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107. Regulation of phagocytosis and (Ca2+)i flux by distinct regions of an Fc receptor

Author

Odin, Joseph A., Edberg, Jeffrey C., Painter, Catherine J., Kimberly, Robert P., and Unkeless, Jay C.

Subjects
Calcium, Dietary -- Research, Immunoglobulin G -- Research, Phagocytosis -- Research, Science and technology, Research
Abstract

The binding of multivalent immunoglobulin G complexes to Fc receptors ([Fc.sub.γ.Rs]) on macrophages activates multiple immune functions. A murine macrophage cell line, but not a fibroblast cell line, that was transfected with human [Fc.sub.γ.RIIA] mediated phagocytosis and an intracellular [Ca.sup.2+] concentration ([[[Ca.sup.2+]].sub.i]) flux upon cross-linking of human [Fc.sub.γ.RIIA]. Transfected macrophages that expressed a truncated receptor lacking 17 carboxy-terminal amino acids phagocytosed small antibody complexes. However, only wild-type transfectants phagocytosed labeled erythrocytes and fluxed [[Ca.sup.2+]].sub.i]. Thus, the cytoplasmic domain of human [Fc.sub.γ.RIIA] conatins distinct functional regions., FC RECEPTORS ([Fc.sub.γ.Rs]) FOR IMMUNO-globulin G (IgG) link humoral and cell-mediated immune responses. Activation of [Fc.sub.γ.Rs] requires cross-linking of multiple receptors by immune complexes. In neutrophils and macrophages, the binding [...]

Published
1991

109. IFNγ induces epigenetic programming of human T-bethi B cells and promotes TLR7/8 and IL-21 induced differentiation

Author

Zumaquero, Esther, primary, Stone, Sara L, additional, Scharer, Christopher D, additional, Jenks, Scott A, additional, Nellore, Anoma, additional, Mousseau, Betty, additional, Rosal-Vela, Antonio, additional, Botta, Davide, additional, Bradley, John E, additional, Wojciechowski, Wojciech, additional, Ptacek, Travis, additional, Danila, Maria I, additional, Edberg, Jeffrey C, additional, Bridges, S Louis, additional, Kimberly, Robert P, additional, Chatham, W Winn, additional, Schoeb, Trenton R, additional, Rosenberg, Alexander F, additional, Boss, Jeremy M, additional, Sanz, Ignacio, additional, and Lund, Frances E, additional

Published
2019
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110. Association of response to TNF inhibitors in rheumatoid arthritis with quantitative trait loci for CD40 and CD39

Author

Spiliopoulou, Athina, primary, Colombo, Marco, additional, Plant, Darren, additional, Nair, Nisha, additional, Cui, Jing, additional, Coenen, Marieke JH, additional, Ikari, Katsunori, additional, Yamanaka, Hisashi, additional, Saevarsdottir, Saedis, additional, Padyukov, Leonid, additional, Bridges Jr., S Louis, additional, Kimberly, Robert P, additional, Okada, Yukinori, additional, van Riel, Piet L CM, additional, Wolbink, Gertjan, additional, van der Horst-Bruinsma, Irene E, additional, de Vries, Niek, additional, Tak, Paul P, additional, Ohmura, Koichiro, additional, Canhão, Helena, additional, Guchelaar, Henk-Jan, additional, Huizinga, Tom WJ, additional, Criswell, Lindsey A, additional, Raychaudhuri, Soumya, additional, Weinblatt, Michael E, additional, Wilson, Anthony G, additional, Mariette, Xavier, additional, Isaacs, John D, additional, Morgan, Ann W, additional, Pitzalis, Costantino, additional, Barton, Anne, additional, and McKeigue, Paul, additional

Published
2019
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111. Author response: IFNγ induces epigenetic programming of human T-bethi B cells and promotes TLR7/8 and IL-21 induced differentiation

Author

Zumaquero, Esther, primary, Stone, Sara L, additional, Scharer, Christopher D, additional, Jenks, Scott A, additional, Nellore, Anoma, additional, Mousseau, Betty, additional, Rosal-Vela, Antonio, additional, Botta, Davide, additional, Bradley, John E, additional, Wojciechowski, Wojciech, additional, Ptacek, Travis, additional, Danila, Maria I, additional, Edberg, Jeffrey C, additional, Bridges, S Louis, additional, Kimberly, Robert P, additional, Chatham, W Winn, additional, Schoeb, Trenton R, additional, Rosenberg, Alexander F, additional, Boss, Jeremy M, additional, Sanz, Ignacio, additional, and Lund, Frances E, additional

Published
2019
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112. Exploring COVID-19 Vaccine Hesitancy Among Stakeholders in African American and Latinx Communities in the Deep South Through the Lens of the Health Belief Model

Author

Bateman, Lori B., Hall, Allyson G., Anderson, William A., Cherrington, Andrea L., Helova, Anna, Judd, Suzanne, Kimberly, Robert, Oates, Gabriela R., Osborne, Tiffany, Ott, Corilyn, Ryan, Melissa, Strong, Christian, and Fouad, Mona N.

Abstract

Purpose The purpose of this study was to qualitatively explore perceptions related to COVID-19 vaccination intention among African American and Latinx participants and suggest intervention strategies.Approach Ninety minute virtual focus groups (N = 8), segmented by county, race and ethnicity were conducted with stakeholders from 3 vulnerable Alabama counties.Participants Participants (N = 67) were primarily African American and Latinx, at least 19 years, and residents or stakeholders in Jefferson, Mobile, and Dallas counties.Setting Focus groups took place virtually over Zoom.Methods The semi-structured guide explored perceptions of COVID-19, with an emphasis on barriers and facilitators to vaccine uptake. Focus groups lasted approximately 90 minutes and were audio recorded, transcribed, and analyzed by a team of 3 investigators, according to the guidelines of Thematic Analysis using NVivo 12. To provide guidance in the development of interventions to decrease vaccine hesitancy, we examined how themes fit with the constructs of the Health Belief Model.Results We found that primary themes driving COVID-19 vaccine hesitancy, ordered from most to least discussed, are mistrust, fear, and lack of information. Additionally, interventions to decrease vaccine hesitancy should be multi-modal, community engaged, and provide consistent, comprehensive messages delivered by trusted sources.

Published
2022
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118. Transancestral mapping and genetic load in systemic lupus erythematosus

Author

Langefeld, C. D., Ainsworth, H. C., Kelly, J. A., Comeau, M. E., Marion, M. C., Howard, T. D., Ramos, P. S., Croker, J. A., Morris, D. L., Sandling, J. K., Almlöf, J. C., Pons-Estel, Bernardo A., Pope, Janet, Raj, Prithvi, Ramsey-Goldman, Rosalind, Reveille, John D., Russell, Laurie P., Sabio, José Mario, Aguilar-Salinas, Carlos A., Scherbarth, Hugo R., Scorza, Raffaella, Seldin, Michael F., Sjowall, Christopher, Svenungsson, Elisabet, Thompson, Susan D., Toloza, Sergio M. A., Truedsson, Lennart, Tusie-Luna, Teresa, Vasconcelos, C., Vilá, Luis M., Wallace, Daniel J., Weisman, Michael H., Wither, Joan E., Bhangale, Tushar, Oksenberg, Jorge R., Rioux, John D., Gregersen, Peter K., Syvanen, Ann-Christine, Ronnblom, Lars, Criswell, Lindsey A., Jacob, Chaim O., Sivils, Kathy L., Tsao, Betty P., Schanberg, Laura E., Behrens, Timothy W., Silverman, Earl D., Alarcón-Riquelme, M. E., Kimberly, Robert P., Harley, John B., Wakeland, Edward K., Graham, Robert R., Gaffney, P. M., Vyse, Timothy J., Acevedo-Vásquez, E. M., Alarcón, G. S., Babini, A. M., Baca, V., Bengtsson, A. A., Berbotto, G. A., Bij, l. M., Brown, E. E., Brunner, H.I., Cardiel, Mario H., Catoggio, Luis, Cervera, Ricard, Cucho-Venegas, Jorge M., Dahlqvist, Solbritt Rantapaa, D'Alfonso, Sandra, Da Silva, Berta Martins, de la Rua Figueroa, Inigo, Doria, Andrea, Edberg, Jeffrey C., Endreffy, Emoke, Esquivel-Valerio, Jorge A., Fortin, Paul R., Freedman, Barry I., Frostegård, Johan, García, Mercedes A., García de la Torre, Ignacio, Gilkeson, G. S., Gladman, Dafna D., Gunnarsson, Iva, Guthridge, Joel M., Huggins, Jennifer L., James, Judith A., Kallenberg, Cees G. M., Kamen, D. L., Karp, David R., Kaufman, Kenneth M, Kottyan, Leah C., Kovacs, Laszlo, Laustrup, Helle, Lauwerys, Bernard R., Li, Quan-Zhen, Maradiaga-Cecena, Marco A., Martín, J., McCune, Joseph M., McWilliams, David R, Merrill, Joan T, Miranda, Pedro, Moctezuma, Jose F., Nath, Swapan K., Niewold, Timothy B., Orozco, Lorena, Ortego-Centeno, N., Petri, Michelle, Pineau, Christian A., National Institute for Health Research (UK), Arthritis Research UK, Alliance for Lupus Research, Junta de Andalucía, National Institute of Arthritis and Musculoskeletal and Skin Diseases (US), National Institutes of Health (US), RILITE Foundation, and Genentech Foundation

Subjects
skin and connective tissue diseases
Abstract

Systemic lupus erythematosus (SLE) is an autoimmune disease with marked gender and ethnic disparities. We report a large transancestral association study of SLE using Immunochip genotype data from 27,574 individuals of European (EA), African (AA) and Hispanic Amerindian (HA) ancestry. We identify 58 distinct non-HLA regions in EA, 9 in AA and 16 in HA (similar to 50% of these regions have multiple independent associations); these include 24 novel SLE regions (P < 5 x 10(-8)), refined association signals in established regions, extended associations to additional ancestries, and a disentangled complex HLA multigenic effect. The risk allele count (genetic load) exhibits an accelerating pattern of SLE risk, leading us to posit a cumulative hit hypothesis for autoimmune disease. Comparing results across the three ancestries identifies both ancestry-dependent and ancestry-independent contributions to SLE risk. Our results are consistent with the unique and complex histories of the populations sampled, and collectively help clarify the genetic architecture and ethnic disparities in SLE., We gratefully acknowledge the Alliance for Lupus Research for funding and support. The research was supported in part by awards from the Arthritis Research UK Special Strategic Award (ref. 19289) and from George Koukis (T.J.V.). In addition, the research was funded/supported by the National Institute for Health Research (NIHR) Biomedical Research Centre based at Guy's and St Thomas' NHS Foundation Trust and King's College London (T.J.V.). The work would not be possible without funding from the NIH grants AR049084 (RPK, EEB); the International Consortium on the Genetics of Systemic Lupus Erythematosus (SLEGEN) AI083194 (J.B.H.); CA141700, AR058621 Proyecto de Excelencia, Consejeria de Andalucia (M.E.A.R.); AR043814 and AR-065626 (B.P.T.); AR060366, MD007909, AI107176 (S.K.N.); AR-057172 (C.O.J.); RC2 AR058959, U19 A1082714, R01 AR063124, P30 GM110766, R01 AR056360 (P.M.G.); P60 AR053308 (L.A.C.), MUSC part is from UL1RR029882 (G.S.G., D.L.K.) and 5P60AR062755 (G.S.G., D.L.K., P.R.R.). Oklahoma Samples U19AI082714, U01AI101934, P30GM103510, U54GM104938 and P30AR053483 (J.A.J., J.M.G.); Northwestern P60 AR066464 and 1U54TR001018 (R.R.G.); This study was supported by the US National Institute of Arthritis and Musculoskeletal and Skin Diseases of the National Institutes of Health (NIH) under Award Numbers K01 AR067280 and P60 AR062755 (PSR); N01AR22265 (funded collection of APPLE samples) (LES) and the APPLE Investigators; R01AR43727, NIH AR 043727 and 069572 (M.P.); NIAMS/NIH P50-AR055503 (D.R.K.). We would like to also thank the RILITE foundation for financial support (C.D.L.). Additional funding for Immunochip genotyping was provided by Genentech.

Published
2017

119. Population‐Specific Patterns of Epigenetic Defects in the B Cell Lineage in Patients With Systemic Lupus Erythematosus.

Author

Breitbach, Megan E., Ramaker, Ryne C., Roberts, Kevin, Kimberly, Robert P., and Absher, Devin

Subjects
ALGORITHMS, B cells, BLACK people, CELL differentiation, ETHNIC groups, GENES, INTERFERONS, RACE, REGRESSION analysis, SYSTEMIC lupus erythematosus, TRANSCRIPTION factors, WHITE people, RECEIVER operating characteristic curves, DNA methylation, EPIGENOMICS, DISEASE risk factors
Abstract

Objective: To determine the stage of B cell development at which a systemic lupus erythematosus (SLE)–associated DNA methylation signature originates in African American (AA) and European American (EA) subjects, and to assess whether epigenetic defects in B cell development patterns could be predictive of SLE status in individual and mixed immune cell populations. Methods: B cells from AA patients (n = 31) and EA patients (n = 49) with or without SLE were sorted using fluorescence‐activated cell sorting into 5 B cell subsets. DNA methylation, measured at ~460,000 CpG sites, was interrogated in each subset. Enrichment analysis of transcription factor interaction at SLE‐associated methylation sites was performed. A random forests algorithm was used to identify an epigenetic signature of SLE in the B cell subsets, which was then validated in an independent cohort of AA and EA patients and healthy controls. Results: Regression analysis across all B cell stages resulted in identification of 60 CpGs that reached genome‐wide significance for SLE‐associated methylation differences (P ≤ 1.07 × 10−7). Interrogation of ethnicity‐specific CpGs associated with SLE revealed a hypomethylated pattern that was enriched for interferon (IFN)–regulated genes and binding of EBF1 in AA patients (each P < 0.001). AA patients with SLE could be distinguished from healthy controls when the predictive model developed with the transitional B cell subset was applied to other B cell subsets (mean receiver operating characteristic [ROC] area under the curve [AUC] 0.98), and when applied to CD19+ pan–B cells (mean ROC AUC 0.95) and CD4+ pan–T cells (mean ROC AUC 0.97) from the independent validation cohort. Conclusion: These results indicate that SLE‐specific methylation patterns are ethnicity dependent. A pattern of epigenetic changes near IFN‐regulated genes early in B cell development is a hallmark of SLE in AA female subjects. EBF1 binding sites are highly enriched for significant methylation changes, implying that this may be a potential regulator of SLE‐associated epigenetic changes. [ABSTRACT FROM AUTHOR]

Published
2020
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120. MRLR: unraveling high-resolution meiotic recombination by linked reads.

Author

Xu, Peng, Kennell, Timothy, Gao, Min, Consortium, Human Genome Structural Variation, Kimberly, Robert P, and Chong, Zechen

Subjects
GENETIC recombination, INTERNET servers, HOMOLOGOUS chromosomes, GAMETES
Abstract

Motivation Meiotic recombination facilitates the transmission of exchanged genetic material between homologous chromosomes and plays a crucial role in increasing the genetic variations in eukaryotic organisms. In humans, thousands of crossover events have been identified by genotyping related family members. However, most of these crossover regions span tens to hundreds of kb, which is not sufficient resolution to accurately identify the crossover breakpoints in a typical trio family. Results We have developed MRLR, a software using 10X linked reads to identify crossover events at a high resolution. By reconstructing the gamete genome, MRLR only requires a trio family dataset and can efficiently discover the crossover events. Using MRLR, we revealed a fine-scale pattern of crossover regions in six human families. From the two closest heterozygous alleles around the crossovers, we determined that MRLR achieved a median resolution 4.5 kb. This method can delineate a genome-wide landscape of crossover events at a precise scale, which is important for both functional and genomic features analysis of meiotic recombination. Availability and implementation MRLR is freely available at https://github.com/ChongLab/MRLR , implemented in Perl. Supplementary information Supplementary data are available at Bioinformatics online. [ABSTRACT FROM AUTHOR]

Published
2020
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121. Genetic influences on susceptibility to rheumatoid arthritis in African-Americans

Author

Laufer, Vincent A, primary, Tiwari, Hemant K, additional, Reynolds, Richard J, additional, Danila, Maria I, additional, Wang, Jelai, additional, Edberg, Jeffrey C, additional, Kimberly, Robert P, additional, Kottyan, Leah C, additional, Harley, John B, additional, Mikuls, Ted R, additional, Gregersen, Peter K, additional, Absher, Devin M, additional, Langefeld, Carl D, additional, Arnett, Donna K, additional, and Bridges, Jr, S Louis, additional

Published
2018
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122. Genome-wide association studies suggest that APOL1-environment interactions more likely trigger kidney disease in African Americans with nondiabetic nephropathy than strong APOL1–second gene interactions

Author

Langefeld, Carl D., primary, Comeau, Mary E., additional, Ng, Maggie C.Y., additional, Guan, Meijian, additional, Dimitrov, Latchezar, additional, Mudgal, Poorva, additional, Spainhour, Mitzie H., additional, Julian, Bruce A., additional, Edberg, Jeffrey C., additional, Croker, Jennifer A., additional, Divers, Jasmin, additional, Hicks, Pamela J., additional, Bowden, Donald W., additional, Chan, Gary C., additional, Ma, Lijun, additional, Palmer, Nicholette D., additional, Kimberly, Robert P., additional, and Freedman, Barry I., additional

Published
2018
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123. Genetic fine mapping of systemic lupus erythematosus MHC associations in Europeans and African Americans

Author

Hanscombe, Ken B, primary, Morris, David L, additional, Noble, Janelle A, additional, Dilthey, Alexander T, additional, Tombleson, Philip, additional, Kaufman, Kenneth M, additional, Comeau, Mary, additional, Langefeld, Carl D, additional, Alarcon-Riquelme, Marta E, additional, Gaffney, Patrick M, additional, Jacob, Chaim O, additional, Sivils, Kathy L, additional, Tsao, Betty P, additional, Alarcon, Graciela S, additional, Brown, Elizabeth E, additional, Croker, Jennifer, additional, Edberg, Jeff, additional, Gilkeson, Gary, additional, James, Judith A, additional, Kamen, Diane L, additional, Kelly, Jennifer A, additional, McCune, Joseph, additional, Merrill, Joan T, additional, Petri, Michelle, additional, Ramsey-Goldman, Rosalind, additional, Reveille, John D, additional, Salmon, Jane E, additional, Scofield, Hal, additional, Utset, Tammy, additional, Wallace, Daniel J, additional, Weisman, Michael H, additional, Kimberly, Robert P, additional, Harley, John B, additional, Lewis, Cathryn M, additional, Criswell, Lindsey A, additional, and Vyse, Timothy J, additional

Published
2018
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124. Genetic variants at the 16p13 locus confer risk for eosinophilic esophagitis

Author

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

Published
2018
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126. A plausibly causal functional lupus-associated risk variant in the STAT1–STAT4 locus

Author

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

Published
2018
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127. Transancestral mapping and genetic load in systemic lupus erythematosus

Author

Langefeld, Carl D., Ainsworth, Hannah C., Graham, Deborah S. Cunninghame, Kelly, Jennifer A., Comeau, Mary E., Marion, Miranda C., Howard, Timothy D., Ramos, Paula S., Croker, Jennifer A., Morris, David L., Sandling, Johanna K., Carlsson Almlöf, Jonas, Acevedo-Vasquez, Eduardo M., Alarcon, Graciela S., Babini, Alejandra M., Baca, Vicente, Bengtsson, Anders A., Berbotto, Guillermo A., Bijl, Marc, Brown, Elizabeth E., Brunner, Hermine I., Cardiel, Mario H., Catoggio, Luis, Cervera, Ricard, Cucho-Venegas, Jorge M., Dahlqvist, Solbritt Rantapaa, D'Alfonso, Sandra, Da Silva, Berta Martins, de la Rua Figueroa, Inigo, Doria, Andrea, Edberg, Jeffrey C., Endreffy, Emoke, Esquivel-Valerio, Jorge A., Fortin, Paul R., Freedman, Barry I., Frostegard, Johan, Garcia, Mercedes A., Garcia de la Torre, Ignacio, Gilkeson, Gary S., Gladman, Dafna D., Gunnarsson, Iva, Guthridge, Joel M., Huggins, Jennifer L., James, Judith A., Kallenberg, Cees G. M., Kamen, Diane L., Karp, David R., Kaufman, Kenneth M., Kottyan, Leah C., Kovacs, Laszlo, Laustrup, Helle, Lauwerys, Bernard R., Li, Quan-Zhen, Maradiaga-Cecena, Marco A., Martin, Javier, McCune, Joseph M., McWilliams, David R., Merrill, Joan T., Miranda, Pedro, Moctezuma, Jose F., Nath, Swapan K., Niewold, Timothy B., Orozco, Lorena, Ortego-Centeno, Norberto, Petri, Michelle, Pineau, Christian A., Pons-Estel, Bernardo A., Pope, Janet, Raj, Prithvi, Ramsey-Goldman, Rosalind, Reveille, John D., Russell, Laurie P., Sabio, Jose M., Aguilar-Salinas, Carlos A., Scherbarth, Hugo R., Scorza, Raffaella, Seldin, Michael F., Sjowall, Christopher, Svenungsson, Elisabet, Thompson, Susan D., Toloza, Sergio M. A., Truedsson, Lennart, Tusie-Luna, Teresa, Vasconcelos, Carlos, Vila, Luis M., Wallace, Daniel J., Weisman, Michael H., Wither, Joan E., Bhangale, Tushar, Oksenberg, Jorge R., Rioux, John D., Gregersen, Peter K., Syvänen, Ann-Christine, Rönnblom, Lars, Criswell, Lindsey A., Jacob, Chaim O., Sivils, Kathy L., Tsao, Betty P., Schanberg, Laura E., Behrens, Timothy W., Silverman, Earl D., Alarcon-Riquelme, Marta E., Kimberly, Robert P., Harley, John B., Wakeland, Edward K., Graham, Robert R., Gaffney, Patrick M., Vyse, Timothy J., Langefeld, Carl D., Ainsworth, Hannah C., Graham, Deborah S. Cunninghame, Kelly, Jennifer A., Comeau, Mary E., Marion, Miranda C., Howard, Timothy D., Ramos, Paula S., Croker, Jennifer A., Morris, David L., Sandling, Johanna K., Carlsson Almlöf, Jonas, Acevedo-Vasquez, Eduardo M., Alarcon, Graciela S., Babini, Alejandra M., Baca, Vicente, Bengtsson, Anders A., Berbotto, Guillermo A., Bijl, Marc, Brown, Elizabeth E., Brunner, Hermine I., Cardiel, Mario H., Catoggio, Luis, Cervera, Ricard, Cucho-Venegas, Jorge M., Dahlqvist, Solbritt Rantapaa, D'Alfonso, Sandra, Da Silva, Berta Martins, de la Rua Figueroa, Inigo, Doria, Andrea, Edberg, Jeffrey C., Endreffy, Emoke, Esquivel-Valerio, Jorge A., Fortin, Paul R., Freedman, Barry I., Frostegard, Johan, Garcia, Mercedes A., Garcia de la Torre, Ignacio, Gilkeson, Gary S., Gladman, Dafna D., Gunnarsson, Iva, Guthridge, Joel M., Huggins, Jennifer L., James, Judith A., Kallenberg, Cees G. M., Kamen, Diane L., Karp, David R., Kaufman, Kenneth M., Kottyan, Leah C., Kovacs, Laszlo, Laustrup, Helle, Lauwerys, Bernard R., Li, Quan-Zhen, Maradiaga-Cecena, Marco A., Martin, Javier, McCune, Joseph M., McWilliams, David R., Merrill, Joan T., Miranda, Pedro, Moctezuma, Jose F., Nath, Swapan K., Niewold, Timothy B., Orozco, Lorena, Ortego-Centeno, Norberto, Petri, Michelle, Pineau, Christian A., Pons-Estel, Bernardo A., Pope, Janet, Raj, Prithvi, Ramsey-Goldman, Rosalind, Reveille, John D., Russell, Laurie P., Sabio, Jose M., Aguilar-Salinas, Carlos A., Scherbarth, Hugo R., Scorza, Raffaella, Seldin, Michael F., Sjowall, Christopher, Svenungsson, Elisabet, Thompson, Susan D., Toloza, Sergio M. A., Truedsson, Lennart, Tusie-Luna, Teresa, Vasconcelos, Carlos, Vila, Luis M., Wallace, Daniel J., Weisman, Michael H., Wither, Joan E., Bhangale, Tushar, Oksenberg, Jorge R., Rioux, John D., Gregersen, Peter K., Syvänen, Ann-Christine, Rönnblom, Lars, Criswell, Lindsey A., Jacob, Chaim O., Sivils, Kathy L., Tsao, Betty P., Schanberg, Laura E., Behrens, Timothy W., Silverman, Earl D., Alarcon-Riquelme, Marta E., Kimberly, Robert P., Harley, John B., Wakeland, Edward K., Graham, Robert R., Gaffney, Patrick M., and Vyse, Timothy J.

Abstract

Systemic lupus erythematosus (SLE) is an autoimmune disease with marked gender and ethnic disparities. We report a large transancestral association study of SLE using Immunochip genotype data from 27,574 individuals of European (EA), African (AA) and Hispanic Amerindian (HA) ancestry. We identify 58 distinct non-HLA regions in EA, 9 in AA and 16 in HA (similar to 50% of these regions have multiple independent associations); these include 24 novel SLE regions (P < 5 x 10(-8)), refined association signals in established regions, extended associations to additional ancestries, and a disentangled complex HLA multigenic effect. The risk allele count (genetic load) exhibits an accelerating pattern of SLE risk, leading us to posit a cumulative hit hypothesis for autoimmune disease. Comparing results across the three ancestries identifies both ancestry-dependent and ancestry-independent contributions to SLE risk. Our results are consistent with the unique and complex histories of the populations sampled, and collectively help clarify the genetic architecture and ethnic disparities in SLE.

Published
2017
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128. Transancestral mapping and genetic load in systemic lupus erythematosus

Author

National Institute for Health Research (UK), Arthritis Research UK, Alliance for Lupus Research, Junta de Andalucía, National Institute of Arthritis and Musculoskeletal and Skin Diseases (US), National Institutes of Health (US), RILITE Foundation, Genentech Foundation, Langefeld, C. D., Ainsworth, H. C., Kelly, J. A., Comeau, M. E., Marion, M. C., Howard, T. D., Ramos, P. S., Croker, J. A., Morris, D. L., Sandling, J. K., Almlöf, J. C., Pons-Estel, Bernardo A., Pope, Janet, Raj, Prithvi, Ramsey-Goldman, Rosalind, Reveille, John D., Russell, Laurie P., Sabio, José Mario, Aguilar-Salinas, Carlos A., Scherbarth, Hugo R., Scorza, Raffaella, Seldin, Michael F., Sjowall, Christopher, Svenungsson, Elisabet, Thompson, Susan D., Toloza, Sergio M. A., Truedsson, Lennart, Tusie-Luna, Teresa, Vasconcelos, C., Vilá, Luis M., Wallace, Daniel J., Weisman, Michael H., Wither, Joan E., Bhangale, Tushar, Oksenberg, Jorge R., Rioux, John D., Gregersen, Peter K., Syvanen, Ann-Christine, Ronnblom, Lars, Criswell, Lindsey A., Jacob, Chaim O., Sivils, Kathy L., Tsao, Betty P., Schanberg, Laura E., Behrens, Timothy W., Silverman, Earl D., Alarcón-Riquelme, M. E., Kimberly, Robert P., Harley, John B., Wakeland, Edward K., Graham, Robert R., Gaffney, P. M., Vyse, Timothy J., Acevedo-Vásquez, E. M., Alarcón, G. S., Babini, A. M., Baca, V., Bengtsson, A. A., Berbotto, G. A., Bij, l. M., Brown, E. E., Brunner, H.I., Cardiel, Mario H., Catoggio, Luis, Cervera, Ricard, Cucho-Venegas, Jorge M., Dahlqvist, Solbritt Rantapaa, D'Alfonso, Sandra, Da Silva, Berta Martins, de la Rua Figueroa, Inigo, Doria, Andrea, Edberg, Jeffrey C., Endreffy, Emoke, Esquivel-Valerio, Jorge A., Fortin, Paul R., Freedman, Barry I., Frostegård, Johan, García, Mercedes A., García de la Torre, Ignacio, Gilkeson, G. S., Gladman, Dafna D., Gunnarsson, Iva, Guthridge, Joel M., Huggins, Jennifer L., James, Judith A., Kallenberg, Cees G. M., Kamen, D. L., Karp, David R., Kaufman, Kenneth M, Kottyan, Leah C., Kovacs, Laszlo, Laustrup, Helle, Lauwerys, Bernard R., Li, Quan-Zhen, Maradiaga-Cecena, Marco A., Martín, J., McCune, Joseph M., McWilliams, David R, Merrill, Joan T, Miranda, Pedro, Moctezuma, Jose F., Nath, Swapan K., Niewold, Timothy B., Orozco, Lorena, Ortego-Centeno, N., Petri, Michelle, Pineau, Christian A., National Institute for Health Research (UK), Arthritis Research UK, Alliance for Lupus Research, Junta de Andalucía, National Institute of Arthritis and Musculoskeletal and Skin Diseases (US), National Institutes of Health (US), RILITE Foundation, Genentech Foundation, Langefeld, C. D., Ainsworth, H. C., Kelly, J. A., Comeau, M. E., Marion, M. C., Howard, T. D., Ramos, P. S., Croker, J. A., Morris, D. L., Sandling, J. K., Almlöf, J. C., Pons-Estel, Bernardo A., Pope, Janet, Raj, Prithvi, Ramsey-Goldman, Rosalind, Reveille, John D., Russell, Laurie P., Sabio, José Mario, Aguilar-Salinas, Carlos A., Scherbarth, Hugo R., Scorza, Raffaella, Seldin, Michael F., Sjowall, Christopher, Svenungsson, Elisabet, Thompson, Susan D., Toloza, Sergio M. A., Truedsson, Lennart, Tusie-Luna, Teresa, Vasconcelos, C., Vilá, Luis M., Wallace, Daniel J., Weisman, Michael H., Wither, Joan E., Bhangale, Tushar, Oksenberg, Jorge R., Rioux, John D., Gregersen, Peter K., Syvanen, Ann-Christine, Ronnblom, Lars, Criswell, Lindsey A., Jacob, Chaim O., Sivils, Kathy L., Tsao, Betty P., Schanberg, Laura E., Behrens, Timothy W., Silverman, Earl D., Alarcón-Riquelme, M. E., Kimberly, Robert P., Harley, John B., Wakeland, Edward K., Graham, Robert R., Gaffney, P. M., Vyse, Timothy J., Acevedo-Vásquez, E. M., Alarcón, G. S., Babini, A. M., Baca, V., Bengtsson, A. A., Berbotto, G. A., Bij, l. M., Brown, E. E., Brunner, H.I., Cardiel, Mario H., Catoggio, Luis, Cervera, Ricard, Cucho-Venegas, Jorge M., Dahlqvist, Solbritt Rantapaa, D'Alfonso, Sandra, Da Silva, Berta Martins, de la Rua Figueroa, Inigo, Doria, Andrea, Edberg, Jeffrey C., Endreffy, Emoke, Esquivel-Valerio, Jorge A., Fortin, Paul R., Freedman, Barry I., Frostegård, Johan, García, Mercedes A., García de la Torre, Ignacio, Gilkeson, G. S., Gladman, Dafna D., Gunnarsson, Iva, Guthridge, Joel M., Huggins, Jennifer L., James, Judith A., Kallenberg, Cees G. M., Kamen, D. L., Karp, David R., Kaufman, Kenneth M, Kottyan, Leah C., Kovacs, Laszlo, Laustrup, Helle, Lauwerys, Bernard R., Li, Quan-Zhen, Maradiaga-Cecena, Marco A., Martín, J., McCune, Joseph M., McWilliams, David R, Merrill, Joan T, Miranda, Pedro, Moctezuma, Jose F., Nath, Swapan K., Niewold, Timothy B., Orozco, Lorena, Ortego-Centeno, N., Petri, Michelle, and Pineau, Christian A.

Abstract

Systemic lupus erythematosus (SLE) is an autoimmune disease with marked gender and ethnic disparities. We report a large transancestral association study of SLE using Immunochip genotype data from 27,574 individuals of European (EA), African (AA) and Hispanic Amerindian (HA) ancestry. We identify 58 distinct non-HLA regions in EA, 9 in AA and 16 in HA (similar to 50% of these regions have multiple independent associations); these include 24 novel SLE regions (P < 5 x 10(-8)), refined association signals in established regions, extended associations to additional ancestries, and a disentangled complex HLA multigenic effect. The risk allele count (genetic load) exhibits an accelerating pattern of SLE risk, leading us to posit a cumulative hit hypothesis for autoimmune disease. Comparing results across the three ancestries identifies both ancestry-dependent and ancestry-independent contributions to SLE risk. Our results are consistent with the unique and complex histories of the populations sampled, and collectively help clarify the genetic architecture and ethnic disparities in SLE.

Published
2017

129. Fosmid clonal library used to screen for a novel variant of FCGR2

Author

Howton, T.C., Ptacek, Travis, Redden, David T., Li, Xinrui, Ji, Chuanyi, Edberg, Jeffrey C., Mukhtar, Shahid, and Kimberly, Robert P.

Subjects
Systemic lupus erythematosus -- Genetic aspects, Genomic libraries -- Research, Plasmids -- Research, Science and technology
Abstract

FOSMID CLONAL LIBRARY USED TO SCREEN FOR A NOVEL VARIANT OF FCGR2B. T.C. HOWTON, TRAVIS PTACEK, DAVID T REDDEN, XINRUI LI, CHUANYI JI, JEFFREY C EDBERG, SHAHID MUKHTAR, ROBERT P [...]

Published
2015

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

Author

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

Subjects
Gene dosage, Liver Cirrhosis, Sarcoidosis, Sex Chromosome Disorders of Sex Development, Case control study, Trisomy, Major clinical study, XXX, Article, Fluorescence, Chromosomes, Autoimmune Diseases, X chromosome, Systemic lupus erythematosus, Rheumatoid, Autoimmune disease, Prevalence, Live birth, Humans, Rheumatoid arthritis, Sex Distribution, Sex Chromosome Aberrations, In Situ Hybridization, Priority journal, Lupus Erythematosus, Fluorescence in situ hybridization, Arthritis, Systemic, Biliary, Quality control, Polymerase chain reaction, Single nucleotide polymorphism, Sjogren's Syndrome, Primary biliary cirrhosis, Sex chromosome aberration, Case-Control Studies, Female, Sex, Karyotype 47, Controlled study, Sex ratio, Human
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 Sjögren'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. © 2016, American College of Rheumatology.

Published
2016
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132. Evaluation ofTRAF6in a large multiancestral lupus cohort

Author

Namjou, Bahram, Choi, Chan-Bum, Harley, Isaac T. W., Alarcón-Riquelme, Marta E., Kelly, Jennifer A., Glenn, Stuart B., Ojwang, Joshua O., Adler, Adam, Kwangwoo Kim, Gallant, Caroline J., Boackle, Susan A., Criswell, Lindsey A., Kimberly, Robert P., Brown, Elizabeth E., Edberg, Jeffrey, Alarcón, Graciela S., Stevens, Anne M., Jacob, Chaim O., Gilkeson, Gary S., Kamen, Diane L., Tsao, Betty P., Anaya, Juan-Manuel, Kim, Eun-Mi, Park, So-Yeon, Sung, Yoon-Kyoung, Guthridge, Joel M., Merrill, Joan T., Petri, Michelle, Ramsey-Goldman, Rosalind, Vilá, Luis M., Niewold, Timothy B., Martin, Javier, Pons-Estel, Bernardo A., Vyse, Timothy J., Freedman, Barry I., Moser, Kathy L., Gaffney, Patrick M., Williams, Adrienne H., Comeau, Mary E., Reveille, John D., Kang, Changwon, James, Judith A., Scofield, R. Hal, Langefeld, Carl D., Kaufman, Kenneth M., Harley, John B., Bae, Sang-Cheol, Junker, Peter, Voss, Anne, and Laustrup, Helle

Subjects
single nucleotide, Male, Linkage disequilibrium, Candidate gene, Heredity, Organogenesis, Tumor necrosis factor receptor associated factor 6, Genome-wide association study, Signal transduction, Cohort Studies, Genetic heterogeneity, Gene Frequency, immune system diseases, Ethnicity, Lupus Erythematosus, Systemic, Immunology and Allergy, Pharmacology (medical), skin and connective tissue diseases, Priority journal, education.field_of_study, Calculation, Gene linkage disequilibrium, Female, Human, Immunopathogenesis, Genotype, Immunology, Population, Single-nucleotide polymorphism, Major clinical study, Biology, Pedigree analysis, Polymorphism, Single Nucleotide, Article, Systemic lupus erythematosus, Rheumatology, Population based case control study, Humans, Genetic Predisposition to Disease, African american, Rheumatoid arthritis, Polymorphism, education, Alleles, Genetic Association Studies, Genetic association, TNF Receptor-Associated Factor 6, Lupus erythematosus, Immunity, Case-control study, Odds ratio, systemic, Thrombocytopenia, Single nucleotide polymorphism, Haplotypes, Case-Control Studies, Meta analysis (topic), Controlled study
Abstract

Objective Systemic lupus erythematosus (SLE) is a heterogeneous autoimmune disease with significant immune system aberrations resulting from complex heritable genetics as well as environmental factors. We undertook to study the role of TRAF6 as a candidate gene for SLE, since it plays a major role in several signaling pathways that are important for immunity and organ development. Methods Fifteen single-nucleotide polymorphisms (SNPs) across TRAF6 were evaluated in 7,490 SLE patients and 6,780 control subjects from different ancestries. Population-based case-control association analyses and meta-analyses were performed. P values, false discovery rate q values, and odds ratios (ORs) with 95% confidence intervals (95% CIs) were calculated. Results Evidence of associations was detected in multiple SNPs. The best overall P values were obtained for SNPs rs5030437 and rs4755453 (P = 7.85 × 10 -5 and P = 4.73 × 10 -5, respectively) without significant heterogeneity among populations (P = 0.67 and P = 0.50, respectively, in Q statistic). In addition, SNP rs540386, which was previously reported to be associated with rheumatoid arthritis (RA), was found to be in linkage disequilibrium with these 2 SNPs (r 2 = 0.95) and demonstrated evidence of association with SLE in the same direction (meta-analysis P = 9.15 × 10 -4, OR 0.89 [95% CI 0.83-0.95]). The presence of thrombocytopenia improved the overall results in different populations (meta-analysis P = 1.99 × 10 -6, OR 0.57 [95% CI 0.45-0.72], for rs5030470). Finally, evidence of family-based association in 34 African American pedigrees with the presence of thrombocytopenia was detected in 1 available SNP (rs5030437) with a Z score magnitude of 2.28 (P = 0.02) under a dominant model. Conclusion Our data indicate the presence of association of TRAF6 with SLE, consistent with the previous report of association with RA. These data provide further support for the involvement of TRAF6 in the pathogenesis of autoimmunity. Copyright © 2012 by the American College of Rheumatology.

Published
2012
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133. Transancestral mapping and genetic load in systemic lupus erythematosus

Author

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

Published
2017
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134. Association of response to TNF inhibitors in rheumatoid arthritis with quantitative trait loci for and CD39.

Author

Spiliopoulou, Athina, Colombo, Marco, Plant, Darren, Nair, Nisha, Jing Cui, Coenen, Marieke J. H., Ikari, Katsunori, Yamanaka, Hisashi, Saevarsdottir, Saedis, Padyukov, Leonid, Bridges, Louis, Kimberly, Robert P., Okada, Yukinori, van Riel, Piet L. C. M., Wolbink, Gertjan, van der Horst-Bruinsma, Irene E., de Vries, Niek, Tak, Paul P., Ohmura, Koichiro, and Canhão, Helena

Abstract

Objectives: We sought to investigate whether genetic effects on response to TNF inhibitors (TNFi) in rheumatoid arthritis (RA) could be localised by considering known genetic susceptibility loci for relevant traits and to evaluate the usefulness of these genetic loci for stratifying drug response.Methods: We studied the relation of TNFi response, quantified by change in swollen joint counts ( Δ SJC) and erythrocyte sedimentation rate ( Δ ESR) with locus-specific scores constructed from genome-wide assocation study summary statistics in 2938 genotyped individuals: 37 scores for RA; scores for 19 immune cell traits; scores for expression or methylation of 93 genes with previously reported associations between transcript level and drug response. Multivariate associations were evaluated in penalised regression models by cross-validation.Results: We detected a statistically significant association between Δ SJC and the RA score at the CD40 locus (p=0.0004) and an inverse association between Δ SJC and the score for expression of CD39 on CD4 T cells (p=0.00005). A previously reported association between CD39 expression on regulatory T cells and response to methotrexate was in the opposite direction. In stratified analysis by concomitant methotrexate treatment, the inverse association was stronger in the combination therapy group and dissipated in the TNFi monotherapy group. Overall, ability to predict TNFi response from genotypic scores was limited, with models explaining less than 1% of phenotypic variance.Conclusions: The association with the CD39 trait is difficult to interpret because patients with RA are often prescribed TNFi after failing to respond to methotrexate. The CD39 and CD40 pathways could be relevant for targeting drug therapy. [ABSTRACT FROM AUTHOR]

Published
2019
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136. X Chromosome Dose and Sex Bias in Autoimmune Diseases : Increased 47,XXX in Systemic Lupus Erythematosus and Sjögren's Syndrome

Author

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

Abstract

OBJECTIVE: More than 80% of autoimmune disease is female dominant, but the mechanism for this female bias is poorly understood. We suspected an X chromosome dose effect and hypothesized that trisomy X (47,XXX, 1 in ∼1,000 live female births) would be increased in female predominant diseases (e.g. systemic lupus erythematosus [SLE], primary Sjögren's syndrome [SS], primary biliary cirrhosis [PBC] and rheumatoid arthritis [RA]) compared to diseases without female predominance (sarcoidosis) and controls. METHODS: We identified 47,XXX subjects using aggregate data from single nucleotide polymorphism (SNP) arrays and confirmed, when possible, by fluorescent in situ hybridization (FISH) or quantitative polymerase chain reaction (q-PCR). RESULTS: We found 47,XXX in seven of 2,826 SLE and three of 1,033 SS female patients, but only in two of the 7,074 female controls (p=0.003, OR=8.78, 95% CI: 1.67-86.79 and p=0.02, OR=10.29, 95% CI: 1.18-123.47; respectively). One 47,XXX subject was present for ∼404 SLE women and ∼344 SS women. 47,XXX was present in excess among SLE and SS subjects. CONCLUSION: The estimated prevalence of SLE and SS in women with 47,XXX was respectively ∼2.5 and ∼2.9 times higher than in 46,XX women and ∼25 and ∼41 times higher than in 46,XY men. No statistically significant increase of 47,XXX was observed in other female-biased diseases (PBC or RA), supporting the idea of multiple pathways to sex bias in autoimmunity. This article is protected by copyright. All rights reserved.

Published
2016
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137. Letter to the Editor Response: Exploring COVID-19 Vaccine Hesitancy Among Stakeholders in African American and Latinx Communities in the Deep South Through the Lens of the Health Belief Model

Author

Bateman, Lori B., Hall, Allyson G., Anderson, William A., Cherrington, Andrea L., Helova, Anna, Judd, Suzanne, Kimberly, Robert, Oates, Gabriela R., Osborne, Tiffany, Ott, Corilyn, Ryan, Melissa, Strong, Christian, and Fouad, Mona N.

Abstract

The purpose of this submission to respond to a Letter to the Editor recently submitted regarding our manuscript, “Exploring COVID-19 Vaccine Hesitancy among Stakeholders in African American and Latinx Communities in the Deep South through the Lens of the Health Belief Model” published in the American Journal of Health Promotion in February, 2022. The manuscript reported on a study that had as its purpose to qualitatively explore perceptions related to COVID-19 vaccination intention among African American and Latinx participants and suggest potential intervention strategies.

Published
2023
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138. End-Stage Renal Disease in African Americans With Lupus Nephritis Is Associated With APOL1

Author

Freedman, Barry I., Langefeld, Carl D., Andringa, Kelly K., Croker, Jennifer A., Williams, Adrienne H., Garner, Neva E., Birmingham, Daniel J., Hebert, Lee A., Hicks, Pamela J., Segal, Mark S., Edberg, Jeffrey C., Brown, Elizabeth E., Alarcón, Graciela S., Costenbader, Karen H., Comeau, Mary E., Criswell, Lindsey A., Harley, John B., James, Judith A., Kamen, Diane L., Lim, S. Sam, Merrill, Joan T., Sivils, Kathy L., Niewold, Timothy B., Patel, Neha M., Petri, Michelle, Ramsey-Goldman, Rosalind, Reveille, John D., Salmon, Jane E., Tsao, Betty P., Gibson, Keisha L., Byers, Joyce R., Vinnikova, Anna K., Lea, Janice P., Julian, Bruce A., and Kimberly, Robert P.

Subjects
Adult, Male, Genotype, Middle Aged, Apolipoprotein L1, Lupus Nephritis, Article, White People, Black or African American, Apolipoproteins, Logistic Models, Risk Factors, Disease Progression, Humans, Kidney Failure, Chronic, Female, Genetic Predisposition to Disease, Lipoproteins, HDL, Alleles
Abstract

Lupus nephritis (LN) is a severe manifestation of systemic lupus erythematosus (SLE) that exhibits familial aggregation and may progress to end-stage renal disease (ESRD). LN is more prevalent among African Americans than among European Americans. This study was undertaken to investigate the hypothesis that the apolipoprotein L1 gene (APOL1) nephropathy risk alleles G1/G2, common in African Americans and rare in European Americans, contribute to the ethnic disparity in risk.APOL1 G1 and G2 nephropathy alleles were genotyped in 855 African American SLE patients with LN-ESRD (cases) and 534 African American SLE patients without nephropathy (controls) and tested for association under a recessive genetic model, by logistic regression.Ninety percent of the SLE patients were female. The mean ± SD age at SLE diagnosis was significantly lower in LN-ESRD cases than in SLE non-nephropathy controls (27.3 ± 10.9 years versus 39.5 ± 12.2 years). The mean ± SD time from SLE diagnosis to development of LN-ESRD in cases was 7.3 ± 7.2 years. The G1/G2 risk alleles were strongly associated with SLE-ESRD, with 25% of cases and 12% of controls having 2 nephropathy alleles (odds ratio [OR] 2.57, recessive model P = 1.49 × 10(-9)), and after adjustment for age, sex, and ancestry admixture (OR 2.72, P = 6.23 × 10(-6)). The age-, sex-, and admixture-adjusted population attributable risk for ESRD among patients with G1/G2 polymorphisms was 0.26, compared to 0.003 among European American patients. The mean time from SLE diagnosis to ESRD development was ∼2 years earlier among individuals with APOL1 risk genotypes (P = 0.01).APOL1 G1/G2 alleles strongly impact the risk of LN-ESRD in African Americans, as well as the time to progression to ESRD. The high frequency of these alleles in African Americans with near absence in European Americans explains an important proportion of the increased risk of LN-ESRD in African Americans.

Published
2014

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

Author

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

Published
2016
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144. Identification of a systemic lupus erythematosus risk locus spanningATG16L2, FCHSD2,andP2RY2in Koreans

Author

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

Published
2015
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145. SNPs in VKORC1 are Risk Factors for Systemic Lupus Erythematosus in Asians: Genetic risk factors for Lupus

Author

Kaiser, Rachel, Taylor, Kimberly E., Deng, Yun, Zhao, Jian, Li, Yonghong, Nititham, Joanne, Chang, Monica, Catanese, Joseph, Begovich, Ann B., Brown, Elizabeth E., Edberg, Jeffrey C., McGwin, Gerald, Alarcón, Graciela S., Ramsey-Goldman, Rosalind, Reveille, John D., Vila, Luis M., Petri, Michelle, Kimberly, Robert P., Feng, Xuebing, Sun, Lingyun, Shen, Nan, Li, Wei, Lu, Jian-Xin, Wakeland, Edward K., Li, Quan-Zhen, Yang, Wanling, Lau, Yu-Lung, Liu, Fei-Lan, Chang, Deh-Ming, Yu, Chack-Yung, Song, Yeong W., Howe, Hwee Siew, Tsao, Betty P., and Criswell, Lindsey A.

Subjects
Adult, Male, Venous Thrombosis, Hemostasis, Genotype, Middle Aged, Polymorphism, Single Nucleotide, Article, Mixed Function Oxygenases, Asian People, Risk Factors, Case-Control Studies, Vitamin K Epoxide Reductases, Humans, Lupus Erythematosus, Systemic, Female, Genetic Predisposition to Disease
Abstract

The increased risk of thrombosis in systemic lupus erythematosus (SLE) may be partially explained by interrelated genetic pathways for thrombosis and SLE. The present study was undertaken to investigate whether 33 established and novel single-nucleotide polymorphisms (SNPs) in 20 genes involved in hemostasis pathways that have been associated with deep venous thrombosis (DVT) in the general population are risk factors for SLE among Asian subjects.Patients in the discovery cohort were enrolled in 1 of 2 North American SLE cohorts. Patients in the replication cohort were enrolled in 1 of 4 Asian or 2 North American cohorts. We first genotyped 263 Asian patients with SLE and 357 healthy Asian control subjects for 33 SNPs in the discovery phase, and then genotyped 5 SNPs in up to an additional 1,496 patients and 993 controls in the replication phase. Patients were compared to controls for bivariate association with minor alleles. Principal components analysis was used to control for intra-Asian ancestry in the replication cohort.Two genetic variants in the gene VKORC1 were highly significant in both the discovery and replication cohorts: rs9934438 (in the discovery cohort, odds ratio [OR] 2.45, P=2×10(-9); in the replication cohort, OR 1.54, P=4×10(-6)) and rs9923231 (in the discovery cohort, OR 2.40, P=6×10(-9); in the replication cohort, OR 1.53, P=5×10(-6)). These associations were significant in the replication cohort after adjustment for intra-Asian ancestry: for rs9934438, OR 1.34, P=0.0029; for rs9923231, OR 1.34, P=0.0032.Genetic variants in VKORC1, which are involved in vitamin K reduction and associated with DVT, correlate with SLE development in Asian subjects. These results suggest that there may be intersecting genetic pathways for the development of SLE and thrombosis.

Published
2013

146. 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, Alarcn-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., Sivils, Kathy Moser, James, Judith A., Kamen, Diane L., Gilkeson, Gary S., Niewold, Timothy B., Merrill, Joan T., Scofield, R. Hal, Criswell, Lindsey A., Stevens, Anne M., Boackle, Susan A., Kim, Jae Hoon, Choi, Jiyoung, Pons-Estel, Bernardo A., Freedman, Barry I., Anaya, Juan Manuel, Martin, Javier, Yu, C. Yung, Chang, Deh Ming, Song, Yeong Wook, Langefeld, Carl D., Chen, Weiling, Grossman, Jennifer M., Cantor, Rita M., Hahn, Bevra H., Tsao, Betty P., Frostegård, Johan, Truedsson, Lennart, de Ramón, Enrique, Sabio, José M., Ortego-Centeno, Norberto, CAllejas, José Luis, González-Escribano, María F., Sánchez-Román, Julio, D'Alfonso, Sandra, Migliarese, Sergio, Sebastiani, Gian Domenico, Galeazzi, Mauro, Witte, Torsten, Lauwerys, Bernard R., Endreffy, Emoke, Kovács, László, Vasconcelos, Carlos, da Silva, Berta Martins, Scherbarth, Hugo R., Marino, Pilar C., Motta, Estela L., Gamron, Susana, Drenkard, Cristina, Menso, Emilia, Allievi, Alberto, Tate, Guillermo A., Presas, Jose L., Palatnik, Simon A., Abdala, Marcelo, Bearzotti, Mariela, Alvarellos, Alejandro, Caeiro, Francisco, Bertoli, Ana, Paira, Sergio, Roverano, Susana, Graf, Cesar E., Bertero, Estela, Caprarulo, Cesar, Buchanan, Griselda, Guillerón, Carolina, Grimaudo, Sebastian, Manni, Jorge, Catoggio, Luis J., Soriano, Enrique R., Santos, Carlos D., Prigione, Cristina, Ramos, Fernando A., Navarro, Sandra M., Berbotto, Guillermo A., Jorfen, Marisa, Romero, Elisa J., Garcia, Mercedes A., Marcos, Juan C., Marcos, Ana I., Perandones, Carlos E., Eimon, Alicia, Parque, Sanatorio, Battagliotti, Cristina G., Acevedo, Eduardo, Cucho, Mariano, de la Torre, Ignacio García, Ríos, Mario Cardiel, Moctezuma, José Francisco, and Ceceña, Marco Maradiaga

Subjects
Cancer Research, medicine.medical_treatment, Genome-wide association study, Gene, Disease predisposition, 0302 clinical medicine, Interleukin 10, immune system diseases, Lupus Erythematosus, Systemic, Disease activity, skin and connective tissue diseases, Genetics (clinical), Regulation of gene expression, 0303 health sciences, TGranscription factor Elk 1, Hispanic or Latino, Interleukin-10, Up-Regulation, 3. Good health, Cytokine, Research Article, Protein Binding, Genotype, lcsh:QH426-470, Inmunología, Single-nucleotide polymorphism, Down regulation, Biology, Polymorphism, Single Nucleotide, White People, 03 medical and health sciences, Asian People, Enfermedades autoinmunes, Lupus eritematoso sistémico, Genetics, medicine, Humans, Genetic Predisposition to Disease, Electrophoretic mobility shift assay, Gene cluster, Allele, Molecular Biology, Alleles, Ecology, Evolution, Behavior and Systematics, ets-Domain Protein Elk-1, 030304 developmental biology, Lupus erythematosus, medicine.disease, Enfermedades, Introns, lcsh:Genetics, Binding affinity, Gene Expression Regulation, Haplotypes, Immunology, Controlled study, Genome-Wide Association Study, 030215 immunology
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., Author Summary Systemic lupus erythematosus (SLE), a debilitating autoimmune disease characterized by the production of pathogenic autoantibodies, has a strong genetic basis. Variants of the IL10 gene, which encodes cytokine interleukin-10 (IL-10) with known function of promoting B cell hyperactivity and autoantibody production, are associated with SLE and other autoimmune diseases, and serum IL-10 levels are elevated in SLE patients correlating with increased disease activity. In this study, to discover SLE-predisposing causal variant(s), we assessed variants within the genomic region containing IL10 and its gene family member IL19, IL20 and IL24 for association with SLE in case and control subjects from diverse ancestries. We identified SLE-associated SNP rs3122605 located at 9.2 kb upstream of IL10 as the most likely causal variant in subjects of European ancestry. The SLE-risk allele of rs3122605 was dose-dependently associated with elevated IL10 expression at both mRNA and protein levels in peripheral blood samples from SLE patients and controls, which could be explained, at least in part, by its preferential binding to Elk-1, a transcription factor activated in B cells during active disease of SLE patients. Elk-1-mediated IL-10 overexpression could be downregulated by inhibiting activation of mitogen-activated protein kinases, suggesting a potential therapeutic target for SLE.

Published
2013
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147. Two Independent Functional Risk Haplotypes in TNIP1 are Associated with Systemic Lupus Erythematosus

Author

Adrianto, Indra, Wang, Shaofeng, Wiley, Graham B., Lessard, Christopher J., Kelly, Jennifer A., Adler, Adam J., Glenn, Stuart B., Williams, Adrienne H., Ziegler, Julie T., Comeau, Mary E., Marion, Miranda C., Wakeland, Benjamin E., Liang, Chaoying, Kaufman, Kenneth M., Guthridge, Joel M., Alarcón-Riquelme, Marta E., Alarcón, Graciela S., Anaya, Juan-Manuel, Bae, Sang-Cheol, Kim, Jae-Hoon, Joo, Young Bin, Boackle, Susan A., Brown, Elizabeth E., Petri, Michelle A., Ramsey-Goldman, Rosalind, Reveille, John D., Vilá, Luis M., Criswell, Lindsey A., Edberg, Jeffrey C., Freedman, Barry I., Gilkeson, Gary S., Jacob, Chaim O., James, Judith A., Kamen, Diane L., Kimberly, Robert P., Martin, Javier, Merrill, Joan T., Niewold, Timothy B., Pons-Estel, Bernardo A., Scofield, R. Hal, Stevens, Anne M., Tsao, Betty P., Vyse, Timothy J., Langefeld, Carl D., Harley, John B., Wakeland, Edward K., Moser, Kathy L., Montgomery, Courtney G., and Gaffney, Patrick M.

Subjects
Genetic Markers, Male, B-Lymphocytes, Asian, Intracellular Signaling Peptides and Proteins, Hispanic or Latino, Polymorphism, Single Nucleotide, Article, United States, White People, Neoplasm Proteins, Black or African American, DNA-Binding Proteins, Haplotypes, Risk Factors, Humans, Lupus Erythematosus, Systemic, Female, Genetic Predisposition to Disease, Adaptor Proteins, Signal Transducing, Cell Line, Transformed
Abstract

Systemic lupus erythematosus (SLE) is an autoimmune disease characterized by autoantibody production and altered type I interferon expression. Genetic surveys and genome-wide association studies have identified30 SLE susceptibility genes. One of these genes, TNIP1, encodes the ABIN1 protein. ABIN1 functions in the immune system by restricting NF-κB signaling. The present study was undertaken to investigate the genetic factors that influence association with SLE in genes that regulate the NF-κB pathway.We analyzed a dense set of genetic markers spanning TNIP1 and TAX1BP1, as well as the TNIP1 homolog TNIP2, in case-control populations of diverse ethnic origins. TNIP1, TNIP2, and TAX1BP1 were fine-mapped in a total of 8,372 SLE cases and 7,492 healthy controls from European-ancestry, African American, Hispanic, East Asian, and African American Gullah populations. Levels of TNIP1 messenger RNA (mRNA) and ABIN1 protein in Epstein-Barr virus-transformed human B cell lines were analyzed by quantitative reverse transcription-polymerase chain reaction and Western blotting, respectively.We found significant associations between SLE and genetic variants within TNIP1, but not in TNIP2 or TAX1BP1. After resequencing and imputation, we identified 2 independent risk haplotypes within TNIP1 in individuals of European ancestry that were also present in African American and Hispanic populations. Levels of TNIP1 mRNA and ABIN1 protein were reduced among subjects with these haplotypes, suggesting that they harbor hypomorphic functional variants that influence susceptibility to SLE by restricting ABIN1 expression.Our results confirm the association signals between SLE and TNIP1 variants in multiple populations and provide new insight into the mechanism by which TNIP1 variants may contribute to SLE pathogenesis.

Published
2012

148. Identification of IRF8, TMEM39A, and IKZF3-ZPBP2 as susceptibility loci for systemic lupus erythematosus in a large-scale multiracial replication study

Author

Lessard, Christopher J., Adrianto, Indra, Ice, John A., Wiley, Graham B., Kelly, Jennifer A., Glenn, Stuart B., Adler, Adam J., Li, He, Rasmussen, Astrid, Williams, Adrienne H., Ziegler, Julie, Comeau, Mary, Marion, Miranda, Wakeland, Benjamin E., Liang, Chaoying, Ramos, Paula S., Grundahl, Kiely M., Gallant, Caroline J., Alarcón-Riquelme, Marta E., Alarcón, Graciela S., Anaya, Juan-Manuel, Bae, Sang-Cheol, Boackle, Susan, Brown, Elizabeth E., Chang, Deh-Ming, Cho, Soo-Kyung, Criswel, Lindsey A., Edberg, Jeffrey C., Freedman, Barry I., Gilkeson, Gary S., Jacob, Chaim O., James, Judith A., Kamen, Diane L., Kimberly, Robert P., Kim, Jae-Hoon, Martin, Javier, Merrill, Joan T., Niewold, Timothy B., Park, So-Yeon, Petri, Michelle A., Pons-Estel, Bernardo A., Ramsey-Goldman, Rosalind, Reveille, John D., Scofield, Robert H., Song, Yeong Wook, Stevens, Anne M., Tsao, Betty P., Vila, Luis M., Vyse, Timothy J., Yu, Chack-Yung, Guthridge, Joel M., Kaufman, Kenneth M., Harley, John B., Wakeland, Edward K., Langefeld, Carl D., Gaffney, Patrick M., Montgomery, Courtney G., and Moser, Kathy L.

Subjects
Male, Chromosome 17Q, Hispanic, Ikzf3 Gene, Genetic Susceptibility, Gene, Genetic Risk, Or8D4 Gene, Indians, Lpp Gene, Ethnicity, Haplotype, African American, European American, Membrane Protein, Immune Response, Irf8 Gene, African Continental Ancestry Group, Transmembrane Protein 39A, Cadm2 Gene, C1Orf64 Gene, Chromosome Mapping, Fam19A2 Gene, Patología, Single Nucleotide, Slu7 Gene, Tmem39A Gene, Genetic Predisposition To Disease, High Risk Population, Interferon Consensus Sequence Binding Protein, Gene Locus, Zpbp2 Gene, Genetic Variability, American Indian, Interferon Regulatory Factors, Priority Journal, Interferon, Female, Hispanic Americans, Sequence Analysis, Genetic Association, North American, Human, Asian Continental Ancestry Group, Gene Sequence, Genotype, Major Clinical Study, European Continental Ancestry Group, Protein Ikzf3, Il12A Gene, Loc6392 Gene, Systemic Lupus Erythematosus, Article, Heritability, Ikaros Transcription Factor, Unclassified Drug, Autoantigen, Lupus eritematoso sistémico, Humans, Zona Pellucida Binding Protein 2, Controlled Study, Gene Identification, Polymorphism, Cfhr1 Gene, Asian, Environmental Factor, Lupus Erythematosus, Gene Mapping, Egg Proteins, Systemic, Immunoregulation, Membrane Proteins, Dna, Genome Analysis, Genética, Haplotypes, Stxbp6 Gene, Single Nucleotide Polymorphism, Adamtsl1 Gene, Immunological Tolerance
Abstract

Systemic lupus erythematosus (SLE) is a chronic heterogeneous autoimmune disorder characterized by the loss of tolerance to self-antigens and dysregulated interferon responses. The etiology of SLE is complex, involving both heritable and environmental factors. Candidate-gene studies and genome-wide association (GWA) scans have been successful in identifying new loci that contribute to disease susceptibility; however, much of the heritable risk has yet to be identified. In this study, we sought to replicate 1,580 variants showing suggestive association with SLE in a previously published GWA scan of European Americans; we tested a multiethnic population consisting of 7,998 SLE cases and 7,492 controls of European, African American, Asian, Hispanic, Gullah, and Amerindian ancestry to find association with the disease. Several genes relevant to immunological pathways showed association with SLE. Three loci exceeded the genome-wide significance threshold: interferon regulatory factor 8 (IRF8; rs11644034; p meta-Euro = 2.08 × 10 -10), transmembrane protein 39A (TMEM39A; rs1132200; p meta-all = 8.62 × 10 -9), and 17q21 (rs1453560; p meta-all = 3.48 × 10 -10) between IKAROS family of zinc finger 3 (AIOLOS; IKZF3) and zona pellucida binding protein 2 (ZPBP2). Fine mapping, resequencing, imputation, and haplotype analysis of IRF8 indicated that three independent effects tagged by rs8046526, rs450443, and rs4843869, respectively, were required for risk in individuals of European ancestry. Eleven additional replicated effects (5 × 10 -8 < p meta-Euro < 9.99 × 10 -5) were observed with CFHR1, CADM2, LOC730109/IL12A, LPP, LOC63920, SLU7, ADAMTSL1, C10orf64, OR8D4, FAM19A2, and STXBP6. The results of this study increase the number of confirmed SLE risk loci and identify others warranting further investigation. © 2012 The American Society of Human Genetics.

Published
2012

149. Association of PPP2CA polymorphisms with SLE susceptibility in multiple ethnic groups

Author

Tan, Wenfeng, Sunahori, Katsue, Zhao, Jian, Deng, Yun, Kaufman, Kenneth M., Kelly, Jennifer A., Langefeld, Carl D., Williams, Adrienne H., Comeau, Mary E., Ziegler, Julie T., Marion, Miranda C., Bae, Sang-Cheol, Lee, Joo Hyun, Lee, Ji-Seon, Chang, Deh-Ming, Song, Yeong Wook, Yu, Chack-Yung, Kimberly, Robert P., Edberg, Jeffrey C., Brown, Elizabeth E., Petri, Michelle A., Ramsey-Goldman, Rosalind, Vilá, Luis M., Reveille, John D., Alarcón-Riquelme, Marta E., Harley, John B., Boackle, Susan A., Stevens, Anne M., Scofield, R. Hal, Merrill, Joan T., Freedman, Barry I., Anaya, Juan-Manuel, Criswell, Lindsey A., Jacob, Chaim O., Vyse, Timothy J., Niewold, Timothy B., Gaffney, Patrick M., Moser, Kathy L., Gilkeson, Gary S., Kamen, Diane L., James, Judith A., Grossman, Jennifer M., Hahn, Bevra H., Tsokos, George C., and Tsao, Betty P.

Subjects
Adult, Male, Polymorphism, Genetic, Adolescent, Genotype, T-Lymphocytes, Hispanic or Latino, Middle Aged, Article, White People, Asian People, Haplotypes, Humans, Interleukin-2, Lupus Erythematosus, Systemic, Female, Genetic Predisposition to Disease, Protein Phosphatase 2, Alleles, Genetic Association Studies
Abstract

T cells from patients with systemic lupus erythematosus (SLE) express increased amounts of PP2Ac, which contributes to decreased production of interleukin-2 (IL-2). Because IL-2 is important in the regulation of several aspects of the immune response, it has been proposed that PP2Ac contributes to the expression of SLE. This study was designed to determine whether genetic variants of PPP2AC are linked to the expression of SLE and specific clinical manifestations and account for the increased expression of PP2Ac.We conducted a trans-ethnic study of 8,695 SLE cases and 7,308 controls of 4 different ancestries. Eighteen single-nucleotide polymorphisms (SNPs) across PPP2CA were genotyped using an Illumina custom array. PPP2CA expression in SLE and control T cells was analyzed by real-time polymerase chain reaction.A 32-kb haplotype comprising multiple SNPs of PPP2CA showed significant association with SLE in Hispanic Americans, European Americans, and Asians, but not in African Americans. Conditional analyses revealed that SNP rs7704116 in intron 1 showed consistently strong association with SLE across Asian, European American, and Hispanic American populations (odds ratio 1.3 [95% confidence interval 1.14-1.31], meta-analysis P=3.8×10(-7)). In European Americans, the largest ethnic data set studied, the risk A allele of rs7704116 was associated with the presence of renal disease, anti-double-stranded DNA, and anti-RNP antibodies. PPP2CA expression was ∼2-fold higher in SLE patients carrying the rs7704116 AG genotype than those carrying the GG genotype (P=0.007).Our data provide the first evidence of an association between PPP2CA polymorphisms and elevated PP2Ac transcript levels in T cells, which implicates a new molecular pathway for SLE susceptibility in European Americans, Hispanic Americans, and Asians.

Published
2011

150. Identification of a systemic lupus erythematosus susceptibility locus at 11p13 between PDHX and CD44 in a multiethnic study

Author

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

Subjects
Male, Asian Continental Ancestry Group, American Native Continental Ancestry Group, Major Clinical Study, European Continental Ancestry Group, Hispanic, Genetic Susceptibility, Pyruvate Dehydrogenase Complex, Caucasian, Systemic Lupus Erythematosus, Chromosomes, Linkage Disequilibrium, Article, Cohort Studies, Cd44V Antigen, Enfermedades autoinmunes, Lupus Eritomatoso Sistémico, Humans, Chromosome 11P, Controlled Study, Pair 11, Antigens, Polymorphism, African American, African Americans, Enfermedades de la piel, Asian, Lupus Erythematosus, Meta Analysis, Systemic, Single Nucleotide, Genetic Predisposition To Disease, Gene Locus, Statistical Analysis, Haplotypes, Genetic Loci, American Indian, Priority Journal, Single Nucleotide Polymorphism, Female, Cd44, Hispanic Americans, Cohort Analysis, Genetic Association, Human
Abstract

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

Published
2011

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