United Kingdom, Haplotypes, Immunology, Female

Abstract

Systemic lupus erythematosus (SLE) is a prototypic autoimmune disease that is caused by genetic and environmental factors. The tumour necrosis factor (TNF) superfamily of genes play a central role in immune regulation and have been proposed to be involved in the development of SLE. TNFRSF5 (CD40) falls on 20q11-13, a region linked with SLE in three independent genome-wide studies. TNFSF5 (CD40L) falls on Xq26 and is the ligand for TNFRSF5. Seven single-nucleotide polymorphisms (SNPs) in CD40 and eight SNPs in CD40L were looked at for linkage disequilibrium (LD) and haplotype analysis in European-Caucasians. Limited haplotype diversity was observed across CD40 and CD40L, and >97% of the diversity was captured. We also examined the association of SNPs and haplotypes in CD40 and CD40L with SLE in European-Caucasians. There was no evidence of association for CD40 or CD40L in 408 European-Caucasian families with SLE from UK. Haplotype tagging SNPs (htSNPs) are made known, which will facilitate analysis for susceptibility in other autoimmune diseases and risk for infectious disease.

Published

2005

126. Association analysis of the R620W polymorphism of protein tyrosine phosphatase PTPN22 in systemic lupus erythematosus families: Increased t allele frequency in systemic lupus erythematosus patients with autoimmune thyroid disease

Author

Philip L. De Jager, John D. Rioux, Daniel J. Wallace, Cecilia M. Lingren, Heikki Julkunen, Brad H. Rovin, C. Yung Yu, Jennifer M. Grossman, Daniel J. Birmingham, Bevra H. Hahn, Juha Kere, Timothy J. Vyse, Lee A. Hebert, Betty P. Tsao, Nunzio Bottini, Hui Wu, Rita M. Cantor, Lisa Farwell, and Deborah S. Cunninghame Graham

Subjects

Immunology, Arginine, White People, Autoimmune Diseases, Cohort Studies, PTPN22, 03 medical and health sciences, 0302 clinical medicine, Gene Frequency, Rheumatology, immune system diseases, medicine, Humans, Lupus Erythematosus, Systemic, Immunology and Allergy, Genetic Predisposition to Disease, Pharmacology (medical), Allele, skin and connective tissue diseases, Allele frequency, 030304 developmental biology, Genetic association, 030203 arthritis & rheumatology, Autoimmune disease, 0303 health sciences, Polymorphism, Genetic, Lupus erythematosus, business.industry, Tryptophan, Protein Tyrosine Phosphatase, Non-Receptor Type 22, Transmission disequilibrium test, medicine.disease, Thyroid Diseases, Connective tissue disease, 3. Good health, Protein Tyrosine Phosphatases, business

Abstract

Objective Recent case–control studies show associations of the minor T allele (of the C1858T single-nucleotide polymorphism corresponding to the R620W amino acid substitution) of PTPN22 with multiple autoimmune diseases, including systemic lupus erythematosus (SLE). We performed family-based association studies of this polymorphism in 4 independent cohorts containing SLE patients and their parents and/or other family members. Methods A total of 2,689 individuals from 902 independent Caucasian families with SLE were genotyped using polymerase chain reaction pyrosequencing (cohorts 1 and 2) and the Sequenom MassArray system (cohorts 3 and 4). The transmission disequilibrium test (TDT) and the pedigree disequilibrium test (PDT) were conducted to assess the evidence of association. Results The 1858 C > T allele frequencies of the parents showed no deviation from Hardy-Weinberg equilibrium within each cohort. No evidence of preferential transmission of the T allele from heterozygous parents to their affected offspring was observed in each of the 4 cohorts or in the combined sample. Consistent with the TDT result, the PDT analysis revealed no significant association between the T allele and SLE. In 54 of the 661 SLE patients (cohorts 1 and 3) with documented autoimmune thyroid disease, the T allele frequency was higher than in individuals with SLE alone (16.7% versus 8.5%; P = 0.008, odds ratio 2.16 [95% confidence interval 1.25–3.72]). Conclusion The R620W polymorphism of the PTPN22 gene is not a major risk allele for SLE susceptibility in our sample of Caucasian individuals from northern America, the UK, or Finland, but it appears to be a risk factor for the concurrent autoimmune diseases of autoimmune thyroid disease and SLE.

Published

2005

127. Models of systemic lupus erythematosus

Author

Timothy J. Vyse and RJ Rigby

Subjects

Systemic lupus erythematosus, business.industry, In silico, Complex disease, Disease, medicine.disease, Systemic autoimmune disease, Pathogenesis, immune system diseases, Drug Discovery, Immunology, Molecular Medicine, Medicine, skin and connective tissue diseases, business

Abstract

Systemic lupus erythematosus (SLE, or lupus) is a systemic autoimmune disease with a complex aetiology and pathogenesis. Several in vivo murine disease models are being studied, using many in vitro and in silico techniques and resources. Combined with emerging technologies such as gene expression analysis, these models are helping researchers understand the complex disease processes in lupus and determine the underlying genetic basis of disease – the first step towards disease-specific therapeutic intervention.

Published

2004

128. Hyper IgE in New Zealand black mice due to a dominant-negative CD23 mutation

Author

RJ Rigby, Eleni Rapsomaniki, Timothy J. Vyse, Helen Ferry, Teresa Lambe, Tiphaine Bouriez, Tanya L. Crockford, Richard J. Cornall, and Graham Lewis

Subjects

Molecular Sequence Data, Immunology, Biology, Immunoglobulin E, medicine.disease_cause, Atopy, Mice, Antigen, immune system diseases, Genetics, medicine, Animals, Point Mutation, Amino Acid Sequence, Allele, Receptor, Alleles, Mutation, Mice, Inbred NZB, Receptors, IgE, Point mutation, CD23, medicine.disease, Mice, Inbred C57BL, biology.protein, Job Syndrome

Abstract

Immunoglobulin E (IgE) plays a critical role in both resistance to parasitic infection and allergy to environmental antigens. The IgE response is in turn regulated by the B-cell co-receptor CD23, and CD23-deficient mice show exaggerated IgE responses and airway hyper-responsiveness. In this report, we show that New Zealand black (NZB) mice express a variant CD23 allele, with mutations in both the C-lectin-binding domain and stalk region, which fails to bind IgE at high affinity and has reduced expression on the cell surface. Expression of the variant CD23 chain interferes with trimerisation of the receptor and has a dominant-negative effect leading to reduced IgE binding in crosses between NZB and other strains. Genetic mapping shows that the variant CD23 leads to an exaggerated primary IgE response, which is independent of other strain-specific effects. These results suggest that NZB mice or mice carrying the variant allele will be useful models for studying both allergy and quantitative traits associated with atopy. The exaggerated IgE response provides an explanation for the natural resistance of NZB mice to parasitic infection by Leishmania.

Published

2004

129. Polymorphism at the C-reactive protein locus influences gene expression and predisposes to systemic lupus erythematosus

Author

Andrew Russell, Mark Walport, Christopher J. Shepherd, Cheri A. Roberton, Richard J Powell, John Meeks, Timothy J. Vyse, John C. Whittaker, Deborah S. Cunninghame Graham, and David A. Isenberg

Subjects

Candidate gene, Genotype, Single-nucleotide polymorphism, Polymerase Chain Reaction, Polymorphism, Single Nucleotide, Article, Linkage Disequilibrium, Cohort Studies, Pathogenesis, Genetics, medicine, Humans, Lupus Erythematosus, Systemic, Family, Genetic Predisposition to Disease, skin and connective tissue diseases, Molecular Biology, Genetics (clinical), Serum amyloid P component, DNA Primers, Polymorphism, Genetic, Lupus erythematosus, Systemic lupus erythematosus, biology, C-reactive protein, Haplotype, Sequence Analysis, DNA, General Medicine, medicine.disease, United Kingdom, Serum Amyloid P-Component, C-Reactive Protein, Gene Expression Regulation, Haplotypes, Immunology, biology.protein, Polymorphism, Restriction Fragment Length

Abstract

Relative deficiency of pentraxin proteins is implicated in the pathogenesis of systemic lupus erythematosus. The C-reactive protein (CRP) response is defective in patients with acute flares of disease, and mice with targeted deletions of the serum amyloid P component gene (Sap) develop a lupus-like illness. In humans, the genes for CRP (CRP) and SAP (APCS) map to 1q23.2 within an interval linked with SLE. We have investigated the candidate genes CRP and APCS in two cohorts totalling 586 UK simplex SLE families. The inheritance of an intronic dinucleotide repeat and seven single nucleotide polymorphisms in the CRP and APCS genes was examined by application of family-based tests of association and linkage. Basal levels of CRP were influenced independently by two polymorphisms at the CRP locus, CRP 2 and CRP 4. Furthermore, the latter polymorphism was linked/associated with SLE and antinuclear autoantibody production. Thus, the polymorphism associated with reduced basal CRP was also associated with the development of SLE. These data support the hypothesis that defective disposal of potentially immunogenic material is a contributory factor in lupus pathogenesis. The identification of polymorphisms that determine basal CRP levels has implications in ischaemic heart disease, where CRP level is an important predictor of risk.

Published

2003

130. UBE2L3 polymorphism amplifies NF-κB activation and promotes plasma cell development, linking linear ubiquitination to multiple autoimmune diseases

Author

Simon Vyse, Myles Lewis, Sebastian Boeltz, Paul J. Lehner, Timothy J. Vyse, Patrick Gordon, Henning Walczak, Tim D. Spector, and Adrian M Shields

Subjects

Plasma cell, Ubiquitin-conjugating enzyme, Real-Time Polymerase Chain Reaction, Polymorphism, Single Nucleotide, Monocytes, Article, Autoimmune Diseases, Ubiquitin, Genetics, medicine, Humans, Genetics(clinical), RNA, Small Interfering, Luciferases, Genetics (clinical), Cells, Cultured, DNA Primers, Autoimmune disease, B-Lymphocytes, CD40, biology, Haplotype, NF-kappa B, Ubiquitination, medicine.disease, NFKB1, Flow Cytometry, Microarray Analysis, 3. Good health, medicine.anatomical_structure, Haplotypes, Immunology, Ubiquitin-Conjugating Enzymes, biology.protein, Tumor necrosis factor alpha, RNA Interference, Genome-Wide Association Study

Abstract

UBE2L3 is associated with increased susceptibility to numerous autoimmune diseases, but the underlying mechanism is unexplained. By using data from a genome-wide association study of systemic lupus erythematosus (SLE), we observed a single risk haplotype spanning UBE2L3, consistently aligned across multiple autoimmune diseases, associated with increased UBE2L3 expression in B cells and monocytes. rs140490 in the UBE2L3 promoter region showed the strongest association. UBE2L3 is an E2 ubiquitin-conjugating enzyme, specially adapted to function with HECT and RING-in-between-RING (RBR) E3 ligases, including HOIL-1 and HOIP, components of the linear ubiquitin chain assembly complex (LUBAC). Our data demonstrate that UBE2L3 is the preferred E2 conjugating enzyme for LUBAC in vivo, and UBE2L3 is essential for LUBAC-mediated activation of NF-κB. By accurately quantifying NF-κB translocation in primary human cells from healthy individuals stratified by rs140490 genotype, we observed that the autoimmune disease risk UBE2L3 genotype was correlated with basal NF-κB activation in unstimulated B cells and monocytes and regulated the sensitivity of NF-κB to CD40 stimulation in B cells and TNF stimulation in monocytes. The UBE2L3 risk allele correlated with increased circulating plasmablast and plasma cell numbers in SLE individuals, consistent with substantially elevated UBE2L3 protein levels in plasmablasts and plasma cells. These results identify key immunological consequences of the UBE2L3 autoimmune risk haplotype and highlight an important role for UBE2L3 in plasmablast and plasma cell development.

Published

2014

131. Reduced Fluorescence versus Forward Scatter Time-of-Flight and Increased Peak versus Integral Fluorescence Ratios Indicate Receptor Clustering in Flow Cytometry

Author

Timothy J. Vyse, Merle Stein, Dirk Mielenz, Benjamin Rhodes, Martin Herrmann, Prabhjoat Chana, Barbara G. Fürnrohr, and Georg Schett

Subjects

Neutrophils, Immunology, Primary Cell Culture, Macrophage-1 Antigen, Receptors, Antigen, B-Cell, Gating, Cell Separation, Biology, Fluorescence, Flow cytometry, Immunoglobulin Fab Fragments, Mice, medicine, Immunology and Allergy, Animals, Humans, Viability assay, Receptor, Cluster analysis, Fluorescent Dyes, B-Lymphocytes, medicine.diagnostic_test, Staining and Labeling, breakpoint cluster region, Carbocyanines, Flow Cytometry, High-Throughput Screening Assays, Mice, Inbred C57BL, Actin Cytoskeleton, Protein Transport, Biophysics, Receptor clustering, Signal transduction

Abstract

Clustering of surface receptors is often required to initiate signal transduction, receptor internalization, and cellular activation. To study the kinetics of clustering, we developed an economic high-throughput method using flow cytometry. The quantification of receptor clustering by flow cytometry is based on the following two observations: first, the fluorescence signal length (FL time-of-flight [ToF]) decreases relative to the forward scatter signal length (FSc-ToF), and second, the peak FL (FL-peak) increases relative to the integral FL (FL-integral) upon clustering of FL-labeled surface receptors. Receptor macroclustering can therefore be quantified using the ratios FL-ToF/FSc-ToF (method ToF) or FL-peak/FL-integral (method Peak). We have used these methods to analyze clustering of two immune receptors known to undergo different conformational and oligomeric states: the BCR and the complement receptor 3 (CR3), on murine splenocytes, purified B cells, and human neutrophils. Engagement of both the BCR and CR3, on immortalized as well as primary murine B cells and human neutrophil, respectively, resulted in decreased FL-ToF/FSc-ToF and increased FL-peak/FL-integral ratios. Manipulation of the actin-myosin cytoskeleton altered BCR clustering which could be measured using the established parameters. To confirm clustering of CR3 on neutrophils, we applied imaging flow cytometry. Because receptor engagement is as a biological process dependent on cell viability, energy metabolism, and temperature, receptor clustering can only be quantified by gating on viable cells under physiological conditions. In summary, with this novel method, receptor clustering on nonadherent cells can easily be monitored by high-throughput conventional flow cytometry.

Published

2014

132. Lupus nephritis susceptibility loci in women with systemic lupus erythematosus

Author

Raphael Zidovetzki, Celine C. Berthier, Jennifer A. Kelly, Michelle Petri, Elizabeth E. Brown, Kathy L. Moser-Sivils, Sharon A. Chung, Timothy W. Behrens, Patrick M. Gaffney, Robert R. Graham, Carl D. Langefeld, M. Ilyas Kamboh, Tushar Bhangale, Adrienne H. Williams, Barry I. Freedman, Deborah S. Cunninghame Graham, Chaim O. Jacob, Marta E. Alarcón-Riquelme, Matthias Kretzler, F. Yesim Demirci, Susan Manzi, John B. Harley, Robert P. Kimberly, Paula S. Ramos, Lindsey A. Criswell, Betty P. Tsao, Laurie P Russell, Timothy J. Vyse, and Jeffrey C. Edberg

Subjects

Adult, Adolescent, Genotype, Population, Lupus nephritis, Genome-wide association study, PDGFRA, Polymorphism, Single Nucleotide, White People, Young Adult, HLA-DR3 Antigen, immune system diseases, medicine, Humans, Lupus Erythematosus, Systemic, Genetic Predisposition to Disease, HLA-DR2 Antigen, RNA, Messenger, education, skin and connective tissue diseases, Child, Genetic association, Aged, education.field_of_study, Systemic lupus erythematosus, business.industry, General Medicine, Middle Aged, medicine.disease, Lupus Nephritis, Phenotype, Basic Research, Nephrology, Immunology, Female, business, Nephritis, Anti-SSA/Ro autoantibodies, Genome-Wide Association Study

Abstract

Lupus nephritis is a manifestation of SLE resulting from glomerular immune complex deposition and inflammation. Lupus nephritis demonstrates familial aggregation and accounts for significant morbidity and mortality. We completed a meta-analysis of three genome-wide association studies of SLE to identify lupus nephritis-predisposing loci. Through genotyping and imputation, >1.6 million markers were assessed in 2000 unrelated women of European descent with SLE (588 patients with lupus nephritis and 1412 patients with lupus without nephritis). Tests of association were computed using logistic regression adjusting for population substructure. The strongest evidence for association was observed outside the MHC and included markers localized to 4q11-q13 (PDGFRA, GSX2; P=4.5×10(-7)), 16p12 (SLC5A11; P=5.1×10(-7)), 6p22 (ID4; P=7.4×10(-7)), and 8q24.12 (HAS2, SNTB1; P=1.1×10(-6)). Both HLA-DR2 and HLA-DR3, two well established lupus susceptibility loci, showed evidence of association with lupus nephritis (P=0.06 and P=3.7×10(-5), respectively). Within the class I region, rs9263871 (C6orf15-HCG22) had the strongest evidence of association with lupus nephritis independent of HLA-DR2 and HLA-DR3 (P=8.5×10(-6)). Consistent with a functional role in lupus nephritis, intra-renal mRNA levels of PDGFRA and associated pathway members showed significant enrichment in patients with lupus nephritis (n=32) compared with controls (n=15). Results from this large-scale genome-wide investigation of lupus nephritis provide evidence of multiple biologically relevant lupus nephritis susceptibility loci.

Published

2014

133. 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

134. MHC associations with clinical and autoantibody manifestations in European SLE

Author

Carl D. Langefeld, David L. Morris, Timothy W. Behrens, Joanne Nititham, Lindsey A. Criswell, K. E. Taylor, Patrick M. Gaffney, Chris Cotsapas, Michael F. Seldin, Bernardo A. Pons-Estel, John B. Harley, R. R. Graham, Michelle M. A. Fernando, Janelle A. Noble, Timothy J. Vyse, John D. Rioux, Peter K. Gregersen, Lisa F. Barcellos, Geoffrey Hom, Sharon A. Chung, Stephen L. Hauser, and Marta E. Alarcón-Riquelme

Subjects

Male, Immunology, Lupus, Genome-wide association study, Human leukocyte antigen, Major histocompatibility complex, Autoimmune Disease, Article, 03 medical and health sciences, 0302 clinical medicine, Genetic, systemic lupus erythematosus, immune system diseases, Models, Clinical Research, Genotype, Genetics, Lupus Erythematosus, Systemic, Humans, 2.1 Biological and endogenous factors, genetics, Systemic Lupus Erythematosus Genetics Consortium, Sub-phenotype analysis, Aetiology, Allele, skin and connective tissue diseases, Genetics (clinical), 030304 developmental biology, Autoantibodies, 030203 arthritis & rheumatology, 0303 health sciences, MHC class II, biology, Models, Genetic, Lupus Erythematosus, Europeans, Inflammatory and immune system, Systemic, Autoantibody, 3. Good health, Europe, meta-analysis, biology.protein, Female, Antibody, MHC, HLA-DRB1 Chains

Abstract

Systemic lupus erythematosus (SLE) is a clinically heterogeneous disease affecting multiple organ systems and characterized by autoantibody formation to nuclear components. Although genetic variation within the major histocompatibility complex (MHC) is associated with SLE, its role in the development of clinical manifestations and autoantibody production is not well defined. We conducted a meta-analysis of four independent European SLE case collections for associations between SLE sub-phenotypes and MHC single-nucleotide polymorphism genotypes, human leukocyte antigen (HLA) alleles and variant HLA amino acids. Of the 11 American College of Rheumatology criteria and 7 autoantibody sub-phenotypes examined, anti-Ro/SSA and anti-La/SSB antibody subsets exhibited the highest number and most statistically significant associations. HLA-DRB1*03:01 was significantly associated with both sub-phenotypes. We found evidence of associations independent of MHC class II variants in the anti-Ro subset alone. Conditional analyses showed that anti-Ro and anti-La subsets are independently associated with HLA-DRB1*0301, and that the HLA-DRB1*03:01 association with SLE is largely but not completely driven by the association of this allele with these sub-phenotypes. Our results provide strong evidence for a multilevel risk model for HLA-DRB1*03:01 in SLE, where the association with anti-Ro and anti-La antibody-positive SLE is much stronger than SLE without these autoantibodies. © 2014 Macmillan Publishers Limited.

Published

2014

135. Evidence for an Interferon-Inducible Gene, Ifi202, in the Susceptibility to Systemic Lupus

Author

Gary Peltz, Timothy J. Vyse, John Allard, Divaker Choubey, Brian L. Kotzin, Shozo Izui, and Stephen J. Rozzo

Subjects

Candidate gene, Immunology, Congenic, Lupus nephritis, Locus (genetics), Apoptosis, Biology, Mice, immune system diseases, medicine, Animals, Lupus Erythematosus, Systemic, Immunology and Allergy, Genetic Predisposition to Disease, Promoter Regions, Genetic, skin and connective tissue diseases, Gene, Oligonucleotide Array Sequence Analysis, Ifi202, Mice, Inbred BALB C, Polymorphism, Genetic, Mice, Inbred NZB, Autoantibody, Intracellular Signaling Peptides and Proteins, Chromosome Mapping, medicine.disease, Phosphoproteins, Molecular biology, Gene expression profiling, Mice, Inbred C57BL, Infectious Diseases, Female, Carrier Proteins

Abstract

The Nba2 locus is a major genetic contribution to disease susceptibility in the (NZB × NZW)F 1 mouse model of systemic lupus. We generated C57BL/6 mice congenic for this NZB locus, and these mice produced antinuclear autoantibodies characteristic of lupus. F 1 offspring of congenic and NZW mice developed high autoantibody levels and severe lupus nephritis similar to (NZB × NZW)F 1 mice. Expression profiling with oligonucleotide microarrays revealed only two differentially expressed genes, interferon-inducible genes Ifi202 and Ifi203 , in congenic versus control mice, and both were within the Nba2 interval. Quantitative PCR localized increased Ifi202 expression to splenic B cells and non-T/non-B cells. These results, together with analyses of promoter region polymorphisms, strain distribution of expression, and effects on cell proliferation and apoptosis, implicate Ifi202 as a candidate gene for lupus.

Published

2001

136. Autoantigen Glycoprotein 70 Expression Is Regulated by a Single Locus, Which Acts as a Checkpoint for Pathogenic Anti-Glycoprotein 70 Autoantibody Production and Hence for the Corresponding Development of Severe Nephritis, in Lupus-Prone BXSB Mice1

Author

Akinori Ida, Shozo Izui, EM Thompson, Aileen McDermott, Bernard J Morley, Michelle E. K. Haywood, Timothy J. Vyse, and Mark Walport

Subjects

chemistry.chemical_classification, education.field_of_study, viruses, Immunology, Population, Autoantibody, Locus (genetics), Biology, medicine.disease, Immune system, chemistry, immune system diseases, medicine, Immunology and Allergy, skin and connective tissue diseases, Glycoprotein, education, Autoantibody production, Nephritis, Chromosome 13

Abstract

Retroviral envelope glycoprotein gp70 is present in the sera of immunologically normal and autoimmune-prone strains of mice. However, only lupus-prone mice spontaneously develop gp70-anti-gp70 immune complexes (gp70IC), and these have been implicated in the development of nephritis. We investigated the genetic factors that affect the production of both free serum gp70 and gp70IC in the lupus-prone BXSB mouse strain by analyzing (BXSB × (C57BL/10 × BXSB)F1)- and (C57BL/10 × (C57BL/10 × BXSB)F1)-backcrossed male mice. Production of gp70 mapped to a single major locus located on chromosome 13 (Bxs6) with a maximum log likelihood of the odds of 36.7 (p = 1.6 × 10−38). The level of gp70IC was highly dependent on Bxs6-related gp70 production, and high titer autoantibody production only occurred when serum gp70 levels were greater than a threshold value of ∼4.0 μg/ml. The subdivision of the (BXSB × (C57BL/10 × BXSB)F1)-backcrossed mice into those homozygous or heterozygous for Bxs6 enabled a remarkable association to be observed between high levels of gp70IC and severe nephritis in the Bxs6 homozygote population. A further mapping study in these two subgroups identified a previously unrecognized interval associated with the production of autoantibodies.

Published

2001

137. The Genetics of SystemicLupus erythe matosus

Author

Cheri A. Roberton and Timothy J. Vyse

Subjects

Genetic Markers, Systemic disease, Genetic Linkage, Physiology, medicine.disease_cause, Linkage Disequilibrium, Genetic determinism, Autoimmunity, Major Histocompatibility Complex, Mice, immune system diseases, Immunopathology, Genetics, medicine, Genetic predisposition, Animals, Humans, Lupus Erythematosus, Systemic, Genetic Predisposition to Disease, skin and connective tissue diseases, Autoimmune disease, Lupus erythematosus, business.industry, General Medicine, medicine.disease, Connective tissue disease, Nephrology, Immunology, business

Abstract

Background: There is a genetic predisposition to human systemic lupus erythematosus (SLE). The genes that contribute to susceptibility are, for the most part, unknown. The introduction of new gene mapping techniques has opened the way to explore lupus genetics on a genome-wide basis. Methods: Microsatellites are simple sequence repeats widely distributed throughout eukaryotic genomes. They exhibit length variation. This polymorphism can be exploited to provide a panoply of genome-wide markers. Thereby, loci linked with lupus have been mapped in lupus-prone mouse strains and in recently published studies in multi-case human families. Results: More than 20 non-MHC (major histocompatibility complex) loci have now been linked with murine lupus. Nine non-MHC loci have been corroborated in human SLE. Some of the mouse intervals are syntenic with human loci raising the tantalizing possibility of common suspectibility genes. Although we await the results of formal gene identification, functional studies in back-cross and congenic analyses indicate that, in the mouse at least, disease genes act at multiple levels in disease development. Conclusions: A large number of genes are involved in the pathogenesis of SLE. The data also suggest that even the MHC contribution is multiple. Having mapped disease loci, geneticists now face the task of closing down on the actual aetiological alleles and demonstrating how they might operate. This undertaking will add significantly to our understanding of disease development.

Published

2000

138. Analysis of MHC Class II Genes in the Susceptibility to Lupus in New Zealand Mice

Author

Stephen J. Rozzo, Timothy J. Vyse, Chella S. David, Ed Palmer, Shozo Izui, and Brian L. Kotzin

Subjects

Immunology, Immunology and Allergy

Abstract

Hybrids of New Zealand Black (NZB) and New Zealand White (NZW) mice spontaneously develop a disease similar to human systemic lupus erythematosus. MHC and non-MHC genes contribute to disease susceptibility in this murine model. Multiple studies have shown that the NZW H2z locus is strongly associated with the development of lupus-like disease in these mice. The susceptibility gene(s) within H2z is not known, but different lines of evidence have pointed to class II MHC genes, either H2-E or H2-A (Ez or Az in NZW). Recent studies from our laboratory showed that Ez does not supplant H2z in the contribution to lupus-like disease. In the present work we generated C57BL/10 (B10) mice transgenic for Aaz and Abz genes (designated B10.Az mice) and used a (B10.Az × NZB)F1 × NZB backcross to assess the contributions of Az genes to disease. A subset of backcross mice produced high levels of IgG autoantibodies and developed severe nephritis. However, no autoimmune phenotype was linked to the Az transgenes. Surprisingly, in the same backcross mice, inheritance of H2b from the nonautoimmune B10 strain was strongly linked with both autoantibody production and nephritis. Taken together with our previous Ez studies, the present work calls into question the importance of class II MHC genes for lupus susceptibility in this model and provides new insight into the role of MHC in lupus-like autoimmunity.

Published

1999

139. Thymic Microenvironment and NZB Mice: The Abnormal Thymic Microenvironment of New Zealand Mice Correlates with Immunopathology

Author

Jin Emon Konishi, Nobuhisa Taguchi, Richard L. Boyd, Mitsuru Naiki, Brian L. Kotzin, Leonard D. Shultz, Sean R. Bennett, Yuichi Takeoka, M. Eric Gershwin, Timothy J. Vyse, and Aftab A. Ansari

Subjects

Pathology, medicine.medical_specialty, Immunology, DNA, Single-Stranded, Autoimmunity, Thymus Gland, Biology, urologic and male genital diseases, medicine.disease_cause, Mice, immune system diseases, Immunopathology, medicine, Animals, Immunology and Allergy, Genetic Predisposition to Disease, skin and connective tissue diseases, Crosses, Genetic, Autoimmune disease, Polymorphism, Genetic, Systemic lupus erythematosus, Mice, Inbred NZB, Autoantibody, DNA, medicine.disease, Lupus Nephritis, Immunoglobulin Isotypes, Chromosome 17 (human), Proteinuria, Chromosome 4, Immunoglobulin G, Nephritis

Abstract

There are distinct microenvironmental abnormalities of thymic architecture in several murine models of SLE defined using immunohistochemistry and a panel of mAb dissected at thymic epithelial markers. To address the issue of the relationship between the thymic microenvironment and autoimmunity, we studied backcross (NZB × NZW) F1 × NZW mice in which 50% of offspring develop nephritis associated with proteinuria and anti-DNA antibodies. We reasoned that if thymic abnormalities are associated with development of disease, the correlation of abnormalities with lupus-like disease in individual backcross mice will form the foundation for identification of the mechanisms involved. In parallel, we directed a genetic linkage analysis, using markers previously shown to be linked to nephritis and IgG autoantibody production, to determine if such loci were similarly associated with microenvironmental changes. Our data demonstrate that all (NZB × NZW) F1 × NZW backcross mice with disease have microenvironmental defects. Although the microenvironmental defects are not sufficient for development of autoimmune disease, the severity of thymic abnormalities correlates with titers of IgG autoantibodies to DNA and with proteinuria. Consistent with past studies of (NZB × NZW) F1 × NZW mice, genetic markers on proximal chromosome 17 (near MHC) and distal chromosome 4 showed trends for linkage with nephritis. Although the markers chosen only covered about 10–15% of the genome, the results demonstrated trends for linkage with thymic medullary abnormalities for loci on distal chromosome 4 and distal chromosome 1. We believe it will be important to define the biochemical nature of the molecules recognized by these mAbs to understand the relationships between thymic architecture and immunopathology.

Published

1999

140. Understanding Lupus: Fishing Genes Out of Mice and Men

Author

Timothy J. Vyse

Subjects

Systemic lupus erythematosus, animal diseases, Immunology, Systemic autoimmunity, Biology, medicine.disease, Infectious Diseases, immune system diseases, Immunity, medicine, Immunology and Allergy, skin and connective tissue diseases, Gene

Abstract

In this issue of Immunity, the Coronin-1A gene Coro1a, which regulates cytoskeletal structure, is shown by Haraldsson et al. (2007) to be a surprising disease-susceptibility gene that contributes to the spontaneous systemic autoimmunity in the MRL mouse, a model of systemic lupus erythematosus.

Published

2008

141. Contributions ofEazandEbzMHC Genes to Lupus Susceptibility in New Zealand Mice

Author

Timothy J. Vyse, Stephen J. Rozzo, Charles G. Drake, Virginia B. Appel, Marianne Lemeur, Shozo Izui, Ed Palmer, and Brian L. Kotzin

Subjects

Immunology, Immunology and Allergy

Abstract

Unlike parental New Zealand Black (NZB) or New Zealand White (NZW) mice, (NZB × NZW)F1 mice exhibit a lupus-like disease characterized by IgG autoantibody production and severe immune complex-mediated nephritis. In studies of the genetic susceptibility to disease in this F1 model, the NZW MHC (H2z) has been strongly linked with the development of disease, and it was hypothesized that class II MHC genes, particularly Ez genes, may underlie this genetic contribution. In the present study, we bred transgenic B6 mice expressing I-Ez or congenic B6 mice carrying H2z with NZB mice and used a backcross analysis to test the hypothesis that Eaz and/or Ebz genes account for the effect of H2z on disease. The genetic analysis of different backcross combinations showed that unlike mice carrying H2z, mice inheriting Ez transgenes do not demonstrate increased IgG autoantibody production or increased incidence of nephritis. Surprisingly, in the same transgenic backcross mice, inheritance of the endogenous H2b from the B6 strain was strongly linked with the production of IgG autoantibodies, but not with disease. Additional experiments suggested that the level of IgG3 autoantibody production, which is controlled by H2, may be important in the pathogenesis of renal disease. Contributions to autoantibody production were also detected from an NZB locus on distal chromosome 1 (previously named Nba2). Together, these studies provide new insight into the role of MHC in lupus-like autoimmunity.

Published

1998

142. Genetics of connective tissue diseases

Author

Timothy J. Vyse and Myles Lewis

Subjects

Pathology, medicine.medical_specialty, medicine.anatomical_structure, medicine, Connective tissue, Biology

Abstract

The advent of genome-wide association studies (GWAS) has been an exciting breakthrough in our understanding of the genetic aetiology of autoimmune diseases. Substantial overlap has been found in susceptibility genes across multiple diseases, from connective tissue diseases and rheumatoid arthritis (RA) to inflammatory bowel disease, coeliac disease, and psoriasis. Major technological advances now permit genotyping of millions of single nucleotide polymorphisms (SNPs). Group analysis of SNPs by haplotypes, aided by completion of the Hapmap project, has improved our ability to pinpoint causal genetic variants. International collaboration to pool large-scale cohorts of patients has enabled GWAS in systemic lupus erythematosus (SLE), systemic sclerosis and Behçet’s disease, with studies in progress for ANCA-associated vasculitis. These ’hypothesis-free’ studies have revealed many novel disease-associated genes. In both SLE and systemic sclerosis, identified genes map to known pathways including antigen presentation (MHC, TNFSF4), autoreactivity of B and T lymphocytes (BLK, BANK1), type I interferon production (STAT4, IRF5) and the NFκ‎‎B pathway (TNIP1). In SLE alone, additional genes appear to be involved in dysregulated apoptotic cell clearance (ITGAM, TREX1, C1q, C4) and recognition of immune complexes (FCGR2A, FCGR3B). Future developments include whole-genome sequencing to identify rare variants, and efforts to understand functional consequences of susceptibility genes. Putative environmental triggers for connective tissue diseases include infectious agents, especially Epstein-Barr virus; cigarette smoking; occupational exposure to toxins including silica; and low vitamin D, due to its immunomodulatory effects. Despite numerous studies looking at toxin exposure and connective tissue diseases, conclusive evidence is lacking, due to either rarity of exposure or rarity of disease.

Published

2013

143. PTPN22 association in systemic lupus erythematosus (SLE) with respect to individual ancestry and clinical sub-phenotypes

Author

Luis M. Vilá, Juan-Manuel Anaya, Bahram Namjou, Graciela S. Alarcón, John B. Harley, Jeffrey C. Edberg, Marta E. Alarcón-Riquelme, Elizabeth E. Brown, R. H. Scofield, Timothy B. Niewold, Jiyoung Choi, Carl D. Langefeld, Robert P. Kimberly, Barry I. Freedman, Betty P. Tsao, Swapan K. Nath, Jennifer A. Kelly, Bernardo A. Pons-Estel, John D. Reveille, Kenneth M. Kaufman, Joel M. Guthridge, Kathy L. Sivils, Susan A. Boackle, Judith A. James, Timothy J. Vyse, Patrick M. Gaffney, Lindsey A. Criswell, Jaehoon Kim, Sharon A. Chung, Chaim O. Jacob, Michelle Petri, Sang Cheol Bae, Joan T. Merrill, Adam Adler, Stuart B. Glenn, Xana Kim-Howard, Rosalind Ramsey-Goldman, Celi Sun, and Gary S. Gilkeson

Subjects

Linkage disequilibrium, US Department of Veterans Affairs Medical Center, Heredity, Non-Clinical Medicine, Oklahoma Medical Research Foundation, lcsh:Medicine, Genome-wide association study, Linkage Disequilibrium, Cincinnati Children’s Hospital Medical Center, 0302 clinical medicine, Gene Frequency, Rosalind Russell Medical Research Center for Arthritis, Lupus Erythematosus, Systemic, University of Puerto Rico Medical Sciences Campus, lcsh:Science, University of Oklahoma Health Sciences Center, 0303 health sciences, Multidisciplinary, Hispanic or Latino, PTPN22, Ethnic Differences, 3. Good health, Division of Rheumatology, Phenotype, Northwestern University Feinberg School of Medicine, Medicine, Research Article, Genotype, Genotypes, Inmunología, Single-nucleotide polymorphism, Biology, Department of Internal Medicine, Polymorphism, Single Nucleotide, Systemic Lupus Erythematosus, White People, Autoimmune Diseases, 03 medical and health sciences, Johns Hopkins University School of Medicine, Rheumatology, Arthritis and Clinical Immunology Research Program, University of Texas Health Science Center at Houston, Lupus eritematoso sistémico, University of Alabama at Birmingham, medicine, Genetics, Humans, Genetic Predisposition to Disease, Allele frequency, 030304 developmental biology, Genetic association, 030203 arthritis & rheumatology, Lupus erythematosus, Health Care Policy, Asian, Lupus Erythematosus, lcsh:R, Autoantibody, Computational Biology, Protein Tyrosine Phosphatase, Non-Receptor Type 22, medicine.disease, Department of Medicine, Enfermedades, Black or African American, Logistic Models, Haplotypes, Antibodies, Anticardiolipin, Immunoglobulin G, Immunology, Genetic Polymorphism, lcsh:Q, Clinical Immunology, Population Genetics

Abstract

Protein tyrosine phosphatase non-receptor type 22 (PTPN22) is a negative regulator of T-cell activation associated with several autoimmune diseases, including systemic lupus erythematosus (SLE). Missense rs2476601 is associated with SLE in individuals with European ancestry. Since the rs2476601 risk allele frequency differs dramatically across ethnicities, we assessed robustness of PTPN22 association with SLE and its clinical sub-phenotypes across four ethnically diverse populations. Ten SNPs were genotyped in 8220 SLE cases and 7369 controls from in European-Americans (EA), African-Americans (AA), Asians (AS), and Hispanics (HS). We performed imputation-based association followed by conditional analysis to identify independent associations. Significantly associated SNPs were tested for association with SLE clinical sub-phenotypes, including autoantibody profiles. Multiple testing was accounted for by using false discovery rate. We successfully imputed and tested allelic association for 107 SNPs within the PTPN22 region and detected evidence of ethnic-specific associations from EA and HS. In EA, the strongest association was at rs2476601 (P = 4.7 × 10(-9), OR = 1.40 (95% CI = 1.25-1.56)). Independent association with rs1217414 was also observed in EA, and both SNPs are correlated with increased European ancestry. For HS imputed intronic SNP, rs3765598, predicted to be a cis-eQTL, was associated (P = 0.007, OR = 0.79 and 95% CI = 0.67-0.94). No significant associations were observed in AA or AS. Case-only analysis using lupus-related clinical criteria revealed differences between EA SLE patients positive for moderate to high titers of IgG anti-cardiolipin (aCL IgG >20) versus negative aCL IgG at rs2476601 (P = 0.012, OR = 1.65). Association was reinforced when these cases were compared to controls (P = 2.7 × 10(-5), OR = 2.11). Our results validate that rs2476601 is the most significantly associated SNP in individuals with European ancestry. Additionally, rs1217414 and rs3765598 may be associated with SLE. Further studies are required to confirm the involvement of rs2476601 with aCL IgG.

Published

2013

144. Admixture Mapping in Lupus Identifies Multiple Functional Variants within IFIH1 Associated with Apoptosis, Inflammation, and Autoantibody Production

Author

Elizabeth E. Brown, Julio E. Molineros, Kathy L. Moser, Stuart B. Glenn, Judith A. James, Jeffrey C. Edberg, Timothy B. Niewold, Adam Adler, Shizhong Han, Marta E. Alarcón-Riquelme, Barry I. Freedman, Robert P. Kimberly, Jennifer A. Kelly, Xana Kim-Howard, Michelle Petri, Gary S. Gilkeson, Betty P. Tsao, Lindsey A. Criswell, Loren L. Looger, Chaim O. Jacob, John B. Harley, Kenneth M. Kaufman, Rosalind Ramsey-Goldman, Timothy J. Vyse, Joel M. Guthridge, Jason H. Moore, Celi Sun, Swapan K. Nath, Scott M. Williams, John D. Reveille, Patrick M. Gaffney, Luis M. Vilá, Graciela S. Alarcón, C. Langefeld, Joan T. Merrill, R. Hal Scofield, and Amit K. Maiti

Subjects

Cancer Research, Interferon-Induced Helicase, IFIH1, Gene Expression, Apoptosis, DEAD-box RNA Helicases, 0302 clinical medicine, Genotype, Molecular Cell Biology, Lupus Erythematosus, Systemic, Genetics (clinical), Genetics, 0303 health sciences, Ku70, Systemic lupus erythematosus, Chromosome Mapping, Antigens, Nuclear, 3. Good health, DNA-Binding Proteins, 030220 oncology & carcinogenesis, Intronic SNP, Research Article, Protein Binding, lcsh:QH426-470, Genetic admixture, Biology, Polymorphism, Single Nucleotide, White People, Molecular Genetics, 03 medical and health sciences, Genetic predisposition, medicine, Humans, Genetic Predisposition to Disease, Allele, Molecular Biology, Ku Autoantigen, Ecology, Evolution, Behavior and Systematics, Alleles, 030304 developmental biology, Autoantibodies, Inflammation, Genome, Human, Autoantibody, medicine.disease, Molecular biology, Black or African American, lcsh:Genetics, Haplotypes, Genetics of Disease, Population Genetics

Abstract

Systemic lupus erythematosus (SLE) is an inflammatory autoimmune disease with a strong genetic component. African-Americans (AA) are at increased risk of SLE, but the genetic basis of this risk is largely unknown. To identify causal variants in SLE loci in AA, we performed admixture mapping followed by fine mapping in AA and European-Americans (EA). Through genome-wide admixture mapping in AA, we identified a strong SLE susceptibility locus at 2q22–24 (LOD = 6.28), and the admixture signal is associated with the European ancestry (ancestry risk ratio ∼1.5). Large-scale genotypic analysis on 19,726 individuals of African and European ancestry revealed three independently associated variants in the IFIH1 gene: an intronic variant, rs13023380 [Pmeta = 5.20×10−14; odds ratio, 95% confidence interval = 0.82 (0.78–0.87)], and two missense variants, rs1990760 (Ala946Thr) [Pmeta = 3.08×10−7; 0.88 (0.84–0.93)] and rs10930046 (Arg460His) [Pdom = 1.16×10−8; 0.70 (0.62–0.79)]. Both missense variants produced dramatic phenotypic changes in apoptosis and inflammation-related gene expression. We experimentally validated function of the intronic SNP by DNA electrophoresis, protein identification, and in vitro protein binding assays. DNA carrying the intronic risk allele rs13023380 showed reduced binding efficiency to a cellular protein complex including nucleolin and lupus autoantigen Ku70/80, and showed reduced transcriptional activity in vivo. Thus, in SLE patients, genetic susceptibility could create a biochemical imbalance that dysregulates nucleolin, Ku70/80, or other nucleic acid regulatory proteins. This could promote antibody hypermutation and auto-antibody generation, further destabilizing the cellular network. Together with molecular modeling, our results establish a distinct role for IFIH1 in apoptosis, inflammation, and autoantibody production, and explain the molecular basis of these three risk alleles for SLE pathogenesis., Author Summary African-Americans (AA) are at increased risk of systemic lupus erythematosus (SLE), but the genetic basis of this risk increase is largely unknown. We used admixture mapping to localize disease-causing genetic variants that differ in frequency across populations. This approach is advantageous for localizing susceptibility genes in recently admixed populations like AA. Our genome-wide admixture scan identified seven admixture signals, and we followed the best signal at 2q22–24 with fine-mapping, imputation-based association analysis and experimental validation. We identified two independent coding variants and a non-coding variant within the IFIH1 gene associated with SLE. Together with molecular modeling, our results establish a distinct role for IFIH1 in apoptosis, inflammation, and autoantibody production, and explain the molecular basis of these three risk alleles for SLE pathogenesis.

Published

2013

145. Genomic Pathology of SLE-Associated Copy-Number Variation at the FCGR2C/FCGR3B/FCGR2B Locus

Author

Michael Mueller, Chack-Yung Yu, Timothy J. Vyse, Paula Barros, R. Andres Floto, H. Terence Cook, Evan E. Eichler, Helmut Schaschl, Amy L. Roberts, Timothy J. Aitman, Karyn Meltz Steinberg, Matthew E. Hurles, Laurence Game, Richard K. Wilson, Abigail S. Witherden, Zhou Zhang, Catherine Schaffner, and Tina Graves

Subjects

Pathology, medicine.medical_specialty, DNA Copy Number Variations, Non-allelic homologous recombination, Locus (genetics), Biology, GPI-Linked Proteins, Polymorphism, Single Nucleotide, Article, 03 medical and health sciences, 0302 clinical medicine, medicine, Genetics, Humans, Lupus Erythematosus, Systemic, Genetics(clinical), Genetic Predisposition to Disease, Copy-number variation, Allele, Gene, Genetics (clinical), 030304 developmental biology, 0303 health sciences, Bacterial artificial chromosome, Haplotype, Receptors, IgG, Chromosome Mapping, Fosmid, Killer Cells, Natural, Gene Deletion, 030215 immunology

Abstract

Reduced FCGR3B copy number is associated with increased risk of systemic lupus erythematosus (SLE). The five FCGR2/FCGR3 genes are arranged across two highly paralogous genomic segments on chromosome 1q23. Previous studies have suggested mechanisms for structural rearrangements at the FCGR2/FCGR3 locus and have proposed mechanisms whereby altered FCGR3B copy number predisposes to autoimmunity, but the high degree of sequence similarity between paralogous segments has prevented precise definition of the molecular events and their functional consequences. To pursue the genomic pathology associated with FCGR3B copy-number variation, we integrated sequencing data from fosmid and bacterial artificial chromosome clones and sequence-captured DNA from FCGR3B-deleted genomes to establish a detailed map of allelic and paralogous sequence variation across the FCGR2/FCGR3 locus. This analysis identified two highly paralogous 24.5 kb blocks within the FCGR2C/FCGR3B/FCGR2B locus that are devoid of nonpolymorphic paralogous sequence variations and that define the limits of the genomic regions in which nonallelic homologous recombination leads to FCGR2C/FCGR3B copy-number variation. Further, the data showed evidence of swapping of haplotype blocks between these highly paralogous blocks that most likely arose from sequential ancestral recombination events across the region. Functionally, we found by flow cytometry, immunoblotting and cDNA sequencing that individuals with FCGR3B-deleted alleles show ectopic presence of FcγRIIb on natural killer (NK) cells. We conclude that FCGR3B deletion juxtaposes the 5′-regulatory sequences of FCGR2C with the coding sequence of FCGR2B, creating a chimeric gene that results in an ectopic accumulation of FcγRIIb on NK cells and provides an explanation for SLE risk associated with reduced FCGR3B gene copy number.

Published

2013

146. Systemic Lupus Erythematosus

Author

Timothy J. Vyse and Benjamin Rhodes

Subjects

business.industry, Medicine, Personalized medicine, Computational biology, business

Published

2013

147. Contributors

Author

Michael J. Ackerman, Minhaz Uddin Ahmed, Sun Hee Ahn, R. Rand Allingham, Jude Alsarraj, Matthew L. Anderson, Brian H. Annex, Christina K. Augustine, Sergio E. Baranzini, Peter J. Barnes, Georgia M. Beasley, Richard C. Becker, Ivor J. Benjamin, D. Woodrow Benson, Jacob Fog Bentzon, Philip S. Bernard, Lars Bertram, Laura M. Beskow, Brigitta Bondy, J. Martijn Bos, Gabriella L. Boulting, Jerome S. Brody, April S. Brown, Kenneth H. Buetow, Lars Bullinger, Atul J. Butte, David J. Carey, George Carlson, David Chen, Maria Chahrour, E. Antonio Chiocca, Alex H. Cho, Carolyn Compton, Robert Cook-Deegan, Nicholas Craddock, Michael Coulter, Samir B. Damani, Jacqueline S. Danik, Sandeep Dave, Russell Dedrick, Frank R. DeLeo, Eleftherios P. Diamandis, Ayotunde O. Dokun, Gregory J. Downing, Stephen L. Eck, Lucas B. Edelman, Kevin C. Eggan, Erling Falk, Hawazin Faruki, Junjie Feng, Eleanora Anna Margaretha Festen, Jose C. Florez, Vance G. Fowler, Jennifer A. Freedman, Hudson H. Freeze, Stefan Fröhling, David J. Galas, Glenn S. Gerhard, Daniel H. Geschwind, Ad Geurts van Kessel, Robert B. Giffin, Geoffrey S. Ginsburg, Megan Goodall, Praveen Govender, Robert C. Green, Chris Gunter, Marta Gwinn, Susanne B. Haga, James R. Heath, Robert A. Hegele, John Holton, Leroy Hood, Kent W. Hunter, Daehee Hwang, Gail Javitt, Gina Jefferson, Sam John, Keith J. Johnson, Toby Johnson, Tisha R. Joy, Sekar Kathiresan, Hasmeena Kathuria, Arabindra B. Katwal, Kensaku Kawamoto, Andrea Kelly, Muin J. Khoury, Jin Woo Kim, Stephen F. Kingsmore, Tod Klingler, Scott D. Kobayashi, Isaac S. Kohane, Virginia Byers Kraus, Roland P. Kuiper, Myla Lai-Goldman, Neil E. Lamb, Sevdalina Nikolova Lambova, Matthew B. Lanktree, Sean E. Lawler, David H. Ledbetter, Charles Lee, Inyoul Lee, Karine G. Le Roch, Samuel Levy, Sophie Limou, Wennuan Liu, Yutao Liu, Barry London, Jeffrey P. MacKeigan, Elaine R. Mardis, Hector Marquez, Marco Marra, Christa Lese Martin, Lisa J. Martin, Steven A. McCarroll, John McHutchison, Howard L. McLeod, Asunción Mejías, Eric B. Meltzer, M. Anthony Moody, Ryan D. Morin, M. Arthur Moseley, Joanna L. Mountain, Ulf Müller-Ladner, Patricia B. Munroe, Bobby G. Ng, Paul W. Noble, Michael C. O’Donovan, Kunle Odunsi, Gilbert S. Omenn, Steve R. Ommen, Lori A. Orlando, Albert D.M.E. Osterhaus, Michael J. Owen, Neelroop N. Parikshak, Keyur Patel, Maria P. Pavlou, Nina P. Paynter, Tanja Pejovic, Michael X. Pham, Robert M. Plenge, Mihai V. Podgoreanu, Nadia Ponts, Nathan D. Price, Bruce Quinn, Francisco J. Quintana, Daniel J. Rader, Octavio Ramilo, Heidi L. Rehm, Benjamin Rhodes, Paul M. Ridker, Erin Rooney Riggs, Jeffrey S. Ross, Wendy S. Rubinstein, Carol J. Saunders, Joan Scott, Nicholas A. Shackel, Svati H. Shah, Richard Simon, Sanjay M. Sisodiya, Saskia L. Smits, John A. Stamatoyannopoulos, Glenn D. Steele, Mark P. Steele, Tessandra Stewart, Giovana R. Thomas, Eric J. Topol, Sean R. Tunis, Aubrey R. Turner, Douglas S. Tyler, David L. Veenstra, Ramprasath Venkatachalam, Deepak Voora, Timothy J. Vyse, Christopher A. Walsh, Katherine Walsh, Hao Wang, Jun Wang, Rinse K. Weersma, Howard L. Weiner, Scott T. Weiss, C. William Wester, David N. Wholley, Janey L. Wiggs, Cisca Wijmenga, Huntington F. Willard, Hywel J. Williams, Marc S. Williams, Cheryl A. Winkler, Janet Woodcock, Christopher W. Woods, Pae C. Wu, Jianfeng Xu, James Yee, Hyuntae Yoo, Timothy Yu, Jing Zhang, and Yurong Zhang

Published

2013

148. Variants at multiple loci implicated in both innate and adaptive immune responses are associated with Sjögren's syndrome

Author

Glen D Houston, Ketan Patel, Jacen S. Maier-Moore, Rajaram Gopalakrishnan, Deborah S. Cunninghame Graham, Erna Harboe, Pamela J. Hughes, Roald Omdal, Corinne Miceli-Richard, Wan-Fai Ng, Patrick M. Gaffney, A. Darise Farris, Kenneth M. Kaufman, Courtney G. Montgomery, Gunnel Nordmark, Mikhail G. Dozmorov, Joel M. Guthridge, James A. Lessard, David M Lewis, Kathy L. Sivils, Per Eriksson, Juan-Manuel Anaya, Maureen Rischmueller, Barbara M. Segal, Xavier Mariette, Jonathan D. Wren, Simon J. Bowman, Adam Adler, Johan G. Brun, Kiely Grundahl, Lasse G. Gøransson, Astrid Rasmussen, Nelson L. Rhodus, Abu N. M. Nazmul-Hossain, Michael D. Rohrer, Michael T. Brennan, James Chodosh, He Li, Jennifer A. Kelly, Kimberly S. Hefner, Torsten Witte, Gabor G. Illei, Judith A. James, Susan C. Lester, R. Hal Scofield, Roland Jonsson, Indra Adrianto, Christopher J. Lessard, Marie Wahren-Herlenius, Maija-Leena Eloranta, Lida Radfar, Lars Rönnblom, Martha E. Grandits, John A. Ice, Donald U. Stone, Andrew J.W. Huang, Helmi Jazebi, John B. Harley, Marika Kvarnström, Timothy J. Vyse, University of Oklahoma Health Sciences Center (OUHSC), Macquarie University, Service de rhumatologie, Université Paris-Sud - Paris 11 (UP11)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Hôpital Bicêtre, New Queen Elizabeth Hospital (NQEH - BIRMINGHAM), New Queen Elisabeth Hospital, Marine Science Institute, University of California, Department of Medical Sciences, Université de Genève (UNIGE), Institute of Sound and Vibration Research, University of Southampton, Centre for Cybersecurity and Cybercrime Investigation [Dublin] (CCI ), University College Dublin [Dublin] (UCD), Computing and Mathematical Sciences [Pasadena]], California Institute of Technology (CALTECH), Zhejiang University, Laboratoire de l'intégration, du matériau au système (IMS), Université Sciences et Technologies - Bordeaux 1-Institut Polytechnique de Bordeaux-Centre National de la Recherche Scientifique (CNRS), Climate Systems Analysis Group [Cape Town] (CSAG), University of Cape Town, Faculty of Medicine, Section of Rheumatology, Imperial College London, Department of Pathology, University of California [San Diego] (UC San Diego), University of California-University of California, Department of Pathology, Immunology and Microbiology, University of California [Davis] (UC Davis), Swedish Defence Research Agency [Stockholm] (FOI), Department of Public Health & Policy, London School of Hygiene and Tropical Medicine (LSHTM), University of Alberta, Centre d'Investigation Clinique (CIC - Brest), Université de Brest (UBO)-Institut National de la Santé et de la Recherche Médicale (INSERM), Lymphocytes B, Autoimmunité et Immunothérapies (LBAI), Université de Brest (UBO)-Institut National de la Santé et de la Recherche Médicale (INSERM)-LabEX IGO Immunothérapie Grand Ouest-Institut Brestois Santé Agro Matière (IBSAM), Université de Brest (UBO), CHRU Brest - Service de Rhumatologie (CHU - BREST - Rhumato), Centre Hospitalier Régional Universitaire de Brest (CHRU Brest), Hôpital Bicêtre-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Université Paris-Sud - Paris 11 (UP11), Lymphocyte B et Auto-immunité (LBAI), and Université de Brest (UBO)-Institut Brestois Santé Agro Matière (IBSAM)

Subjects

[SDV]Life Sciences [q-bio], Intron, Genome-wide association study, HLA DR antigen, Adaptive Immunity, TNFAIP3, Gene locus, 0302 clinical medicine, IL12A, STAT4 protein, Haplotype, Innate, MESH: Genetic Variation, Interferon regulatory factor 5, STAT4, MESH: Genetic Association Studies, Priority journal, Genetics, Innate immunity, 0303 health sciences, HLA DQB1 antigen, Acquired immune system, Chromatin immunoprecipitation, 3. Good health, Securin, Sjogren's Syndrome, [SDV.MHEP.RSOA]Life Sciences [q-bio]/Human health and pathology/Rhumatology and musculoskeletal system, MESH: Immunity, Innate, HLA system, Human, Adaptive immunity, Case control study, Human leukocyte antigen, Major clinical study, Biology, FCGR2A, MESH: Genetic Loci, Article, HLA DQA1 antigen, 03 medical and health sciences, medicine, Humans, Genetic Association Studies, 030304 developmental biology, 030203 arthritis & rheumatology, Autoimmune disease, Interleukin 12p35, MESH: Humans, Chromosome 8, B lymphocyte induced maturation protein 1, Histocompatibility Antigens Class II, Immunity, Genetic Variation, medicine.disease, Gene frequency, Immunity, Innate, MESH: Sjogren's Syndrome, Genetic Loci, Immunology, Chemokine receptor CXCR5, MESH: Histocompatibility Antigens Class II, Genetic association, Meta analysis (topic), Protein protein interaction, Genetic variability, Controlled study, Sjoegren syndrome, MESH: Adaptive Immunity, [SDV.MHEP]Life Sciences [q-bio]/Human health and pathology

Abstract

Sjögren's syndrome is a common autoimmune disease (affecting ?0.7% of European Americans) that typically presents as keratoconjunctivitis sicca and xerostomia. Here we report results of a large-scale association study of Sjögren's syndrome. In addition to strong association within the human leukocyte antigen (HLA) region at 6p21 (P meta = 7.65 × 10 -114), we establish associations with IRF5-TNPO3 (P meta = 2.73 × 10 -19), STAT4 (P meta = 6.80 × 10 -15), IL12A (P meta = 1.17 × 10 -10), FAM167A-BLK (P meta = 4.97 × 10 -10), DDX6-CXCR5 (P meta = 1.10 × 10 -8) and TNIP1 (P meta = 3.30 × 10 -8). We also observed suggestive associations (P meta less than 5 × 10 -5) with variants in 29 other regions, including TNFAIP3, PTTG1, PRDM1, DGKQ, FCGR2A, IRAK1BP1, ITSN2 and PHIP, among others. These results highlight the importance of genes that are involved in both innate and adaptive immunity in Sjögren's syndrome. © 2013 Nature America, Inc. All rights reserved.

Published

2013

149. Trans-ancestral studies fine map the SLE-susceptibility locus TNFSF4

Author

Anne M. Stevens, Timothy B. Niewold, Juan-Manuel Anaya, Chaim O. Jacob, Diane L. Kamen, Patrick M. Gaffney, Barry I. Freedman, Susan A. Boackle, Sandra G. Guerra, John B. Harley, Robert P. Kimberly, Bernardo A. Pons-Estel, Joan T. Merrill, R. Hal Scofield, Marta E. Alarcón-Riquelme, Elizabeth E. Brown, Kenneth M. Kaufman, Joel M. Guthridge, Carl D. Langefeld, Timothy J. Vyse, Javier Martin, Soyeon Park, Sang Hoon Han, Betty P. Tsao, Talat H. Malik, Jennifer A. Kelly, Harinder Manku, Judith A. James, Kathy L. Moser, Nan Shen, Celi Sun, Gary S. Gilkeson, Lindsey A. Criswell, Amr H. Sawalha, Sang Cheol Bae, Swapan K. Nath, Jeffrey C. Edberg, and Peter A. Gregersen

Subjects

Male, Cancer Research, Linkage disequilibrium, Genome-wide association study, Antibody production, OX40 ligand, Linkage Disequilibrium, Evolución & genética, 0302 clinical medicine, Autoantibody, Genetics of the Immune System, Lupus Erythematosus, Systemic, Lymphocytes, African American, Genetics (clinical), Genetics, Allele, 0303 health sciences, education.field_of_study, NF-kappa B, Chromosome Mapping, Hispanic or Latino, American Indian, Female, Alelos, Research Article, Anticuerpos, Genotype, lcsh:QH426-470, Population, Immunology, Inmunología, Locus (genetics), OX40 Ligand, Biology, Polymorphism, Single Nucleotide, White People, Molecular Genetics, 03 medical and health sciences, Asian People, Humans, Genetic Predisposition to Disease, 1000 Genomes Project, education, Molecular Biology, Ecology, Evolution, Behavior and Systematics, Transcription factor RelA, Alleles, 030304 developmental biology, 030203 arthritis & rheumatology, Haplotype, Human Genetics, Genética, Black or African American, lcsh:Genetics, Haplotypes, Cell isolation, Genetics of Disease, Imputation (genetics), Population Genetics, Genome-Wide Association Study

Abstract

We previously established an 80 kb haplotype upstream of TNFSF4 as a susceptibility locus in the autoimmune disease SLE. SLE-associated alleles at this locus are associated with inflammatory disorders, including atherosclerosis and ischaemic stroke. In Europeans, the TNFSF4 causal variants have remained elusive due to strong linkage disequilibrium exhibited by alleles spanning the region. Using a trans-ancestral approach to fine-map the locus, utilising 17,900 SLE and control subjects including Amerindian/Hispanics (1348 cases, 717 controls), African-Americans (AA) (1529, 2048) and better powered cohorts of Europeans and East Asians, we find strong association of risk alleles in all ethnicities; the AA association replicates in African-American Gullah (152,122). The best evidence of association comes from two adjacent markers: rs2205960-T (P = 1.71×10-34, OR = 1.43[1.26-1.60]) and rs1234317-T (P = 1.16×10-28, OR = 1.38[1.24-1.54]). Inference of fine-scale recombination rates for all populations tested finds the 80 kb risk and non-risk haplotypes in all except African-Americans. In this population the decay of recombination equates to an 11 kb risk haplotype, anchored in the 5′ region proximal to TNFSF4 and tagged by rs2205960-T after 1000 Genomes phase 1 (v3) imputation. Conditional regression analyses delineate the 5′ risk signal to rs2205960-T and the independent non-risk signal to rs1234314-C. Our case-only and SLE-control cohorts demonstrate robust association of rs2205960-T with autoantibody production. The rs2205960-T is predicted to form part of a decameric motif which binds NF-κBp65 with increased affinity compared to rs2205960-G. ChIP-seq data also indicate NF-κB interaction with the DNA sequence at this position in LCL cells. Our research suggests association of rs2205960-T with SLE across multiple groups and an independent non-risk signal at rs1234314-C. rs2205960-T is associated with autoantibody production and lymphopenia. Our data confirm a global signal at TNFSF4 and a role for the expressed product at multiple stages of lymphocyte dysregulation during SLE pathogenesis. We confirm the validity of trans-ancestral mapping in a complex trait. © 2013 Manku et al.

Published

2013

150. Effect of genetic background on the contribution of New Zealand Black loci to autoimmune lupus nephritis

Author

Brian L. Kotzin, Charles G. Drake, Timothy J. Vyse, and Stephen J. Rozzo

Subjects

Genetic Markers, Male, Aging, Genetic Linkage, Lupus nephritis, Congenic, Mice, Inbred Strains, Locus (genetics), Major histocompatibility complex, Major Histocompatibility Complex, Mice, Species Specificity, Genetic linkage, medicine, Animals, Humans, Crosses, Genetic, Recombination, Genetic, Genetics, Mice, Inbred BALB C, Multidisciplinary, Systemic lupus erythematosus, biology, Genetic heterogeneity, Chromosome Mapping, Biological Sciences, medicine.disease, Lupus Nephritis, Mice, Inbred C57BL, Genetic marker, biology.protein, Female

Abstract

Autoimmune diseases such as systemic lupus erythematosus are complex genetic traits with contributions from major histocompatibility complex (MHC) genes and multiple unknown non-MHC genes. Studies of animal models of lupus have provided important insight into the immunopathogenesis of disease, and genetic analyses of these models overcome certain obstacles encountered when studying human patients. Genome-wide scans of different genetic crosses have been used to map several disease-linked loci in New Zealand hybrid mice. Although some consensus exists among studies mapping the New Zealand Black (NZB) and New Zealand White (NZW) loci that contribute to lupus-like disease, considerable variability is also apparent. A variable in these studies is the genetic background of the non-autoimmune strain, which could influence genetic contributions from the affected strain. A direct examination of this question was undertaken in the present study by mapping NZB nephritis-linked loci in backcrosses involving different non-autoimmune backgrounds. In a backcross with MHC-congenic C57BL/6J mice,H2zappeared to be the strongest genetic determinant of severe lupus nephritis, whereas in a backcross with congenic BALB/cJ mice,H2zshowed no influence on disease expression. NZB loci on chromosomes 1, 4, 11, and 14 appeared to segregate with disease in the BALB/cJ cross, but only the influence of the chromosome 1 locus spanned both crosses and showed linkage with disease when all mice were considered. Thus, the results indicate that contributions from disease-susceptibility loci, including MHC, may vary markedly depending on the non-autoimmune strain used in a backcross analysis. These studies provide insight into variables that affect genetic heterogeneity and add an important dimension of complexity for linkage analyses of human autoimmune disease.

Published

1996