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1. Comparative lifespan and healthspan of nonhuman primate species common to biomedical research

Author

Huber, Hillary F., Ainsworth, Hannah C., Quillen, Ellen E., Salmon, Adam, Ross, Corinna, Azhar, Adinda D., Bales, Karen, Basso, Michele A., Coleman, Kristine, Colman, Ricki, Darusman, Huda S., Hopkins, William, Hotchkiss, Charlotte E., Jorgensen, Matthew J., Kavanagh, Kylie, Li, Cun, Mattison, Julie A., Nathanielsz, Peter W., Saputro, Suryo, Scorpio, Diana G., Sosa, Paul-Michael, Vallender, Eric J., Wang, Yaomin, Zeiss, Caroline J., Shively, Carol A., and Cox, Laura A.

Published
2024
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2. Epigenetic MLH1 silencing concurs with mismatch repair deficiency in sporadic, naturally occurring colorectal cancer in rhesus macaques

Author

Deycmar, Simon, Johnson, Brendan J., Ray, Karina, Schaaf, George W., Ryan, Declan Patrick, Cullin, Cassandra, Dozier, Brandy L., Ferguson, Betsy, Bimber, Benjamin N., Olson, John D., Caudell, David L., Whitlow, Christopher T., Solingapuram Sai, Kiran Kumar, Romero, Emily C., Villinger, Francois J., Burgos, Armando G., Ainsworth, Hannah C., Miller, Lance D., Hawkins, Gregory A., Chou, Jeff W., Gomes, Bruno, Hettich, Michael, Ceppi, Maurizio, Charo, Jehad, and Cline, J. Mark

Published
2024
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3. APOL1 Kidney-Risk Variants Induce Mitochondrial Fission

Author

Ma, Lijun, Ainsworth, Hannah C, Snipes, James A, Murea, Mariana, Choi, Young A, Langefeld, Carl D, Parks, John S, Bharadwaj, Manish S, Chou, Jeff W, Hemal, Ashok K, Petrovic, Snezana, Craddock, Ann L, Cheng, Dongmei, Hawkins, Gregory A, Miller, Lance D, Hicks, Pamela J, Saleem, Moin A, Divers, Jasmin, Molina, Anthony JA, and Freedman, Barry I

Subjects
Biomedical and Clinical Sciences, Genetics, Kidney Disease, Biotechnology, Prevention, 2.1 Biological and endogenous factors, Aetiology, Renal and urogenital, African Americans, APOL1, chronic kidney disease, FSGS, mitochondria, Biomedical and clinical sciences, Health sciences
Abstract

IntroductionAPOL1 G1 and G2 nephropathy-risk variants cause mitochondrial dysfunction and contribute to kidney disease. Analyses were performed to determine the genetic regulation of APOL1 and elucidate potential mechanisms in APOL1-nephropathy.MethodsA global gene expression analysis was performed in human primary renal tubule cell lines derived from 50 African American individuals. Follow-up gene knock out, cell-based rescue, and microscopy experiments were performed.ResultsAPOL1 genotypes did not alter APOL1 expression levels in the global gene expression analysis. Expression quantitative trait locus (eQTL) analysis in polyinosinic-polycytidylic acid (poly IC)-stimulated renal tubule cells revealed that single nucleotide polymorphism (SNP) rs513349 adjacent to BAK1 was a trans eQTL for APOL1 and a cis eQTL for BAK1; APOL1 and BAK1 were co-expressed in cells. BAK1 knockout in a human podocyte cell line resulted in diminished APOL1 protein, supporting a pivotal effect for BAK1 on APOL1 expression. Because BAK1 is involved in mitochondrial dynamics, mitochondrial morphology was examined in primary renal tubule cells and HEK293 Tet-on cells of various APOL1 genotypes. Mitochondria in APOL1 wild-type (G0G0) tubule cells maintained elongated morphology when stimulated by low-dose poly IC, whereas those with G1G1, G2G2, and G1G2 genotypes appeared to fragment. HEK293 Tet-on cells overexpressing APOL1 G0, G1, and G2 were created; G0 cells appeared to promote mitochondrial fusion, whereas G1 and G2 induced mitochondrial fission. The mitochondrial dynamic regulator Mdivi-1 significantly preserved cell viability and mitochondrial cristae structure and reversed mitochondrial fission induced by overexpression of G1 and G2.ConclusionResults suggest the mitochondrial fusion/fission pathway may be a therapeutic target in APOL1-nephropathy.

Published
2020

4. Curating Genetic Associations With Rheumatologic Autoimmune Diseases to Improve Patient Outcomes.

Author

Bridges, S. Louis, Shapira, Rachel, Aksentijevich, Ivona, Mack, Steven J., Merriman, Tony R., Klein, Clarissa J., Bowen, B. Monica, Klein, Teri E., Ainsworth, Hannah C., Langefeld, Carl D., de Jesus, Adriana A., Deuitch, Natalie T., Ombrello, Michael J., Fernandez‐Ruiz, Ruth, Fernández‐Viña, Marcelo, Keseler, Ingrid M., Wright, Matt W., Lakhanpal, Amit, Laufer, Vincent A., and Varga, John

Subjects
RHEUMATISM diagnosis, GENETICS of autoimmune diseases, PROTEINS, TREATMENT effectiveness, CONSORTIA, GENETIC mutation, ACCURACY, RHEUMATISM, GENETICS, GENETIC testing, HLA-B27 antigen, PHENOTYPES, ALLELES, COMMITTEES, GROUP process, SYMPTOMS
Abstract

The article offers update on the curation of genetic associations with rheumatologic autoimmune diseases to improve patient outcomes. Topics discussed include monogenic autoimmune and/or autoinflammatory conditions, development of a framework for curation of HLA disease associations, development of a methodology for curation of complex, multigenic diseases, and curation of disease-associated somatic variants.

Published
2024
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6. Transancestral mapping and genetic load in systemic lupus erythematosus.

Author

Langefeld, Carl D, Ainsworth, Hannah C, Cunninghame Graham, Deborah S, Kelly, Jennifer A, Comeau, Mary E, Marion, Miranda C, Howard, Timothy D, Ramos, Paula S, Croker, Jennifer A, Morris, David L, Sandling, Johanna K, Almlöf, Jonas Carlsson, Acevedo-Vásquez, Eduardo M, Alarcón, 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 Rantapää, D'Alfonso, Sandra, Da Silva, Berta Martins, de la Rúa Figueroa, Iñigo, Doria, Andrea, Edberg, Jeffrey C, Endreffy, Emőke, Esquivel-Valerio, Jorge A, Fortin, Paul R, Freedman, Barry I, Frostegård, Johan, García, Mercedes A, de la Torre, Ignacio García, Gilkeson, Gary S, Gladman, Dafna D, Gunnarsson, Iva, Guthridge, Joel M, Huggins, Jennifer L, James, Judith A, Kallenberg, Cees GM, Kamen, Diane L, Karp, David R, Kaufman, Kenneth M, Kottyan, Leah C, Kovács, László, Laustrup, Helle, Lauwerys, Bernard R, Li, Quan-Zhen, Maradiaga-Ceceña, Marco A, Martín, Javier, McCune, Joseph M, McWilliams, David R, Merrill, Joan T, Miranda, Pedro, Moctezuma, José 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, José M, Aguilar-Salinas, Carlos A, Scherbarth, Hugo R, Scorza, Raffaella, Seldin, Michael F, Sjöwall, Christopher, Svenungsson, Elisabet, Thompson, Susan D, Toloza, Sergio MA, Truedsson, Lennart, Tusié-Luna, Teresa, Vasconcelos, Carlos, Vilá, 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, and Behrens, Timothy W

Subjects
Humans, Lupus Erythematosus, Systemic, HLA Antigens, Logistic Models, Case-Control Studies, Mutagenesis, Insertional, Age of Onset, Sequence Deletion, Genetic Load, Multifactorial Inheritance, Polymorphism, Single Nucleotide, African Continental Ancestry Group, American Native Continental Ancestry Group, European Continental Ancestry Group, Hispanic Americans, Lupus Erythematosus, Systemic, Mutagenesis, Insertional, Polymorphism, Single Nucleotide
Abstract

Systemic lupus erythematosus (SLE) is an autoimmune disease with marked gender and ethnic disparities. We report a large transancestral association study of SLE using Immunochip genotype data from 27,574 individuals of European (EA), African (AA) and Hispanic Amerindian (HA) ancestry. We identify 58 distinct non-HLA regions in EA, 9 in AA and 16 in HA (∼50% of these regions have multiple independent associations); these include 24 novel SLE regions (P

Published
2017

7. Genetic and Clinical Predictors of Age of ESKD in Individuals With Autosomal Dominant Tubulointerstitial Kidney Disease Due to UMOD Mutations

Author

Kidd, Kendrah, Vylet’al, Petr, Schaeffer, Céline, Olinger, Eric, Živná, Martina, Hodaňová, Kateřina, Robins, Victoria, Johnson, Emily, Taylor, Abbigail, Martin, Lauren, Izzi, Claudia, Jorge, Sofia C., Calado, Joaquim, Torres, Rosa J., Lhotta, Karl, Steubl, Dominik, Gale, Daniel P., Gast, Christine, Gombos, Eva, Ainsworth, Hannah C., Chen, Ying Maggie, Almeida, Jorge Reis, de Souza, Cintia Fernandes, Silveira, Catarina, Raposeiro, Rita, Weller, Nelson, Conlon, Peter J., Murray, Susan L., Benson, Katherine A., Cavalleri, Gianpiero L., Votruba, Miroslav, Vrbacká, Alena, Amoroso, Antonio, Gianchino, Daniela, Caridi, Gianluca, Ghiggeri, Gian Marco, Divers, Jasmin, Scolari, Francesco, Devuyst, Olivier, Rampoldi, Luca, Kmoch, Stanislav, and Bleyer, Anthony J.

Published
2020
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9. Comparison of different gene addition strategies to modify placental derived-mesenchymal stromal cells to produce FVIII

Author

Ramamurthy, Ritu M., primary, Rodriguez, Martin, additional, Ainsworth, Hannah C., additional, Shields, Jordan, additional, Meares, Diane, additional, Bishop, Colin, additional, Farland, Andrew, additional, Langefeld, Carl D., additional, Atala, Anthony, additional, Doering, Christopher B., additional, Spencer, H. Trent, additional, Porada, Christopher D., additional, and Almeida-Porada, Graça, additional

Published
2022
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11. Brief Report: Association of Natural Killer Cell Ligand Polymorphism HLA–C Asn80Lys With the Development of Anti‐SSA/Ro–Associated Congenital Heart Block

Author

Ainsworth, Hannah C., Marion, Miranda C., Bertero, Tiziana, Brucato, Antonio, Cimaz, Rolando, Costedoat‐Chalumeau, Nathalie, Fredi, Micaela, Gaffney, Patrick, Kelly, Jennifer, Levesque, Kateri, Maltret, Alice, Morel, Nathalie, Ramoni, Veronique, Ruffatti, Amelia, Langefeld, Carl D., Buyon, Jill P., and Clancy, Robert M.

Published
2017
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13. 140-OR: Machine Learning for Metabolite Estimation to Examine Contributors to Glucose Homeostasis and Adiposity: The GUARDIAN Consortium

Author

ALLRED, NICHOLETTE, primary, AINSWORTH, HANNAH C., additional, GUO, XIUQING, additional, MACKAY, ADRIENNE W., additional, NYASIMI, FESTUS, additional, MELIA, OWEN, additional, LIANG, YANYU, additional, BOWDEN, DONALD W., additional, TAYLOR, KENT, additional, RAFFEL, LESLIE J., additional, BUCHANAN, THOMAS A., additional, WATANABE, RICHARD M., additional, ROTTER, JEROME I., additional, WAGENKNECHT, LYNNE E., additional, LANGEFELD, CARL D., additional, and IM, HAE K., additional

Published
2022
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15. Genome-Wide Association Study in an Amerindian Ancestry Population Reveals Novel Systemic Lupus Erythematosus Risk Loci and the Role of European Admixture

Author

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

Published
2016
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16. Nucleic Acid-Sensing and Interferon-Inducible Pathways Show Differential Methylation in MZ Twins Discordant for Lupus and Overexpression in Independent Lupus Samples: Implications for Pathogenic Mechanism and Drug Targeting

Author

Marion, Miranda C., primary, Ramos, Paula S., additional, Bachali, Prathyusha, additional, Labonte, Adam C., additional, Zimmerman, Kip D., additional, Ainsworth, Hannah C., additional, Heuer, Sarah E., additional, Robl, Robert D., additional, Catalina, Michelle D., additional, Kelly, Jennifer A., additional, Howard, Timothy D., additional, Lipsky, Peter E., additional, Grammer, Amrie C., additional, and Langefeld, Carl D., additional

Published
2021
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17. Additional file 1 of Single-cell expression quantitative trait loci (eQTL) analysis of SLE-risk loci in lupus patient monocytes

Author

Ghodke-Puranik, Yogita, Jin, Zhongbo, Zimmerman, Kip D., Ainsworth, Hannah C., Fan, Wei, Jensen, Mark A., Dorschner, Jessica M., Vsetecka, Danielle M., Amin, Shreyasee, Makol, Ashima, Ernste, Floranne, Osborn, Thomas, Moder, Kevin, Chowdhary, Vaidehi, Langefeld, Carl D., and Niewold, Timothy B.

Abstract

Additional file 1: Supplemental Figure 1. Scatter plots of purified classical and non-classical monocytes. PBMCs = peripheral blood mononuclear cells, percentages in the gates for classical and non-classical monocytes indicate the purity of populations purified. Supplemental Figure 2. Quantile ��� quantile plot showing eQTL associations with SLE risk loci. A) Classical monocytes; B) Non-classical monocytes. A very early deviation of the observed from the expected P value for eQTL associations suggested high type I error, which we found to relate to within-person correlations and distributional properties of the single cell data as described in the paper. eQTL associations that remained significant after using the approaches described in the Methods to correct for the distributional properties of the data are highlighted in orange for classical and magenta for non-classical monocytes. Supplemental Figure 3. On/off pattern of IRF1 gene expression in monocytes from a single cell RNA sequencing study examining patients with multiple myeloma. X-axis shows individual patients and the Y-axis shows gene expression values for the IRF1 transcript. Each plotted dot represents the expression level for IRF1 in one cell. Bars show the median, error bars show the interquartile range. Data from public database as reported in Haradhvala, N.J., et al., Cancer Research, 2019.

Published
2021
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18. Plasma Mucin-1 (CA15-3) Levels in Autosomal Dominant Tubulointerstitial Kidney Disease due to MUC1 Mutations

Author

Vylet’al, Petr, primary, Kidd, Kendrah, additional, Ainsworth, Hannah C., additional, Springer, Drahomíra, additional, Vrbacká, Alena, additional, Přistoupilová, Anna, additional, Hughey, Rebecca P., additional, Alper, Seth L., additional, Lennon, Niall, additional, Harrison, Steven, additional, Harden, Maegan, additional, Robins, Victoria, additional, Taylor, Abbigail, additional, Martin, Lauren, additional, Howard, Katrice, additional, Bitar, Ibrahim, additional, Langefeld, Carl D., additional, Barešová, Veronika, additional, Hartmannová, Hana, additional, Hodaňová, Kateřina, additional, Zima, Tomáš, additional, Živná, Martina, additional, Kmoch, Stanislav, additional, and Bleyer, Anthony J., additional

Published
2021
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22. Plasma Mucin-1 (CA15-3) Levels in Autosomal Dominant Tubulointerstitial Kidney Disease due to MUC1 Mutations.

Author

Vylet'al, Petr, Kidd, Kendrah, Ainsworth, Hannah C., Springer, Drahomíra, Vrbacká, Alena, Přistoupilová, Anna, Hughey, Rebecca P., Alper, Seth L., Lennon, Niall, Harrison, Steven, Harden, Maegan, Robins, Victoria, Taylor, Abbigail, Martin, Lauren, Howard, Katrice, Bitar, Ibrahim, Langefeld, Carl D., Barešová, Veronika, Hartmannová, Hana, and Hodaňová, Kateřina

Subjects
KIDNEY diseases, BREAST cancer, GLOMERULAR filtration rate, CIRCULATING tumor DNA, GENDER, PEDIATRIC nephrology
Abstract

Introduction: Patients with ADTKD-MUC1 have one allele producing normal mucin-1 (MUC1) and one allele producing mutant MUC1, which remains intracellular. We hypothesized that ADTKD-MUC1 patients, who have only 1 secretory-competent wild-type MUC1 allele, should exhibit decreased plasma mucin-1 (MUC1) levels. To test this hypothesis, we repurposed the serum CA15-3 assay used to measure MUC1 in breast cancer to measure plasma MUC1 levels in ADTKD-MUC1.Methods: This cross-sectional study analyzed CA15-3 levels in a reference population of 6,850 individuals, in 85 individuals with ADTKD-MUC1, and in a control population including 135 individuals with ADTKD-UMOD and 114 healthy individuals.Results: Plasma CA15-3 levels (mean ± standard deviation) were 8.6 ± 4.3 U/mL in individuals with ADTKD-MUC1 and 14.6 ± 5.6 U/mL in controls (p < 0.001). While there was a significant difference in mean CA15-3 levels, there was substantial overlap between the 2 groups. Plasma CA15-3 levels were <5 U/mL in 22% of ADTKD-MUC1 patients, in 0/249 controls, and in 1% of the reference population. Plasma CA15-3 levels were >20 U/mL in 1/85 ADTKD-MUC1 patients, in 18% of control individuals, and in 25% of the reference population. Segregation of plasma CA15-3 levels by the rs4072037 genotype did not significantly improve differentiation between affected and unaffected individuals. CA15-3 levels were minimally affected by gender and estimated glomerular filtration rate.Discussion/conclusions: Plasma CA15-3 levels in ADTKD-MUC1 patients are approximately 40% lower than levels in healthy individuals, though there is significant overlap between groups. Further investigations need to be performed to see if plasma CA15-3 levels would be useful in diagnosis, prognosis, or assessing response to new therapies in this disorder. [ABSTRACT FROM AUTHOR]

Published
2021
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23. The genetic profile of RF-positive polyarticular juvenile idiopathic arthritis (JIA) resembles adult rheumatoid arthritis (RA)

Author

Hinks, Anne, Marion, Miranda C., Cobb, Joanna, Comeau, Mary E., Sudman, Marc, Ainsworth, Hannah C, Bowes, John, Becker, Mara L, Bohnsack, John F., Haas, Johannes-Peter, Lovell, Daniel J, Mellins, Elizabeth D, Nelson, J. Lee, Nordal, Ellen, Punaro, Marilynn, Reed, Ann M., Rosé, Carlos D., Rosenberg, Alan M, Rygg, Marite, Smith, Samantha L, Stevens, Anne M, Videm, Vibeke, Wallace, Carol A., Wedderburn, Lucy R, Yarwood, Annie, Yeung, Rae S M, Langefeld, Carl D., Thompson, Susan D., Thomson, Wendy, and Prahalad, Sampath

Subjects
musculoskeletal diseases, genetic structures, immune system diseases, skin and connective tissue diseases, eye diseases
Abstract

Objective: Juvenile idiopathic arthritis (JIA) is comprised of seven heterogeneous categories of chronic childhood arthritides. About 5% of children with JIA have rheumatoid factor (RF) positive arthritis, which phenotypically resembles adult rheumatoid arthritis (RA). Our objective was to compare and contrast the genetics of RF-positive polyarticular JIA with RA, and selected other JIA categories, to more fully understand the pathophysiological relationships of inflammatory arthropathies. Methods: RF-positive polyarticular JIA cases (n=340) and controls (n=14,412) were genotyped using the Immunochip array. Single nucleotide polymorphisms (SNPs) were tested for association using a logistic regression model adjusting for admixture proportions. Weighted genetic risk scores (wGRS) of published RA and JIA risk loci were calculated and their ability to predict RF-positive polyarticular JIA were compared. Results: As expected, the HLA region was strongly associated with RF-positive polyarticular JIA (p=5.51x10-31). Nineteen of 44 RA risk loci and 6 of 27 oligoarticular/RF-negative polyarticular JIA risk loci were associated (p70 years. Conclusions: RF-positive polyarticular JIA is genetically more similar to adult RA than to the most common JIA categories and thus appears to be a childhood-onset presentation of autoantibody positive RA. These findings suggest common disease mechanisms, which could lead to novel therapeutic targets and shared treatment strategies.

Published
2018
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24. Brief Report: The Genetic Profile of Rheumatoid Factor-Positive Polyarticular Juvenile Idiopathic Arthritis Resembles That of Adult Rheumatoid Arthritis

Author

Hinks, Anne, Marion, Miranda C., Cobb, Joanna, Comeau, Mary E., Sudman, Marc, Ainsworth, Hannah C., Bowes, John, Becker, Mara L., Bohnsack, John F., Haas, Johannes-Peter, Lovell, Daniel J., Mellins, Elizabeth D., Nelson, J. Lee, Nordal, Ellen Berit, Punaro, Marilynn, Reed, Ann M., Rose, Carlos D., Rosenberg, Alan M., Rygg, Marite, Smith, Samantha L., Stevens, Anne M., Videm, Vibeke, Wallace, Carol A., Wedderburn, Lucy R., Yarwood, Annie, Yeung, Rae S.M., Langefeld, Carl D., Thompson, Susan D., Thomson, Wendy, and Prahalad, Sampath

Subjects
musculoskeletal diseases, Adult, Male, genetic structures, Adolescent, Genotype, VDP::Medical disciplines: 700::Clinical medical disciplines: 750::Rheumatology: 759, Genetic Profile, Polymorphism, Single Nucleotide, Arthritis, Juvenile, VDP::Medisinske Fag: 700::Klinisk medisinske fag: 750::Reumatologi: 759, Arthritis, Rheumatoid, Logistic Models, Phenotype, immune system diseases, Rheumatoid Factor, Humans, Female, skin and connective tissue diseases, Child, Autoantibodies
Abstract

This is the peer reviewed version of the following article: Hinks, A., Marion, M.C., Cobb, J., Comeau, M.E., Sudman, M., Ainsworth, H.C., ... Prahalad, S. (2018). Brief Report: The Genetic Profile of Rheumatoid Factor? Positive Polyarticular Juvenile Idiopathic Arthritis Resembles That of Adult Rheumatoid Arthritis. Arthritis & Rheumatology, 70(6), 957-962, which has been published in final form at https://doi.org/10.1002/art.40443. This article may be used for non-commercial purposes in accordance with Wiley Terms and Conditions for Use of Self-Archived Versions. Objective: Juvenile idiopathic arthritis (JIA) comprises 7 heterogeneous categories of chronic childhood arthritides. Approximately 5% of children with JIA have rheumatoid factor (RF)–positive arthritis, which phenotypically resembles adult rheumatoid arthritis (RA). Our objective was to compare and contrast the genetics of RF‐positive polyarticular JIA with those of RA and selected other JIA categories, to more fully understand the pathophysiologic relationships of inflammatory arthropathies. Methods: Patients with RF‐positive polyarticular JIA (n = 340) and controls (n = 14,412) were genotyped using the Immunochip array. Single‐nucleotide polymorphisms were tested for association using a logistic regression model adjusting for admixture proportions. We calculated weighted genetic risk scores (wGRS) of reported RA and JIA risk loci, and we compared the ability of these wGRS to predict RF‐positive polyarticular JIA. Results: As expected, the HLA region was strongly associated with RF‐positive polyarticular JIA (P = 5.51 × 10−31). Nineteen of 44 RA risk loci and 6 of 27 oligoarticular/RF‐negative polyarticular JIA risk loci were associated with RF‐positive polyarticular JIA (P < 0.05). The RA wGRS predicted RF‐positive polyarticular JIA (area under the curve [AUC] 0.71) better than did the oligoarticular/RF‐negative polyarticular JIA wGRS (AUC 0.59). The genetic profile of patients with RF‐positive polyarticular JIA was more similar to that of RA patients with age at onset 16–29 years than to that of RA patients with age at onset ≥70 years. Conclusion: RF‐positive polyarticular JIA is genetically more similar to adult RA than to the most common JIA categories and thus appears to be a childhood‐onset presentation of autoantibody‐positive RA. These findings suggest common disease mechanisms, which could lead to novel therapeutic targets and shared treatment strategies.

Published
2017

26. BD-01 E-genes identified via transancestral SNP mapping and gene expression analysis reveal novel targeted therapies for african-american and european-american SLE patients

Author

Owen, Katherine A, primary, Aidukaitis, Bryce N, additional, Labonte, Adam C, additional, Catalina, Michelle D, additional, Bachali, Prathyusha, additional, Dittman, James, additional, Geraci, Nicholas, additional, Rouffa, Sean, additional, Ainsworth, Hannah C, additional, Marion, Miranda C, additional, Howard, Timothy D, additional, Langefeld, Carl D, additional, Lipsky, Peter E, additional, and Grammer, Amrie C, additional

Published
2018
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27. Novel targeted therapies for African-American and European-American SLE patients identified from E-Genes elucidated by transancestral SNP mapping

Author

Aidukaitis, Bryce N., primary, Labonte, Adam C., additional, Catalina, Michelle D., additional, Bachali, Prathyusha, additional, Rouffa, Sean, additional, Ainsworth, Hannah C., additional, Marion, Miranda C., additional, Howard, Timothy D., additional, Langefeld, Carl D., additional, Lipsky, Peter E., additional, and Grammer, Amrie C., additional

Published
2018
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28. 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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29. Allele-specific methylation in the FADS genomic region in DNA from human saliva, CD4+ cells, and total leukocytes

Author

Biomedical Engineering and Mechanics, Rahbar, Elaheh, Waits, Charlotte M. K., Kirby, Edward H., Miller, Leslie R., Ainsworth, Hannah C., Cui, Tao, Sergeant, Susan, Howard, Timothy D., Langefeld, Carl D., Chilton, Floyd H., Biomedical Engineering and Mechanics, Rahbar, Elaheh, Waits, Charlotte M. K., Kirby, Edward H., Miller, Leslie R., Ainsworth, Hannah C., Cui, Tao, Sergeant, Susan, Howard, Timothy D., Langefeld, Carl D., and Chilton, Floyd H.

Abstract

Background Genetic variants within the fatty acid desaturase (FADS) gene cluster (human Chr11) are important regulators of long-chain (LC) polyunsaturated fatty acid (PUFA) biosynthesis in the liver and consequently have been associated with circulating LC-PUFA levels. More recently, epigenetic modifications such as DNA methylation, particularly within the FADS cluster, have been shown to affect LC-PUFA levels. Our lab previously demonstrated strong associations of allele-specific methylation (ASM) between a single nucleotide polymorphism (SNP) rs174537 and CpG sites across the FADS region in human liver tissues. Given that epigenetic signatures are tissue-specific, we aimed to evaluate the methylation status and ASM associations between rs174537 and DNA methylation obtained from human saliva, CD4+ cells and total leukocytes derived from whole blood. The goals were to (1) determine if DNA methylation from these peripheral samples would display similar ASM trends as previously observed in human liver tissues and (2) evaluate the associations between DNA methylation and circulating LC-PUFAs. Results DNA methylation at six CpG sites spanning FADS1 and FADS2 promoter regions and a putative FADS enhancer region were determined in two Caucasian cohorts of healthy volunteers: leukocytes in cohort 1 (n = 89, median age = 43, 35% male) and saliva and CD4+ cells in cohort 2 (n = 32, median age = 41, 41% male). Significant ASM between rs174537 and DNA methylation at three CpG sites located in the FADS2 promoter region (i.e., chr11:61594865, chr11:61594876, chr11:61594907) and one CpG site in the putative enhancer region (chr11:61587979) were observed with leukocytes. In CD4+ cells, significant ASM was observed at CpG sites chr11:61594876 and chr11:61584894. Genotype at rs174537 was significantly associated with DNA methylation from leukocytes. Similar trends were observed with CD4+ cells, but not with saliva. DNA methylation from leukocytes and CD4+ cells also significantly co

Published
2018

31. GWAS in an Amerindian ancestry population reveals novel systemic lupus erythematosus risk loci and the role of European admixture

Author

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

Subjects
Male, Argentina, Article, White People, HLA-DQ Antigens, Peru, Odds Ratio, HLA-DQ beta-Chains, Humans, Lupus Erythematosus, Systemic, Genetic Predisposition to Disease, Chile, Mexico, American Indian or Alaska Native, Principal Component Analysis, CD11b Antigen, Chromosomes, Human, Pair 10, NADPH Oxidases, Mitochondrial Proton-Translocating ATPases, STAT4 Transcription Factor, beta Karyopherins, United States, DNA-Binding Proteins, Interleukin-1 Receptor-Associated Kinases, Haplotypes, Case-Control Studies, Interferon Regulatory Factors, Female, Genome-Wide Association Study
Abstract

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

Published
2016

32. Uncovering the DNA methylation landscape in key regulatory regions within the FADS cluster

Author

Rahbar, Elaheh, primary, Ainsworth, Hannah C., additional, Howard, Timothy D., additional, Hawkins, Gregory A., additional, Ruczinski, Ingo, additional, Mathias, Rasika, additional, Seeds, Michael C., additional, Sergeant, Susan, additional, Hixson, James E., additional, Herrington, David M., additional, Langefeld, Carl D., additional, and Chilton, Floyd H., additional

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

Author

UCL - SSS/IREC/RUMA - Pôle de Pathologies rhumatismales, UCL - (SLuc) Service de rhumatologie, 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., Almlöf, Jonas Carlsson, Acevedo-Vásquez, Eduardo M., Alarcón, 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 Rantapää, D’Alfonso, Sandra, Da Silva, Berta Martins, de la Rúa Figueroa, Iñigo, Doria, Andrea, Edberg, Jeffrey C., Endreffy, Emőke, Esquivel-Valerio, Jorge A., Fortin, Paul R., Freedman, Barry I., Frostegård, Johan, García, Mercedes A., de la Torre, Ignacio García, 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., Kovács, László, Laustrup, Helle, Lauwerys, Bernard, Li, Quan-Zhen, Maradiaga-Ceceña, Marco A., Martín, Javier, McCune, Joseph M., McWilliams, David R., Merrill, Joan T., Miranda, Pedro, Moctezuma, José 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, José M., Aguilar-Salinas, Carlos A., Scherbarth, Hugo R., Scorza, Raffaella, Seldin, Michael F., Sjöwall, Christopher, Svenungsson, Elisabet, Thompson, Susan D., Toloza, Sergio M. A., Truedsson, Lennart, Tusié-Luna, Teresa, Vasconcelos, Carlos, Vilá, 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., UCL - SSS/IREC/RUMA - Pôle de Pathologies rhumatismales, UCL - (SLuc) Service de rhumatologie, 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., Almlöf, Jonas Carlsson, Acevedo-Vásquez, Eduardo M., Alarcón, 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 Rantapää, D’Alfonso, Sandra, Da Silva, Berta Martins, de la Rúa Figueroa, Iñigo, Doria, Andrea, Edberg, Jeffrey C., Endreffy, Emőke, Esquivel-Valerio, Jorge A., Fortin, Paul R., Freedman, Barry I., Frostegård, Johan, García, Mercedes A., de la Torre, Ignacio García, 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., Kovács, László, Laustrup, Helle, Lauwerys, Bernard, Li, Quan-Zhen, Maradiaga-Ceceña, Marco A., Martín, Javier, McCune, Joseph M., McWilliams, David R., Merrill, Joan T., Miranda, Pedro, Moctezuma, José 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, José M., Aguilar-Salinas, Carlos A., Scherbarth, Hugo R., Scorza, Raffaella, Seldin, Michael F., Sjöwall, Christopher, Svenungsson, Elisabet, Thompson, Susan D., Toloza, Sergio M. A., Truedsson, Lennart, Tusié-Luna, Teresa, Vasconcelos, Carlos, Vilá, 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., and Silverman, Earl D.

Abstract

Systemic lupus erythematosus (SLE) is an autoimmune disease with marked gender and ethnic disparities. We report a large transancestral association study of SLE using Immunochip genotype data from 27,574 individuals of European (EA), African (AA) and Hispanic Amerindian (HA) ancestry. We identify 58 distinct non-HLA regions in EA, 9 in AA and 16 in HA (∼50% of these regions have multiple independent associations); these include 24 novel SLE regions (P<5 × 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

36. Genome-wide imputation study identifies novel HLA locus for pulmonary fibrosis and potential role for auto-immunity in fibrotic idiopathic interstitial pneumonia

Author

Fingerlin, Tasha E., primary, Zhang, Weiming, additional, Yang, Ivana V., additional, Ainsworth, Hannah C., additional, Russell, Pamela H., additional, Blumhagen, Rachel Z., additional, Schwarz, Marvin I., additional, Brown, Kevin K., additional, Steele, Mark P., additional, Loyd, James E., additional, Cosgrove, Gregory P., additional, Lynch, David A., additional, Groshong, Steve, additional, Collard, Harold R., additional, Wolters, Paul J., additional, Bradford, Williamson Z., additional, Kossen, Karl, additional, Seiwert, Scott D., additional, du Bois, Roland M., additional, Garcia, Christine Kim, additional, Devine, Megan S., additional, Gudmundsson, Gunnar, additional, Isaksson, Helgi J., additional, Kaminski, Naftali, additional, Zhang, Yingze, additional, Gibson, Kevin F., additional, Lancaster, Lisa H., additional, Maher, Toby M., additional, Molyneaux, Philip L., additional, Wells, Athol U., additional, Moffatt, Miriam F., additional, Selman, Moises, additional, Pardo, Annie, additional, Kim, Dong Soon, additional, Crapo, James D., additional, Make, Barry J., additional, Regan, Elizabeth A., additional, Walek, Dinesha S., additional, Daniel, Jerry J., additional, Kamatani, Yoichiro, additional, Zelenika, Diana, additional, Murphy, Elissa, additional, Smith, Keith, additional, McKean, David, additional, Pedersen, Brent S., additional, Talbert, Janet, additional, Powers, Julia, additional, Markin, Cheryl R., additional, Beckman, Kenneth B., additional, Lathrop, Mark, additional, Freed, Brian, additional, Langefeld, Carl D., additional, and Schwartz, David A., additional

Published
2016
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37. Brief Report: The Genetic Profile of Rheumatoid Factor–Positive Polyarticular Juvenile Idiopathic Arthritis Resembles That of Adult Rheumatoid Arthritis.

Author

Hinks, Anne, Marion, Miranda C., Cobb, Joanna, Comeau, Mary E., Sudman, Marc, Ainsworth, Hannah C., Bowes, John, Juvenile Idiopathic Arthritis Consortium for Immunochip, Becker, Mara L., Bohnsack, John F., Haas, Johannes‐Peter, Lovell, Daniel J., Mellins, Elizabeth D., Nelson, J. Lee, Nordal, Ellen, Punaro, Marilynn, Reed, Ann M., Rose, Carlos D., Rosenberg, Alan M., and Rygg, Marite

Subjects
GENETICS of rheumatoid arthritis, AGE factors in disease, GENETIC polymorphisms, PROBABILITY theory, RHEUMATOID arthritis, BIOCHIPS, JUVENILE idiopathic arthritis, LOGISTIC regression analysis, OLIGONUCLEOTIDE arrays, GENOTYPES, GENETICS
Abstract

Objective: Juvenile idiopathic arthritis (JIA) comprises 7 heterogeneous categories of chronic childhood arthritides. Approximately 5% of children with JIA have rheumatoid factor (RF)–positive arthritis, which phenotypically resembles adult rheumatoid arthritis (RA). Our objective was to compare and contrast the genetics of RF‐positive polyarticular JIA with those of RA and selected other JIA categories, to more fully understand the pathophysiologic relationships of inflammatory arthropathies. Methods: Patients with RF‐positive polyarticular JIA (n = 340) and controls (n = 14,412) were genotyped using the Immunochip array. Single‐nucleotide polymorphisms were tested for association using a logistic regression model adjusting for admixture proportions. We calculated weighted genetic risk scores (wGRS) of reported RA and JIA risk loci, and we compared the ability of these wGRS to predict RF‐positive polyarticular JIA. Results: As expected, the HLA region was strongly associated with RF‐positive polyarticular JIA (P = 5.51 × 10−31). Nineteen of 44 RA risk loci and 6 of 27 oligoarticular/RF‐negative polyarticular JIA risk loci were associated with RF‐positive polyarticular JIA (P < 0.05). The RA wGRS predicted RF‐positive polyarticular JIA (area under the curve [AUC] 0.71) better than did the oligoarticular/RF‐negative polyarticular JIA wGRS (AUC 0.59). The genetic profile of patients with RF‐positive polyarticular JIA was more similar to that of RA patients with age at onset 16–29 years than to that of RA patients with age at onset ≥70 years. Conclusion: RF‐positive polyarticular JIA is genetically more similar to adult RA than to the most common JIA categories and thus appears to be a childhood‐onset presentation of autoantibody‐positive RA. These findings suggest common disease mechanisms, which could lead to novel therapeutic targets and shared treatment strategies. [ABSTRACT FROM AUTHOR]

Published
2018
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38. Association of Natural Killer Cell Ligand Polymorphism HLA-C Asn80Lys With the Development of Anti- SSA/Ro-Associated Congenital Heart Block.

Author

Ainsworth, Hannah C., Marion, Miranda C., Bertero, Tiziana, Brucato, Antonio, Cimaz, Rolando, Costedoat‐Chalumeau, Nathalie, Fredi, Micaela, Gaffney, Patrick, Kelly, Jennifer, Levesque, Kateri, Maltret, Alice, Morel, Nathalie, Ramoni, Veronique, Ruffatti, Amelia, Langefeld, Carl D., Buyon, Jill P., and Clancy, Robert M.

Subjects
*GENETICS of autoimmune diseases, *ALLELES, *AUTOIMMUNE diseases, *SIBLINGS, *CONGENITAL heart disease, *GENETIC polymorphisms, *HEART block, *PROBABILITY theory, *SEX distribution, *LOGISTIC regression analysis, *DATA analysis, *MICROARRAY technology, *ODDS ratio, *GENOTYPES, *FETUS, *GENETICS
Abstract

Objective Fetal exposure to maternal anti- SSA/Ro antibodies is necessary but not sufficient for the development of autoimmune congenital heart block ( CHB), suggesting that other factors, such as fetal genetic predisposition, are important. Given the previously described association between major histocompatibility complex alleles and CHB risk, we undertook the present study to test the hypothesis that a variant form of HLA-C Asn80Lys, which binds with high affinity to an inhibitory killer cell immunoglobulin-like receptor ( KIR) and thus renders natural killer ( NK) cells incapable of restricting inflammation, contributes to the development of CHB. Methods Members of 192 pedigrees in the US and Europe (194 cases of CHB, 91 unaffected siblings, 152 fathers, 167 mothers) and 1,073 out-of-study controls were genotyped on the Immunochip single-nucleotide polymorphism microarray. Imputation was used to identify associations at HLA-C Asn80Lys (Asn, C1; Lys, C2) and KIR. Tests for association were performed using logistic regression. McNemar's test and the pedigree disequilibrium test ( PDT) were used for matched analyses between affected and unaffected children. Results Compared with out-of-study controls of the same sex, the C2 allele was less frequent in the mothers (odds ratio [ OR] 0.63, P = 0.0014) and more frequent in the fathers ( OR 1.40, P = 0.0123), yielding a significant sex-by-C2 interaction ( P = 0.0002). The C2 allele was more frequent in affected siblings than in unaffected siblings ( OR 3.67, P = 0.0025), which was consistent with the PDT results ( P = 0.016); these results were observed in both sexes and across the US and European cohorts. There was no difference in the frequency of the inhibitory KIR genotype ( KIR AA) between affected and unaffected children ( P = 0.55). Conclusion These data establish C2 as a novel genetic risk factor associated with CHB. This observation supports a model in which fetuses with C2 ligand expression and maternal anti- SSA/Ro positivity may have impaired NK cell surveillance, resulting in unchecked cardiac inflammation and scarring. [ABSTRACT FROM AUTHOR]

Published
2017
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39. DNA Methylation in an Enhancer Region of the FADS Cluster Is Associated with FADS Activity in Human Liver

Author

Howard, Timothy D., primary, Mathias, Rasika A., additional, Seeds, Michael C., additional, Herrington, David M., additional, Hixson, James E., additional, Shimmin, Lawrence C., additional, Hawkins, Greg A., additional, Sellers, Matthew, additional, Ainsworth, Hannah C., additional, Sergeant, Susan, additional, Miller, Leslie R., additional, and Chilton, Floyd H., additional

Published
2014
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40. Adaptive Evolution of the FADS Gene Cluster within Africa

Author

Mathias, Rasika A., primary, Fu, Wenqing, additional, Akey, Joshua M., additional, Ainsworth, Hannah C., additional, Torgerson, Dara G., additional, Ruczinski, Ingo, additional, Sergeant, Susan, additional, Barnes, Kathleen C., additional, and Chilton, Floyd H., additional

Published
2012
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42. Differences in arachidonic acid levels and fatty acid desaturase (FADS) gene variants in African Americans and European Americans with diabetes or the metabolic syndrome

Author

Sergeant, Susan, primary, Hugenschmidt, Christina E., additional, Rudock, Megan E., additional, Ziegler, Julie T., additional, Ivester, Priscilla, additional, Ainsworth, Hannah C., additional, Vaidya, Dhananjay, additional, Douglas Case, L., additional, Langefeld, Carl D., additional, Freedman, Barry I., additional, Bowden, Donald W., additional, Mathias, Rasika A., additional, and Chilton, Floyd H., additional

Published
2011
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43. Differences in arachidonic acid levels and fatty acid desaturase (FADS) gene variants in African Americans and European Americans with diabetes or the metabolic syndrome.

Author

Sergeant, Susan, Hugenschmidt, Christina E., Rudock, Megan E., Ziegler, Julie T., Ivester, Priscilla, Ainsworth, Hannah C., Vaidya, Dhananjay, Douglas Case, L., Langefeld, Carl D., Freedman, Barry I., Bowden, Donald W., Mathias, Rasika A., and Chilton, Floyd H.

Subjects
ARACHIDONIC acid, FATTY acids, DIABETES, METABOLIC syndrome, AFRICAN Americans, EUROPEAN Americans
Abstract

Over the past 50 years, increases in dietary n-6 PUFA, such as linoleic acid, have been hypothesised to cause or exacerbate chronic inflammatory diseases. The present study examines an individual's innate capacity to synthesise n-6 long-chain PUFA (LC-PUFA) with respect to the fatty acid desaturase (FADS) locus in Americans of African and European descent with diabetes or the metabolic syndrome. Compared with European Americans (EAm), African Americans (AfAm) exhibited markedly higher serum levels of arachidonic acid (AA) (EAm 7·9 (sd 2·1), AfAm 9·8 (sd 1·9) % of total fatty acids; P < 2·29 × 10− 9) and the AA:n-6-precursor fatty acid ratio, which estimates FADS1 activity (EAm 5·4 (sd 2·2), AfAm 6·9 (sd 2·2); P = 1·44 × 10− 5). In all, seven SNP mapping to the FADS locus revealed strong association with AA, EPA and dihomo-γ-linolenic acid (DGLA) in the EAm. Importantly, EAm homozygous for the minor allele (T) had significantly lower AA levels (TT 6·3 (sd 1·0); GG 8·5 (sd 2·1); P = 3·0 × 10− 5) and AA:DGLA ratios (TT 3·4 (sd 0·8), GG 6·5 (sd 2·3); P = 2·2 × 10− 7) but higher DGLA levels (TT 1·9 (sd 0·4), GG 1·4 (sd 0·4); P = 3·3 × 10− 7) compared with those homozygous for the major allele (GG). Allele frequency patterns suggest that the GG genotype at rs174537 (associated with higher circulating levels of AA) is much higher in AfAm (0·81) compared with EAm (0·46). Similarly, marked differences in rs174537 genotypic frequencies were observed in HapMap populations. These data suggest that there are probably important differences in the capacity of different populations to synthesise LC-PUFA. These differences may provide a genetic mechanism contributing to health disparities between populations of African and European descent. [ABSTRACT FROM PUBLISHER]

Published
2012
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45. Comparative lifespan and healthspan of nonhuman primate species common to biomedical research.

Author

Huber HF, Ainsworth HC, Quillen EE, Salmon A, Ross C, Azhar AD, Bales K, Basso MA, Coleman K, Colman R, Darusman HS, Hopkins W, Hotchkiss CE, Jorgensen MJ, Kavanagh K, Li C, Mattison JA, Nathanielsz PW, Saputro S, Scorpio DG, Sosa PM, Vallender EJ, Wang Y, Zeiss CJ, Shively CA, and Cox LA

Abstract

There is a critical need to generate age- and sex-specific survival curves to characterize chronological aging consistently across nonhuman primates (NHP) used in biomedical research. Sex-specific Kaplan-Meier survival curves were computed in 12 translational aging models: baboon, bonnet macaque, chimpanzee, common marmoset, coppery titi monkey, cotton-top tamarin, cynomolgus macaque, Japanese macaque, pigtail macaque, rhesus macaque, squirrel monkey, and vervet/African green. After employing strict inclusion criteria, primary results are based on 12,269 NHP that survived to adulthood and died of natural/health-related causes. A secondary analysis was completed for 32,616 NHP that died of any cause. Results show a pattern of reduced male survival among catarrhines (African and Asian primates), especially macaques, but not platyrrhines (Central and South American primates). For many species, median lifespans were lower than previously reported. An important consideration is that these analyses may offer a better reflection of healthspan than lifespan since research NHP are typically euthanized for humane welfare reasons before their natural end of life. This resource represents the most comprehensive characterization of sex-specific lifespan and age-at-death distributions for 12 biomedically relevant species, to date. These results clarify relationships among NHP ages and provide a valuable resource for the aging research community, improving human-NHP age equivalencies, informing investigators of expected survival rates, providing a metric for comparisons in future studies, and contributing to understanding of factors driving lifespan differences within and among species., Competing Interests: Ethical Statement/Conflict of Interests The authors declare no competing interests.

Published
2024
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