Your search keyword '"Kimberly, Robert P"' showing total 14 results

1. A comprehensive analysis of shared loci between systemic lupus erythematosus (SLE) and sixteen autoimmune diseases reveals limited genetic overlap.

Author

Ramos, Paula S, Criswell, Lindsey A, Moser, Kathy L, Comeau, Mary E, Williams, Adrienne H, Pajewski, Nicholas M, Chung, Sharon A, Graham, Robert R, Zidovetzki, Raphael, Kelly, Jennifer A, Kaufman, Kenneth M, Jacob, Chaim O, Vyse, Timothy J, Tsao, Betty P, Kimberly, Robert P, Gaffney, Patrick M, Alarcón-Riquelme, Marta E, Harley, John B, Langefeld, Carl D, and International Consortium on the Genetics of Systemic Erythematosus

Subjects

International Consortium on the Genetics of Systemic Erythematosus, Humans, Arthritis, Rheumatoid, Colitis, Ulcerative, Crohn Disease, Lupus Erythematosus, Systemic, Diabetes Mellitus, Type 1, Autoimmune Diseases, Genetic Predisposition to Disease, Receptors, Interleukin, Case-Control Studies, Cohort Studies, Polymorphism, Single Nucleotide, European Continental Ancestry Group, OX40 Ligand, Interleukin-2 Receptor alpha Subunit, Genome-Wide Association Study, Genetic Pleiotropy, V-Set Domain-Containing T-Cell Activation Inhibitor 1, Arthritis, Rheumatoid, Colitis, Ulcerative, Lupus Erythematosus, Systemic, Diabetes Mellitus, Type 1, Receptors, Interleukin, Polymorphism, Single Nucleotide, Genetics, Developmental Biology

Abstract

In spite of the well-known clustering of multiple autoimmune disorders in families, analyses of specific shared genes and polymorphisms between systemic lupus erythematosus (SLE) and other autoimmune diseases (ADs) have been limited. Therefore, we comprehensively tested autoimmune variants for association with SLE, aiming to identify pleiotropic genetic associations between these diseases. We compiled a list of 446 non-Major Histocompatibility Complex (MHC) variants identified in genome-wide association studies (GWAS) of populations of European ancestry across 17 ADs. We then tested these variants in our combined Caucasian SLE cohorts of 1,500 cases and 5,706 controls. We tested a subset of these polymorphisms in an independent Caucasian replication cohort of 2,085 SLE cases and 2,854 controls, allowing the computation of a meta-analysis between all cohorts. We have uncovered novel shared SLE loci that passed multiple comparisons adjustment, including the VTCN1 (rs12046117, P = 2.02×10(-06)) region. We observed that the loci shared among the most ADs include IL23R, OLIG3/TNFAIP3, and IL2RA. Given the lack of a universal autoimmune risk locus outside of the MHC and variable specificities for different diseases, our data suggests partial pleiotropy among ADs. Hierarchical clustering of ADs suggested that the most genetically related ADs appear to be type 1 diabetes with rheumatoid arthritis and Crohn's disease with ulcerative colitis. These findings support a relatively distinct genetic susceptibility for SLE. For many of the shared GWAS autoimmune loci, we found no evidence for association with SLE, including IL23R. Also, several established SLE loci are apparently not associated with other ADs, including the ITGAM-ITGAX and TNFSF4 regions. This study represents the most comprehensive evaluation of shared autoimmune loci to date, supports a relatively distinct non-MHC genetic susceptibility for SLE, provides further evidence for previously and newly identified shared genes in SLE, and highlights the value of studies of potentially pleiotropic genes in autoimmune diseases.

Published

2011

2. Genome-Wide DNA Methylation Analysis of Systemic Lupus Erythematosus Reveals Persistent Hypomethylation of Interferon Genes and Compositional Changes to CD4+ T-cell Populations

Author

Absher, Devin M., primary, Li, Xinrui, additional, Waite, Lindsay L., additional, Gibson, Andrew, additional, Roberts, Kevin, additional, Edberg, Jeffrey, additional, Chatham, W. Winn, additional, and Kimberly, Robert P., additional

Published

2013

3. Trans-Ancestral Studies Fine Map the SLE-Susceptibility Locus TNFSF4

Author

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

Published

2013

4. Genome-Wide Association Study and Gene Expression Analysis Identifies CD84 as a Predictor of Response to Etanercept Therapy in Rheumatoid Arthritis

Author

Cui, Jing, primary, Stahl, Eli A., additional, Saevarsdottir, Saedis, additional, Miceli, Corinne, additional, Diogo, Dorothee, additional, Trynka, Gosia, additional, Raj, Towfique, additional, Mirkov, Maša Umiċeviċ, additional, Canhao, Helena, additional, Ikari, Katsunori, additional, Terao, Chikashi, additional, Okada, Yukinori, additional, Wedrén, Sara, additional, Askling, Johan, additional, Yamanaka, Hisashi, additional, Momohara, Shigeki, additional, Taniguchi, Atsuo, additional, Ohmura, Koichiro, additional, Matsuda, Fumihiko, additional, Mimori, Tsuneyo, additional, Gupta, Namrata, additional, Kuchroo, Manik, additional, Morgan, Ann W., additional, Isaacs, John D., additional, Wilson, Anthony G., additional, Hyrich, Kimme L., additional, Herenius, Marieke, additional, Doorenspleet, Marieke E., additional, Tak, Paul-Peter, additional, Crusius, J. Bart A., additional, van der Horst-Bruinsma, Irene E., additional, Wolbink, Gert Jan, additional, van Riel, Piet L. C. M., additional, van de Laar, Mart, additional, Guchelaar, Henk-Jan, additional, Shadick, Nancy A., additional, Allaart, Cornelia F., additional, Huizinga, Tom W. J., additional, Toes, Rene E. M., additional, Kimberly, Robert P., additional, Bridges, S. Louis, additional, Criswell, Lindsey A., additional, Moreland, Larry W., additional, Fonseca, João Eurico, additional, de Vries, Niek, additional, Stranger, Barbara E., additional, De Jager, Philip L., additional, Raychaudhuri, Soumya, additional, Weinblatt, Michael E., additional, Gregersen, Peter K., additional, Mariette, Xavier, additional, Barton, Anne, additional, Padyukov, Leonid, additional, Coenen, Marieke J. H., additional, Karlson, Elizabeth W., additional, and Plenge, Robert M., additional

Published

2013

5. Retraction: An African Ancestry-Specific Allele of CTLA4 Confers Protection against Rheumatoid Arthritis in African Americans

Author

Kelley, James M., primary, Hughes, Laura B., additional, Faggard, Jeffrey D., additional, Danila, Maria I., additional, Crawford, Monica H., additional, Edberg, Yuanqing, additional, Padilla, Miguel A., additional, Tiwari, Hemant K., additional, Westfall, Andrew O., additional, Alarcón, Graciela S., additional, Conn, Doyt L., additional, Jonas, Beth L., additional, Callahan, Leigh F., additional, Smith, Edwin A., additional, Brasington, Richard D., additional, Allison, David B., additional, Kimberly, Robert P., additional, Moreland, Larry W., additional, Edberg, Jeffrey C., additional, and Bridges, S. Louis, additional

Published

2009

6. An African Ancestry-Specific Allele of CTLA4 Confers Protection against Rheumatoid Arthritis in African Americans

Author

Kelley, James M., primary, Hughes, Laura B., additional, Faggard, Jeffrey D., additional, Danila, Maria I., additional, Crawford, Monica H., additional, Edberg, Yuanqing, additional, Padilla, Miguel A., additional, Tiwari, Hemant K., additional, Westfall, Andrew O., additional, Alarcón, Graciela S., additional, Conn, Doyt L., additional, Jonas, Beth L., additional, Callahan, Leigh F., additional, Smith, Edwin A., additional, Brasington, Richard D., additional, Allison, David B., additional, Kimberly, Robert P., additional, Moreland, Larry W., additional, Edberg, Jeffrey C., additional, and Bridges, S. Louis, additional

Published

2009

7. Regional Admixture Mapping and Structured Association Testing: Conceptual Unification and an Extensible General Linear Model

Author

Redden, David T, primary, Divers, Jasmin, additional, Vaughan, Laura Kelly, additional, Tiwari, Hemant K, additional, Beasley, T. Mark, additional, Fernández, José R, additional, Kimberly, Robert P, additional, Feng, Rui, additional, Padilla, Miguel A, additional, Liu, Nianjun, additional, Miller, Michael B, additional, and Allison, David B, additional

Published

2006

8. Regional Admixture Mapping and Structured Association Testing: Conceptual Unification and an Extensible General Linear Model

Author

Redden, David T., primary, Divers, Jasmin, additional, Vaughan, Laura, additional, Tiwari, Hemant K, additional, Beasley, Mark Mark, additional, Fernandez, Jose R., additional, Kimberly, Robert P, additional, Feng, Rui, additional, Padilla, Miguel, additional, Lui, Nianjun, additional, Miller, Michael B., additional, and Allison, David B., additional

Published

2005

9. Preferential Binding to Elk-1 by SLE-Associated IL10 Risk Allele Upregulates IL10 Expression.

Author

Sakurai, Daisuke, Zhao, Jian, Deng, Yun, Kelly, Jennifer A., Brown, Elizabeth E., Harley, John B., Bae, Sang-Cheol, Alarcόn-Riquelme, Marta E., Edberg, Jeffrey C., Kimberly, Robert P., Ramsey-Goldman, Rosalind, Petri, Michelle A., Reveille, John D., Vilá, Luis M., Alarcón, Graciela S., Kaufman, Kenneth M., Vyse, Timothy J., Jacob, Chaim O., Gaffney, Patrick M., and Sivils, Kathy Moser

Subjects

CYTOKINES, INTERLEUKINS, SYSTEMIC lupus erythematosus, AUTOIMMUNE diseases, SINGLE nucleotide polymorphisms

Abstract

Immunoregulatory cytokine interleukin-10 (IL-10) is elevated in sera from patients with systemic lupus erythematosus (SLE) correlating with disease activity. The established association of IL10 with SLE and other autoimmune diseases led us to fine map causal variant(s) and to explore underlying mechanisms. We assessed 19 tag SNPs, covering the IL10 gene cluster including IL19, IL20 and IL24, for association with SLE in 15,533 case and control subjects from four ancestries. The previously reported IL10 variant, rs3024505 located at 1 kb downstream of IL10, exhibited the strongest association signal and was confirmed for association with SLE in European American (EA) (P = 2.7×10−8, OR = 1.30), but not in non-EA ancestries. SNP imputation conducted in EA dataset identified three additional SLE-associated SNPs tagged by rs3024505 (rs3122605, rs3024493 and rs3024495 located at 9.2 kb upstream, intron 3 and 4 of IL10, respectively), and SLE-risk alleles of these SNPs were dose-dependently associated with elevated levels of IL10 mRNA in PBMCs and circulating IL-10 protein in SLE patients and controls. Using nuclear extracts of peripheral blood cells from SLE patients for electrophoretic mobility shift assays, we identified specific binding of transcription factor Elk-1 to oligodeoxynucleotides containing the risk (G) allele of rs3122605, suggesting rs3122605 as the most likely causal variant regulating IL10 expression. Elk-1 is known to be activated by phosphorylation and nuclear localization to induce transcription. Of interest, phosphorylated Elk-1 (p-Elk-1) detected only in nuclear extracts of SLE PBMCs appeared to increase with disease activity. Co-expression levels of p-Elk-1 and IL-10 were elevated in SLE T, B cells and monocytes, associated with increased disease activity in SLE B cells, and were best downregulated by ERK inhibitor. Taken together, our data suggest that preferential binding of activated Elk-1 to the IL10 rs3122605-G allele upregulates IL10 expression and confers increased risk for SLE in European Americans. [ABSTRACT FROM AUTHOR]

Published

2013

10. MicroRNA-3148 Modulates Allelic Expression of Toll-Like Receptor 7 Variant Associated with Systemic Lupus Erythematosus.

Author

Yun Deng, Jian Zhao, Sakurai, Daisuke, Kaufman, Kenneth M., Edberg, Jeffrey C., Kimberly, Robert P., Kamen, Diane L., Gilkeson, Gary S., Jacob, Chaim O., Scofield, R. Hal, Langefeld, Carl D., Kelly, Jennifer A., Ramsey-Goldman, Rosalind, Petri, Michelle A., Reveille, John D., Vilá, Luis M., Alarcón, Graciela S., Vyse, Timothy J., Pons-Estel, Bernardo A., and Freedman, Barry I.

Subjects

MICRORNA, COMPLEMENTATION (Genetics), GENE expression, SYSTEMIC lupus erythematosus, GENETICS of autoimmune diseases, GENETICS

Abstract

We previously reported that the G allele of rs3853839 at 3' untranslated region (UTR) of Toll-like receptor 7 (TLR7) was associated with elevated transcript expression and increased risk for systemic lupus erythematosus (SLE) in 9,274 Eastern Asians [P = 6.5x10-10, odds ratio (OR) (95%CI) = 1.27 (1.17-1.36)]. Here, we conducted trans-ancestral fine-mapping in 13,339 subjects including European Americans, African Americans, and Amerindian/Hispanics and confirmed rs3853839 as the only variant within the TLR7-TLR8 region exhibiting consistent and independent association with SLE (Pmeta = 7.5x10-11, OR = 1.24 [1.18-1.34]). The risk G allele was associated with significantly increased levels of TLR7 mRNA and protein in peripheral blood mononuclear cells (PBMCs) and elevated luciferase activity of reporter gene in transfected cells. TLR7 39UTR sequence bearing the non-risk C allele of rs3853839 matches a predicted binding site of microRNA-3148 (miR-3148), suggesting that this microRNA may regulate TLR7 expression. Indeed, miR-3148 levels were inversely correlated with TLR7 transcript levels in PBMCs from SLE patients and controls (R² = 0.255, P = 0.001). Overexpression of miR-3148 in HEK-293 cells led to significant dose-dependent decrease in luciferase activity for construct driven by TLR7 39UTR segment bearing the C allele (P = 0.0003). Compared with the G-allele construct, the C-allele construct showed greater than two-fold reduction of luciferase activity in the presence of miR-3148. Reduced modulation by miR-3148 conferred slower degradation of the risk G-allele containing TLR7 transcripts, resulting in elevated levels of gene products. These data establish rs3853839 of TLR7 as a shared risk variant of SLE in 22,613 subjects of Asian, EA, AA, and Amerindian/Hispanic ancestries (Pmeta = 2.0x10-19, OR = 1.25 [1.20-1.32]), which confers allelic effect on transcript turnover via differential binding to the epigenetic factor miR-3148. [ABSTRACT FROM AUTHOR]

Published

2013

11. Admixture mapping in lupus identifies multiple functional variants within IFIH1 associated with apoptosis, inflammation, and autoantibody production.

Author

Molineros JE, Maiti AK, Sun C, Looger LL, Han S, Kim-Howard X, Glenn S, Adler A, Kelly JA, Niewold TB, Gilkeson GS, Brown EE, Alarcón GS, Edberg JC, Petri M, Ramsey-Goldman R, Reveille JD, Vilá LM, Freedman BI, Tsao BP, Criswell LA, Jacob CO, Moore JH, Vyse TJ, Langefeld CL, Guthridge JM, Gaffney PM, Moser KL, Scofield RH, Alarcón-Riquelme ME, Williams SM, Merrill JT, James JA, Kaufman KM, Kimberly RP, Harley JB, and Nath SK

Subjects

Alleles, Antigens, Nuclear genetics, Antigens, Nuclear immunology, Apoptosis genetics, Autoantibodies genetics, Autoantibodies immunology, Chromosome Mapping, DNA-Binding Proteins genetics, DNA-Binding Proteins immunology, Genetic Predisposition to Disease, Genome, Human, Haplotypes, Humans, Inflammation genetics, Interferon-Induced Helicase, IFIH1, Ku Autoantigen, Lupus Erythematosus, Systemic immunology, Polymorphism, Single Nucleotide, Protein Binding, White People genetics, Black or African American genetics, DEAD-box RNA Helicases genetics, Lupus Erythematosus, Systemic 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 [P(meta) = 5.20×10(-14); odds ratio, 95% confidence interval = 0.82 (0.78-0.87)], and two missense variants, rs1990760 (Ala946Thr) [P(meta) = 3.08×10(-7); 0.88 (0.84-0.93)] and rs10930046 (Arg460His) [P(dom) = 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., Competing Interests: The authors have declared that no competing interests exist.

Published

2013

12. MicroRNA-3148 modulates allelic expression of toll-like receptor 7 variant associated with systemic lupus erythematosus.

Author

Deng Y, Zhao J, Sakurai D, Kaufman KM, Edberg JC, Kimberly RP, Kamen DL, Gilkeson GS, Jacob CO, Scofield RH, Langefeld CD, Kelly JA, Ramsey-Goldman R, Petri MA, Reveille JD, Vilá LM, Alarcón GS, Vyse TJ, Pons-Estel BA, Freedman BI, Gaffney PM, Sivils KM, James JA, Gregersen PK, Anaya JM, Niewold TB, Merrill JT, Criswell LA, Stevens AM, Boackle SA, Cantor RM, Chen W, Grossman JM, Hahn BH, Harley JB, Alarcόn-Riquelme ME, Brown EE, and Tsao BP

Subjects

3' Untranslated Regions, Black or African American genetics, Alleles, Asian People genetics, Gene Expression Regulation genetics, HEK293 Cells, Hispanic or Latino genetics, Humans, Lupus Erythematosus, Systemic metabolism, Polymorphism, Single Nucleotide, White People, Genetic Predisposition to Disease, Lupus Erythematosus, Systemic genetics, MicroRNAs genetics, Toll-Like Receptor 7 genetics, Toll-Like Receptor 7 metabolism

Abstract

We previously reported that the G allele of rs3853839 at 3'untranslated region (UTR) of Toll-like receptor 7 (TLR7) was associated with elevated transcript expression and increased risk for systemic lupus erythematosus (SLE) in 9,274 Eastern Asians [P = 6.5×10(-10), odds ratio (OR) (95%CI) = 1.27 (1.17-1.36)]. Here, we conducted trans-ancestral fine-mapping in 13,339 subjects including European Americans, African Americans, and Amerindian/Hispanics and confirmed rs3853839 as the only variant within the TLR7-TLR8 region exhibiting consistent and independent association with SLE (Pmeta = 7.5×10(-11), OR = 1.24 [1.18-1.34]). The risk G allele was associated with significantly increased levels of TLR7 mRNA and protein in peripheral blood mononuclear cells (PBMCs) and elevated luciferase activity of reporter gene in transfected cells. TLR7 3'UTR sequence bearing the non-risk C allele of rs3853839 matches a predicted binding site of microRNA-3148 (miR-3148), suggesting that this microRNA may regulate TLR7 expression. Indeed, miR-3148 levels were inversely correlated with TLR7 transcript levels in PBMCs from SLE patients and controls (R(2) = 0.255, P = 0.001). Overexpression of miR-3148 in HEK-293 cells led to significant dose-dependent decrease in luciferase activity for construct driven by TLR7 3'UTR segment bearing the C allele (P = 0.0003). Compared with the G-allele construct, the C-allele construct showed greater than two-fold reduction of luciferase activity in the presence of miR-3148. Reduced modulation by miR-3148 conferred slower degradation of the risk G-allele containing TLR7 transcripts, resulting in elevated levels of gene products. These data establish rs3853839 of TLR7 as a shared risk variant of SLE in 22,613 subjects of Asian, EA, AA, and Amerindian/Hispanic ancestries (Pmeta  = 2.0×10(-19), OR = 1.25 [1.20-1.32]), which confers allelic effect on transcript turnover via differential binding to the epigenetic factor miR-3148., Competing Interests: The authors have declared that no competing interests exist.

Published

2013

13. Preferential binding to Elk-1 by SLE-associated IL10 risk allele upregulates IL10 expression.

Author

Sakurai D, Zhao J, Deng Y, Kelly JA, Brown EE, Harley JB, Bae SC, Alarcόn-Riquelme ME, Edberg JC, Kimberly RP, Ramsey-Goldman R, Petri MA, Reveille JD, Vilá LM, Alarcón GS, Kaufman KM, Vyse TJ, Jacob CO, Gaffney PM, Sivils KM, James JA, Kamen DL, Gilkeson GS, Niewold TB, Merrill JT, Scofield RH, Criswell LA, Stevens AM, Boackle SA, Kim JH, Choi J, Pons-Estel BA, Freedman BI, Anaya JM, Martin J, Yu CY, Chang DM, Song YW, Langefeld CD, Chen W, Grossman JM, Cantor RM, Hahn BH, and Tsao BP

Subjects

Alleles, Asian People, Gene Expression Regulation, Genome-Wide Association Study, Genotype, Haplotypes, Hispanic or Latino, Humans, Interleukin-10 biosynthesis, Introns, Lupus Erythematosus, Systemic pathology, Polymorphism, Single Nucleotide, Protein Binding, Up-Regulation, White People genetics, ets-Domain Protein Elk-1 biosynthesis, Genetic Predisposition to Disease, Interleukin-10 genetics, Lupus Erythematosus, Systemic genetics, ets-Domain Protein Elk-1 genetics

Abstract

Immunoregulatory cytokine interleukin-10 (IL-10) is elevated in sera from patients with systemic lupus erythematosus (SLE) correlating with disease activity. The established association of IL10 with SLE and other autoimmune diseases led us to fine map causal variant(s) and to explore underlying mechanisms. We assessed 19 tag SNPs, covering the IL10 gene cluster including IL19, IL20 and IL24, for association with SLE in 15,533 case and control subjects from four ancestries. The previously reported IL10 variant, rs3024505 located at 1 kb downstream of IL10, exhibited the strongest association signal and was confirmed for association with SLE in European American (EA) (P = 2.7×10⁻⁸, OR = 1.30), but not in non-EA ancestries. SNP imputation conducted in EA dataset identified three additional SLE-associated SNPs tagged by rs3024505 (rs3122605, rs3024493 and rs3024495 located at 9.2 kb upstream, intron 3 and 4 of IL10, respectively), and SLE-risk alleles of these SNPs were dose-dependently associated with elevated levels of IL10 mRNA in PBMCs and circulating IL-10 protein in SLE patients and controls. Using nuclear extracts of peripheral blood cells from SLE patients for electrophoretic mobility shift assays, we identified specific binding of transcription factor Elk-1 to oligodeoxynucleotides containing the risk (G) allele of rs3122605, suggesting rs3122605 as the most likely causal variant regulating IL10 expression. Elk-1 is known to be activated by phosphorylation and nuclear localization to induce transcription. Of interest, phosphorylated Elk-1 (p-Elk-1) detected only in nuclear extracts of SLE PBMCs appeared to increase with disease activity. Co-expression levels of p-Elk-1 and IL-10 were elevated in SLE T, B cells and monocytes, associated with increased disease activity in SLE B cells, and were best downregulated by ERK inhibitor. Taken together, our data suggest that preferential binding of activated Elk-1 to the IL10 rs3122605-G allele upregulates IL10 expression and confers increased risk for SLE in European Americans., Competing Interests: The authors have declared that no competing interests exist.

Published

2013

14. Association of genetic variants in complement factor H and factor H-related genes with systemic lupus erythematosus susceptibility.

Author

Zhao J, Wu H, Khosravi M, Cui H, Qian X, Kelly JA, Kaufman KM, Langefeld CD, Williams AH, Comeau ME, Ziegler JT, Marion MC, Adler A, Glenn SB, Alarcón-Riquelme ME, Pons-Estel BA, Harley JB, Bae SC, Bang SY, Cho SK, Jacob CO, Vyse TJ, Niewold TB, Gaffney PM, Moser KL, Kimberly RP, Edberg JC, Brown EE, Alarcon GS, Petri MA, Ramsey-Goldman R, Vilá LM, Reveille JD, James JA, Gilkeson GS, Kamen DL, Freedman BI, Anaya JM, Merrill JT, Criswell LA, Scofield RH, Stevens AM, Guthridge JM, Chang DM, Song YW, Park JA, Lee EY, Boackle SA, Grossman JM, Hahn BH, Goodship TH, Cantor RM, Yu CY, Shen N, and Tsao BP

Subjects

Black or African American genetics, Alleles, Asian People genetics, Case-Control Studies, Chromosomes, Human, Pair 1 genetics, Gene Deletion, Gene Frequency, Genotype, Hispanic or Latino genetics, Humans, Introns, Lupus Erythematosus, Systemic ethnology, White People genetics, Antigens, Neoplasm genetics, Biomarkers, Tumor genetics, Complement Factor H genetics, Genetic Predisposition to Disease, Lupus Erythematosus, Systemic genetics, Polymorphism, Single Nucleotide

Abstract

Systemic lupus erythematosus (SLE), a complex polygenic autoimmune disease, is associated with increased complement activation. Variants of genes encoding complement regulator factor H (CFH) and five CFH-related proteins (CFHR1-CFHR5) within the chromosome 1q32 locus linked to SLE, have been associated with multiple human diseases and may contribute to dysregulated complement activation predisposing to SLE. We assessed 60 SNPs covering the CFH-CFHRs region for association with SLE in 15,864 case-control subjects derived from four ethnic groups. Significant allelic associations with SLE were detected in European Americans (EA) and African Americans (AA), which could be attributed to an intronic CFH SNP (rs6677604, in intron 11, P(meta) = 6.6×10(-8), OR = 1.18) and an intergenic SNP between CFHR1 and CFHR4 (rs16840639, P(meta) = 2.9×10(-7), OR = 1.17) rather than to previously identified disease-associated CFH exonic SNPs, including I62V, Y402H, A474A, and D936E. In addition, allelic association of rs6677604 with SLE was subsequently confirmed in Asians (AS). Haplotype analysis revealed that the underlying causal variant, tagged by rs6677604 and rs16840639, was localized to a ~146 kb block extending from intron 9 of CFH to downstream of CFHR1. Within this block, the deletion of CFHR3 and CFHR1 (CFHR3-1Δ), a likely causal variant measured using multiplex ligation-dependent probe amplification, was tagged by rs6677604 in EA and AS and rs16840639 in AA, respectively. Deduced from genotypic associations of tag SNPs in EA, AA, and AS, homozygous deletion of CFHR3-1Δ (P(meta) = 3.2×10(-7), OR = 1.47) conferred a higher risk of SLE than heterozygous deletion (P(meta) = 3.5×10(-4), OR = 1.14). These results suggested that the CFHR3-1Δ deletion within the SLE-associated block, but not the previously described exonic SNPs of CFH, might contribute to the development of SLE in EA, AA, and AS, providing new insights into the role of complement regulators in the pathogenesis of SLE., Competing Interests: The authors have declared that no competing interests exist.

Published

2011