Your search keyword '"Marion, Miranda C."' showing total 17 results

1. Platelet Glycoprotein Ib α‐Chain as a Putative Therapeutic Target for Juvenile Idiopathic Arthritis: A Mendelian Randomization Study.

Author

Luo, Shan, Clarke, Sarah L. N., Ramanan, Athimalaipet V., Thompson, Susan D., Langefeld, Carl D., Marion, Miranda C., Grom, Alexei A., Schooling, C. Mary, Gaunt, Tom R., Yeung, Shiu Lun Au, and Zheng, Jie

Subjects

CARDIOVASCULAR diseases risk factors, JUVENILE idiopathic arthritis, AUTOIMMUNE diseases, GLYCOPROTEINS, PLATELET count

Abstract

Objective: To ascertain the role of platelet glycoprotein Ib α‐chain (GPIbα) plasma protein levels in cardiovascular, autoimmune, and autoinflammatory diseases and whether its effects are mediated by platelet count. Methods: We performed a two‐sample Mendelian randomization (MR) study, using both a cis‐acting protein quantitative trait locus (cis‐pQTL) and trans‐pQTL near the GP1BA and BRAP genes as instruments. To assess if platelet count mediated the effect, we then performed a two‐step MR study. Putative associations (GPIbα/platelet count/disease) detected by MR analyses were subsequently assessed using multiple‐trait colocalization analyses. Results: After correction for multiple testing (Bonferroni‐corrected threshold P ≤ 2 × 10−3), GPIbα, instrumented by either cis‐pQTL or trans‐pQTL, was causally implicated with an increased risk of oligoarticular and rheumatoid factor (RF)–negative polyarticular juvenile idiopathic arthritis (JIA). These effects of GPIbα appeared to be mediated by platelet count and were supported by strong evidence of colocalization (probability of all 3 traits sharing a common causal variant ≥0.80). GPIbα instrumented by cis‐pQTL did not appear to affect cardiovascular risk, although the GPIbα trans‐pQTL was associated with an increased risk of cardiovascular diseases and autoimmune diseases but a decreased risk of autoinflammatory diseases, suggesting that this trans‐acting instrument operates through other pathways. Conclusion: The role of platelets in thrombosis is well‐established; however, our findings provide some novel genetic evidence that platelets may be causally implicated in the development of oligoarticular and RF‐negative polyarticular JIA, and indicate that GPIbα may serve as a putative therapeutic target for these JIA subtypes. [ABSTRACT FROM AUTHOR]

Published

2021

2. Association of SLCO1B1 *14 Allele with Poor Response to Methotrexate in Juvenile Idiopathic Arthritis Patients.

Author

Ramsey, Laura B., Moncrieffe, Halima, Smith, Chelsey N., Sudman, Marc, Marion, Miranda C., Langefeld, Carl D., Becker, Mara L., and Thompson, Susan D.

Abstract

Objective: Variants in the SLCO1B1 gene, encoding a hepatic methotrexate (MTX) transporter, affect clearance of high‐dose MTX. We tested whether in the *14 and *15 alleles of SLCO1B1 influenced the response to low‐dose MTX in juvenile idiopathic arthritis (JIA) patients. Methods: The study included 310 JIA patients genotyped for three single nucleotide polymorphisms (SNPs) in SLCO1B1 (rs4149056, rs2306283, and rs11045819). A patient's SLCO1B1 diplotype was determined by combining the SNPs into the *1a, *1b, *4, *5, *14, and *15 alleles. Number of active joints at follow‐up (visit closest to 6 months of treatment and prior to starting a tumor necrosis factor inhibitor) was used as the dependent variable in a negative binomial regression model that included active joint count at baseline as a covariate. Results: The SLCO1B1*14 allele was associated with less response to MTX (P = 0.024) and the *15 allele was not associated with response to MTX (P = 0.392). Conclusion: SLCO1B1 alleles may be associated with poor response to MTX in JIA patients. The *14 allele has been associated with fast clearance (low exposure) after high‐dose MTX in patients with leukemia. Thus, the SLCO1B1 gene may be informative for precision dosing of MTX in JIA patients. Patients carrying the *14 allele may require a higher dose than noncarriers to achieve a similar response to MTX. [ABSTRACT FROM AUTHOR]

Published

2019

3. 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

4. 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

5. Genome-Wide Association Meta-Analysis Reveals Novel Juvenile Idiopathic Arthritis Susceptibility Loci.

Author

McIntosh, Laura A., Marion, Miranda C., Sudman, Marc, Comeau, Mary E., Becker, Mara L., Bohnsack, John F., Fingerlin, Tasha E., Griffin, Thomas A., Haas, J. Peter, Lovell, Daniel J., Maier, Lisa A., Nigrovic, Peter A., Prahalad, Sampath, Punaro, Marilynn, Rosé, Carlos D., Wallace, Carol A., Wise, Carol A., Moncrieffe, Halima, Howard, Timothy D., and Langefeld, Carl D.

Subjects

*AUTOIMMUNE diseases, *DISEASE susceptibility, *GENE expression, *GENETIC polymorphisms, *HUMAN genome, *LONGITUDINAL method, *META-analysis, *PROBABILITY theory, *EVIDENCE-based medicine, *JUVENILE idiopathic arthritis, *MICROARRAY technology, *GENOTYPES, *GENETICS, *DISEASE risk factors

Abstract

Objective Juvenile idiopathic arthritis (JIA) is the most common childhood rheumatic disease and has a strong genomic component. To date, JIA genetic association studies have had limited sample sizes, used heterogeneous patient populations, or included only candidate regions. The aim of this study was to identify new associations between JIA patients with oligoarticular disease and those with IgM rheumatoid factor (RF)−negative polyarticular disease, which are clinically similar and the most prevalent JIA disease subtypes. Methods Three cohorts comprising 2,751 patients with oligoarticular or RF-negative polyarticular JIA were genotyped using the Affymetrix Genome-Wide SNP Array 6.0 or the Illumina HumanCoreExome-12+ Array. Overall, 15,886 local and out-of-study controls, typed on these platforms or the Illumina HumanOmni2.5, were used for association analyses. High-quality single-nucleotide polymorphisms (SNPs) were used for imputation to 1000 Genomes prior to SNP association analysis. Results Meta-analysis showed evidence of association ( P < 1 × 10−6) at 9 regions: PRR9_ LOR ( P = 5.12 × 10−8), ILDR1_ CD86 ( P = 6.73 × 10−8), WDFY4 ( P = 1.79 × 10−7), PTH1R ( P = 1.87 × 10−7), RNF215 ( P = 3.09 × 10−7), AHI1_ LINC00271 ( P = 3.48 × 10−7), JAK1 ( P = 4.18 × 10−7), LINC00951 ( P = 5.80 × 10−7), and HBP1 ( P = 7.29 × 10−7). Of these, PRR9_LOR, ILDR1_CD86, RNF215, LINC00951, and HBP1 were shown, for the first time, to be autoimmune disease susceptibility loci. Furthermore, associated SNPs included cis expression quantitative trait loci for WDFY4, CCDC12, MTP18, SF3A1, AHI1, COG5, HBP1, and GPR22. Conclusion This study provides evidence of both unique JIA risk loci and risk loci overlapping between JIA and other autoimmune diseases. These newly associated SNPs are shown to influence gene expression, and their bounding regions tie into molecular pathways of immunologic relevance. Thus, they likely represent regions that contribute to the pathology of oligoarticular JIA and RF-negative polyarticular JIA. [ABSTRACT FROM AUTHOR]

Published

2017

6. Enrichment of associations in genes with fibrosis, apoptosis, and innate immunity functions with cardiac manifestations of neonatal lupus.

Author

Ramos, Paula S., Marion, Miranda C., Langefeld, Carl D., Buyon, Jill P., and Clancy, Robert M.

Subjects

*APOPTOSIS, *CONFIDENCE intervals, *EPIDEMIOLOGY, *GENES, *IMMUNE system, *RESEARCH funding, *GENOMICS, *SYSTEMIC lupus erythematosus, *DATA analysis, *FIBROSIS, *EQUIPMENT & supplies, *CHILDREN, *GENETICS

Abstract

Objective The proposed pathogenesis of the cardiac manifestations of neonatal lupus (cardiac-NL) involves maternal autoantibodies to the RNPs SSA/Ro and SSB/La, enhanced by as-yet-unknown factors that likely involve dysregulation of both inflammatory and fibrotic fetal responses. This study was designed to improve the power to detect specific associations in genes with candidate biologic functions. Methods Using data from our genome-wide association study of 116 Caucasian children with cardiac-NL and 3,351 Caucasian controls, we tested for enrichment of single-nucleotide polymorphism (SNP) associations in genes with candidate biologic functions related to fibrosis, immune function, apoptosis, T cell function, cell infiltration, innate immune cell function, interferon, Toll-like receptors, and calcium channels. After linkage disequilibrium pruning and exclusion of the extended HLA region, a total of 15,103 SNPs in 3,068 genes remained. Results A highly significant enrichment of P values was observed for genes related to fibrosis ( P = 2.27 × 10−9), apoptosis ( P = 7.67 × 10−7), and innate immune cell ( P = 2.53 × 10−6), immune ( P = 5.01 × 10−4), T cell ( P = 2.23 × 10−4), and interferon functions ( P = 1.64 × 10−3). The most significant non-HLA associations included the sialyltransferase gene ST8SIA2 (rs1487982; odds ratio 2.20 [95% confidence interval 1.52-3.19], P = 3.37 × 10−5), the integrin gene ITGA1 (rs2432143; odds ratio 2.31 [95% confidence interval 1.54-3.45], P = 4.54 × 10−5), and the complement regulator gene CSMD1 (rs7002001; odds ratio 2.41 [95% confidence interval 1.57-3.72], P = 6.33 × 10−5). Conclusion This study identified novel candidate genes associated with cardiac-NL and highlights the value of studying this cohort for advancing knowledge regarding the genetic etiology of this syndrome. Identification of causal alleles is expected to provide critical insight into the molecular mechanisms responsible for linking maternal autoantibodies to cardiac scarring in these fetuses/neonates. [ABSTRACT FROM AUTHOR]

Published

2012

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

Author

Sánchez, Elena, Rasmussen, Astrid, Riba, Laura, Acevedo-Vasquez, Eduardo, Kelly, Jennifer A., Langefeld, Carl D., Williams, Adrianne H., Ziegler, Julie T., Comeau, Mary E., Marion, Miranda C., García-De La Torre, Ignacio, Maradiaga-Ceceña, Marco A., Cardiel, Mario H., Esquivel-Valerio, Jorge A., Rodriguez-Amado, Jacqueline, Moctezuma, José Francisco, Miranda, Pedro, Perandones, Carlos E., Castel, Cecilia, and Laborde, Hugo A.

Subjects

AGE distribution, CHI-squared test, CONFIDENCE intervals, EPIDEMIOLOGY, ETHNOLOGY, GENES, INDIGENOUS peoples of the Americas, REGRESSION analysis, RESEARCH funding, STATISTICS, SYSTEMIC lupus erythematosus, T-test (Statistics), LOGISTIC regression analysis, DATA analysis, SOCIOECONOMIC factors, DATA analysis software, SYMPTOMS, GENETICS

Abstract

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

Published

2012

8. Association of two independent functional risk haplotypes in TNIP1 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, and Kim, Jae-Hoon

Subjects

SYSTEMIC lupus erythematosus, CONFIDENCE intervals, EPIDEMIOLOGY, GENES, POLYMERASE chain reaction, RESEARCH funding, RISK assessment, STATISTICS, T-test (Statistics), WESTERN immunoblotting, LOGISTIC regression analysis, GENOMICS, DATA analysis, EQUIPMENT & supplies, CASE-control method, REVERSE transcriptase polymerase chain reaction, DATA analysis software, MICROARRAY technology, GENETICS

Abstract

Objective 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 identified >30 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. Methods 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. Results 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. Conclusion 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. [ABSTRACT FROM AUTHOR]

Published

2012

9. Genome-wide association analysis of juvenile idiopathic arthritis identifies a new susceptibility locus at chromosomal region 3q13.

Author

Thompson, Susan D., Marion, Miranda C., Sudman, Marc, Ryan, Mary, Tsoras, Monica, Howard, Timothy D., Barnes, Michael G., Ramos, Paula S., Thomson, Wendy, Hinks, Anne, Haas, Johannes-Peter, Prahalad, Sampath, Bohnsack, John F., Wise, Carol A., Punaro, Marilynn, Rosé, Carlos D., Pajewski, Nicholas M., Spigarelli, Michael, Keddache, Mehdi, and Wagner, Michael

Subjects

*ANALYSIS of variance, *CONFIDENCE intervals, *EPIDEMIOLOGY, *GENES, *GENETIC polymorphisms, *RESEARCH funding, *JUVENILE idiopathic arthritis, *GENOMICS, *DATA analysis, *EQUIPMENT & supplies, *CASE-control method

Abstract

Objective In a genome-wide association study of Caucasian patients with juvenile idiopathic arthritis (JIA), we have previously described findings limited to autoimmunity loci shared by JIA and other diseases. The present study was undertaken to identify novel JIA-predisposing loci using genome-wide approaches. Methods The discovery cohort consisted of Caucasian JIA cases (n = 814) and local controls (n = 658) genotyped on the Affymetrix Genome-Wide SNP 6.0 Array, along with 2,400 out-of-study controls. In a replication study, we genotyped 10 single-nucleotide polymorphisms (SNPs) in 1,744 cases and 7,010 controls from the US and Europe. Results Analysis within the discovery cohort provided evidence of associations at 3q13 within C3orf1 and near CD80 (rs4688011) (odds ratio [OR] 1.37, P = 1.88 × 10−6) and at 10q21 near JMJD1C (rs647989 [OR 1.59, P = 6.1 × 10−8], rs12411988 [OR 1.57, P = 1.16 × 10−7], and rs10995450 [OR 1.31, P = 6.74 × 10−5]). Meta-analysis provided further evidence of association for these 4 SNPs ( P = 3.6 × 10−7 for rs4688011, P = 4.33 × 10−5 for rs6479891, P = 2.71 × 10−5 for rs12411988, and P = 5.39 × 10−5 for rs10995450). Gene expression data on 68 JIA cases and 23 local controls showed cis expression quantitative trait locus associations for C3orf1 SNP rs4688011 ( P = 0.024 or P = 0.034, depending on the probe set) and JMJD1C SNPs rs6479891 and rs12411988 ( P = 0.01 or P = 0.04, depending on the probe set and P = 0.008, respectively). Using a variance component liability model, it was estimated that common SNP variation accounts for approximately one-third of JIA susceptibility. Conclusion Genetic association results and correlated gene expression findings provide evidence of JIA association at 3q13 and suggest novel genes as plausible candidates in disease pathology. [ABSTRACT FROM AUTHOR]

Published

2012

10. Preferential transmission of genetic risk variants of candidate loci at 6p21 from asymptomatic grandparents to mothers of children with neonatal lupus.

Author

Saxena, Amit, McDonnell, Erin, Ramos, Paula S., Sajuthi, Satria, Marion, Miranda C., Langefeld, Carl D., Buyon, Jill P., and Clancy, Robert M.

Subjects

SYSTEMIC lupus erythematosus, AUTOANTIBODIES, CHI-squared test, CONFIDENCE intervals, ENZYME-linked immunosorbent assay, EPIDEMIOLOGY, GENES, QUESTIONNAIRES, RESEARCH funding, RISK assessment, DATA analysis, DESCRIPTIVE statistics, GENETICS

Abstract

Objective Neonatal lupus (NL) occurs in fetuses exposed to maternal anti-SSA/Ro and/or anti-SSB/La antibodies, although the mothers themselves may not manifest any clinical disease. A focus on transmission of risk factors for NL from maternal grandparents to mothers of children with NL may yield dividends toward understanding the aggregation of autoantibodies and genetic factors in affected families. This study was perforned to determine the role of maternal grandparents in the development of the autoimmune phenotype of mothers of children with NL. Methods Fifty-one mothers of children with cardiac and/or cutaneous NL, 48 maternal grandmothers, and 35 maternal grandfathers in the Research Registry for Neonatal Lupus were interrogated for clinical symptoms by questionnaire and underwent laboratory assessments, including determination of anti-SSA/Ro and anti-SSB/La antibody status (by enzyme-linked immunosorbent assay) and genotype at rs1800629 ( TNFα) and rs7775397 ( C6orf10) (allelic discrimination). The transmission disequilibrium test (TDT) was computed to test for nonrandom transmission from maternal grandparents to mothers of children with NL. Results The common phenotypic feature in mothers of children with NL was the autoantibody and not the clinical profile; 7 had lupus, 14 had Sjögren's syndrome, 7 had both, and 23 were asymptomatic. Mothers of children with NL were significantly enriched for the risk alleles at both TNFα and C6orf10. The grandparents of children with NL carried minimal burden for autoimmune disease or abnormal antibody production and were not enriched in the genetic risk factors. However, the TDT analysis showed significant excess transmission of the risk alleles at both TNFα (odds ratio [OR] 6.67, P = 3.93 × 10−4) and C6orf10 (OR 35.0, P = 3.74 × 10−5) to mothers of children with NL. Conclusion Mothers of children with NL are enriched for the TNFα and C6orf10 risk alleles, which are preferentially inherited from the asymptomatic maternal grandparents. These findings support the hypothesis that the development of NL and genetic etiology are multigenerational. [ABSTRACT FROM AUTHOR]

Published

2012

11. Association of PPP2CA polymorphisms with systemic lupus erythematosus 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., and Brown, Elizabeth E.

Subjects

SYSTEMIC lupus erythematosus, AUTOANTIBODIES, COMPUTER software, CONFIDENCE intervals, EPIDEMIOLOGY, GENES, GENETIC polymorphisms, POLYMERASE chain reaction, RESEARCH funding, DATA analysis, CASE-control method, REVERSE transcriptase polymerase chain reaction, GENETICS

Abstract

Objective 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. Methods 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. Results 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). Conclusion 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. [ABSTRACT FROM AUTHOR]

Published

2011

12. Identification of Candidate Loci at 6p21 and 21q22 in a Genome-Wide Association Study of Cardiac Manifestations of Neonatal Lupus.

Author

Clancy, Robert M., Marion, Miranda C., Kaufman, Kenneth M., Ramos, Paula S., Adler, Adam, Harley, John B., Langefeld, Carl D., and Buyon, Jill P.

Abstract

The article evaluates single-nucleotide polymorphisms (SNP) for associations with cardiac neonatal lupus in children of European ancestry. A total of 116 subjects were genotyped and merged with 3,351 controls. The results showed that the 17 most significant associations with cardiac neonatal lupus were found in the HLA region. The region near the MICB gene showed the strongest variant. The results suggested that variation near genes related to inflammatory and apoptotic responses may promote cardiac injury caused by passively acquired autoantibodies.

Published

2010

13. The Susceptibility Loci Juvenile Idiopathic Arthritis Shares With Other Autoimmune Diseases Extend to PTPN2, COG6, and ANGPT1.

Author

Thompson, Susan D., Sudman, Marc, Ramos, Paula S., Marion, Miranda C., Ryan, Mary, Tsoras, Monica, Weiler, Tracey, Wagner, Michael, Keddache, Mehdi, Haas, J. Peter, Mueller, Cornelia, Prahalad, Sampath, Bohnsack, John, Wise, Carol A., Punaro, Marilynn, Dongping Zhang, Rosé, Carlos D., Comeau, Mary E., Divers, Jasmin, and Glass, David N.

Abstract

The article tests the associations between non-major histocompatibility complex susceptibility loci previously reported in autoimmune diseases and juvenile idiopathic arthritis (JIA). Published autoimmune disease genome-wide association studies were reviewed and 257 single-nucleotide polymorphisms (SNPs) were selected while 168 were imputed with quality. Replication was sought for 21 SNPs in a second group. The results showed general susceptibility loci for autoimmunity are shared across diseases, suggesting the potential for common therapy.

Published

2010

14. Features associated with, and the impact of, hemolytic anemia in patients with systemic lupus erythematosus: LX, results from a multiethnic cohort.

Author

Durán, Sergio, Apte, Mandar, Alarcón, Graciela S., Marion, Miranda C., Edberg, Jeffrey C., Kimberly, Robert P., Zhang, Jie, Langefeld, Carl D., ViLá, Luis M., and Reveille, John D.

Published

2008

15. A159: The Autoimmune Genetic Architecture of Childhood Onset Rheumatoid Arthritis.

Author

Prahalad, Sampath, Marion, Miranda C., Cobb, Joanna, Sudman, Marc, Hinks, Anne, Pichavant, Mina, Ponder, Lori, Reed, Ann M., Wallace, Carol, Becker, Mara L., Yeung, Rae S. M., Rosenberg, Alan M., Punaro, Marilynn G., Mellins, Elizabeth D., Nelson, J. Lee, Videm, Vibeke, Rygg, Marite, Nordal, Ellen, Brown, Matthew A., and Cutler, David

Subjects

*GENETICS of autoimmune diseases, *EPIDEMIOLOGY, *GENES, *GENETIC polymorphisms, *GENETIC research, *PROBABILITY theory, *PHENOTYPES, *BIOCHIPS, *DATA analysis

Abstract

Background/Purpose: Genome-wide association studies have identified susceptibility loci for many autoimmune diseases, including rheumatoid arthritis (RA) and juvenile idiopathic arthritis (JIA). About 5% of children with JIA have rheumatoid factor positive arthritis that is phenotypically similar to adult seropositive RA, thus representing childhood onset RA (CORA). To understand the genetic architecture of CORA risk relative to other autoimmune diseases, we genotyped CORA cases and controls on the Immunochip, a custom array designed by the Immunochip Consortium to fine map autoimmune disease-associated loci shared across 11 autoimmune phenotypes. Methods: Genotyping was completed on 340 CORA cases (mean onset age: 10.2 ± 4.2 yrs) and 11624 controls. Standard SNP and sample QC was performed (e.g., removing samples with call rate <98%, admixture outliers). To test for SNP association with CORA a logistic regression model was computed with Caucasian admixture proportions (ADMIXTURE) as covariates (SNPLash). False discovery rate (FDR) adjusted p-values (PFDR) are reported to account for the actual number of tests computed. Results: SNP rs3129769, near HLA DRB1 was the most significantly associated (PFDR <3×10-25), and is in linkage disequilibrium with the HLA DRB1 SNP reported in RA (rs660895, PFDR <1×10-24). Outside the HLA region, 28 regions had ≥1 SNP meeting genome-wide significance (PFDR<0.05). The best signal of association was on 22q13 (rs9610687, OR = 0.57, PFDR < 0.0002) near IL2RB, followed by the PTPN22 locus (rs6679677, OR = 1.83, PFDR < 0.0005), an intergenic SNP on chromosome 4 (rs970036, OR = 1.78, PFDR < 0.002) and an intronic SNP (19p13, rs3787016 PFDR < 0.002) in the POLR2E gene, which encodes a subunit of RNA polymerase II. Some loci which have previously been implicated in RA had evidence of association including MMEL (rs751358 PFDR < 0.003), IRF5 (rs4731531 PFDR < 0.006) and CCR6 (rs11575078 PFDR < 0.03). In addition using the FDR-based threshold we identified several potential SNPs (rs10918214, 1q23; rs28491312, 14q31) not previously implicated in RA. Conclusion: Immunochip analysis of the largest cohort of CORA investigated to date has confirmed the HLA DRB1 association and identified several other loci associated with CORA. Comparisons among loci associated with CORA and those identified in RA and other forms of JIA are underway and will help delineate the unique genetic factors for CORA susceptibility. [ABSTRACT FROM AUTHOR]

Published

2014

16. Morphometric analysis of arteriolar tortuosity in human cerebral white matter of preterm, young and aged subjects.

Author

Thore, Clara R., Anstrom, John A., Moody, Dixon M., Challa, Venkata R., Marion, Miranda C., and Brown, William R.

Subjects

ARTERIES, BRAIN, ALZHEIMER'S disease, BLOOD vessels, CAPILLARIES

Abstract

Arteriolar tortuosities, consisting of vascular coils, loops and spirals, appear in cerebral white matter (WM) in some individuals. Autopsy brains were studied from 55 subjects ranging in age from 23 weeks postconception to 102 years. Fourteen of these subjects were diagnosed with leukoaraiosis (LA) and 7 with Alzheimer's disease (AD). Using computerized morphometry, vascular curl (curvilinear length/straight length) was measured in every WM arteriole >100 pm long in one alkaline phosphatase-stained, celloidin section per subject. Vascular curl (Mean ±SD) in subcortical (1.15 ± 0.09) and in deep (1.13 ± 0.18) WM were not different (P=0.93). High curl scores (≥2.00) were observed in subjects older than 40 years, but not in preterm and young (3 months to 27 yrs) subjects. While some older adults, like younger subjects, had low curl scores, other aged individuals had high curl scores indicative of tortuosity. Both incidence (P=0.009) and severity (P=0.0297) of tortuosity were significantly elevated in subjects >40 yrs compared to young subjects. Curl scores were not significantly increased in AD or LA compared to subjects without AD or LA. We conclude that 1) tortuous vessels are not present in preterm babies, children, or young adults, 2) significant tortuosity begins in middle age, and 3) in a subset of aged individuals, tortuosity does not appear regardless of longevity. [ABSTRACT FROM AUTHOR]

Published

2007

17. Brief report: enrichment of associations in genes with fibrosis, apoptosis, and innate immunity functions with cardiac manifestations of neonatal lupus.

Author

Ramos PS, Marion MC, Langefeld CD, Buyon JP, and Clancy RM

Subjects

Case-Control Studies, Fibrosis genetics, Genome-Wide Association Study, Humans, Infant, Newborn, Linkage Disequilibrium genetics, Lupus Erythematosus, Systemic genetics, Polymorphism, Single Nucleotide genetics, Apoptosis genetics, Immunity, Innate genetics, Lupus Erythematosus, Systemic congenital, Myocardium pathology

Abstract

Objective: The proposed pathogenesis of the cardiac manifestations of neonatal lupus (cardiac-NL) involves maternal autoantibodies to the RNPs SSA/Ro and SSB/La, enhanced by as-yet-unknown factors that likely involve dysregulation of both inflammatory and fibrotic fetal responses. This study was designed to improve the power to detect specific associations in genes with candidate biologic functions., Methods: Using data from our genome-wide association study of 116 Caucasian children with cardiac-NL and 3,351 Caucasian controls, we tested for enrichment of single-nucleotide polymorphism (SNP) associations in genes with candidate biologic functions related to fibrosis, immune function, apoptosis, T cell function, cell infiltration, innate immune cell function, interferon, Toll-like receptors, and calcium channels. After linkage disequilibrium pruning and exclusion of the extended HLA region, a total of 15,103 SNPs in 3,068 genes remained., Results: A highly significant enrichment of P values was observed for genes related to fibrosis (P = 2.27 × 10(-9) ), apoptosis (P = 7.67 × 10(-7) ), and innate immune cell (P = 2.53 × 10(-6) ), immune (P = 5.01 × 10(-4) ), T cell (P = 2.23 × 10(-4) ), and interferon functions (P = 1.64 × 10(-3) ). The most significant non-HLA associations included the sialyltransferase gene ST8SIA2 (rs1487982; odds ratio 2.20 [95% confidence interval 1.52-3.19], P = 3.37 × 10(-5) ), the integrin gene ITGA1 (rs2432143; odds ratio 2.31 [95% confidence interval 1.54-3.45], P = 4.54 × 10(-5) ), and the complement regulator gene CSMD1 (rs7002001; odds ratio 2.41 [95% confidence interval 1.57-3.72], P = 6.33 × 10(-5) )., Conclusion: This study identified novel candidate genes associated with cardiac-NL and highlights the value of studying this cohort for advancing knowledge regarding the genetic etiology of this syndrome. Identification of causal alleles is expected to provide critical insight into the molecular mechanisms responsible for linking maternal autoantibodies to cardiac scarring in these fetuses/neonates., (Copyright © 2012 by the American College of Rheumatology.)

Published

2012