Your search keyword '"Clancy, Robert M."' showing total 11 results

1. Reactivity to the p305 Epitope of the α1G T-Type Calcium Channel and Autoimmune-Associated Congenital Heart Block.

Author

Markham AJ, Rasmussen SE, Salmon JE, Martinez-Ortiz W, Cardozo TJ, Clancy RM, and Buyon JP

Subjects

Adult, Antibodies, Antinuclear blood, Antibodies, Antinuclear genetics, Apoptosis, Autoantibodies blood, Autoantibodies immunology, Autoimmune Diseases blood, Autoimmune Diseases immunology, Biomarkers blood, Calcium Channels, T-Type blood, Calcium Channels, T-Type genetics, Epitopes blood, Epitopes immunology, Female, Heart Block blood, Heart Block immunology, Humans, Infant, Newborn, Pregnancy, Risk Factors, Young Adult, Antibodies, Antinuclear immunology, Autoimmune Diseases complications, Calcium Channels, T-Type immunology, Heart Block congenital

Abstract

Background: Only 2% of mothers positive for anti-SSA/Ro (Ro) antibodies have children with congenital heart block (CHB). This study aimed to determine whether reactivity with p305, an epitope within the α1G T-type calcium channel, confers added risk over anti-Ro antibodies., Methods and Results: Using sera from anti-Ro-exposed pregnancies resulting in offspring with CHB, no disease but CHB-sibling, and no disease and no CHB-sibling, as well as disease (lupus without anti-Ro) and healthy controls, reactivities were determined for binding to Ro60, p305, and an epitope within Ro60, p133-Ro60, which shares structural properties with p305, including key amino acids and an α-helical structure. Candidate peptides were further evaluated in an in vitro model that assessed the binding of maternal antibodies to apoptotic cells. In anti-Ro-positive mothers, anti-p305 autoantibodies (>3 SD above healthy controls) were detected in 3/59 (5%) CHB pregnancies, 4/30 (13%) unaffected pregnancies with a CHB-sibling, and 0/42 (0%) of unaffected pregnancies with no CHB-sibling. For umbilical bloods (61 CHB, 41 healthy with CHB sibling), no association of anti-p305 with outcome was detected; however, overall levels of anti-p305 were elevated compared to mothers during pregnancy in all groups studied. For anti-p133-Ro60, reactivity paralleled that of anti-p305. In the screen employing apoptotic cells, p133-Ro60, but not p305, significantly attenuated the binding of immunoglobulin G isolated from a mother whose child had CHB (42.1% reduced to 13.9%, absence/presence of p133-Ro60, respectively, P<0.05)., Conclusions: These data suggest that anti-p305 is not a robust maternal marker for assessing increased risk of CHB during an anti-SSA/Ro pregnancy., (© 2015 The Authors. Published on behalf of the American Heart Association, Inc., by Wiley Blackwell.)

Published

2015

2. Complement receptor 3 influences toll-like receptor 7/8-dependent inflammation: implications for autoimmune diseases characterized by antibody reactivity to ribonucleoproteins.

Author

Reed JH, Jain M, Lee K, Kandimalla ER, Faridi MH, Buyon JP, Gupta V, and Clancy RM

Subjects

Allosteric Site, Anti-Inflammatory Agents pharmacology, Cell Adhesion, Down-Regulation, Heterozygote, Humans, Inflammation, Leukocytes, Mononuclear cytology, Leukocytes, Mononuclear metabolism, Lupus Erythematosus, Systemic metabolism, Macrophages cytology, Models, Genetic, Myeloid Differentiation Factor 88 metabolism, RNA metabolism, Signal Transduction, Autoimmune Diseases metabolism, CD11b Antigen biosynthesis, Gene Expression Regulation, Macrophage-1 Antigen metabolism, Macrophages metabolism, Toll-Like Receptor 7 metabolism, Toll-Like Receptor 8 metabolism

Abstract

Toll-like receptor (TLR) signaling is an important component in the inflammatory response generated in diseases characterized by autoantibody reactivity to proteins such as SSA/Ro in complex with endogenous nucleic acids. Complement receptor 3 (CR3), a genetic variant of which has been identified as a risk factor in systemic lupus erythematosus, has been shown to induce tolerogenic responses in dendritic cells and suppress TLR4 responses in a murine sepsis model. Accordingly, this study addressed the hypothesis that activation of CR3, influenced by genotype of CD11b, negatively regulates TLR7/8-dependent effector function. Allosteric activation of CD11b via pretreatment with the small molecule, leukadhedrin 1 (LA1), significantly attenuated TLR7/8-induced (hY3 RNA, R848) secretion of TNFα in THP-1 cells and human macrophages isolated from donors homozygous for the ancestral common ITGAM allele at rs1143679. This inhibition was accompanied by profound degradation of the adaptor protein MyD88, an effect not observed with direct inhibition of TLR ligation by an antagonist oligonucleotide. In contrast, the addition of LA1 after incubation with the TLR agonists did not result in MyD88 degradation and subsequent attenuation of TNFα secretion. In TLR7/8-stimulated macrophages isolated from donors heterozygous for the CD11b variant, pretreatment with LA1 did not down-regulate TNFα release. These novel findings support a negative cross-talk between CR3 and TLR pathways likely to be induced by antibodies reactive with ribonucleoproteins and point to the development of CR3-specific agonists as potential therapeutics for diseases such as neonatal lupus.

Published

2013

3. Autoimmune-associated congenital heart block: dissecting the cascade from immunologic insult to relentless fibrosis.

Author

Clancy RM and Buyon JP

Subjects

Animals, Autoantigens immunology, Autoantigens metabolism, Autoimmune Diseases immunology, Autoimmune Diseases pathology, Fibrosis pathology, Heart Block immunology, Heart Block pathology, Heart Defects, Congenital, Humans, Isoantibodies immunology, Isoantibodies metabolism, Lupus Erythematosus, Systemic immunology, Lupus Erythematosus, Systemic pathology, Macrophages pathology, Myocytes, Cardiac immunology, Myocytes, Cardiac pathology, Autoimmune Diseases congenital, Fibrosis etiology, Heart Block congenital, Lupus Erythematosus, Systemic congenital

Abstract

Few diseases exemplify the integration of research from bench to bedside as well as neonatal lupus, often described as a model of passively acquired autoimmunity. The signature histologic lesion of autoimmune congenital heart block (CHB) is fibrosis of the conducting tissue and, in some cases, the surrounding myocardium. Although anti-SSA/Ro-SSB/La antibodies are detected in > 85% of mothers whose fetuses are identified with conduction abnormalities in a structurally normal heart, the risk for a woman with the candidate antibodies to have a child with CHB is 2%. The mechanism by which maternal anti-SSA/Ro-SSB/La antibodies initiate and finally eventuate in atrioventricular nodal scarring is not yet defined, but it is clear that the antibodies alone are insufficient to cause disease and fetal factors are likely contributory. Previous in vitro and in vivo studies suggest that the pathologic cascade is initiated via apoptosis, resulting in translocation of SSA/Ro-SSB/La antigens to the cell surface where they are bound by maternal autoantibodies. Subsequently, the Fc portion of the bound immunoglobulin engages Fcgamma receptors on tissue macrophages, resulting in release of TGF-beta at a threshold favoring a profibrotic milieu and irreversible scarring. This cascade also involves tissue-specific activation of TGF-beta, which promotes the modulation of fibroblasts into myofibroblasts, a scarring phenotype. Recent findings point to genetic polymorphisms that promote high production of TGF-beta as possible fetal risk factors for CHB. Further elucidation of maternal and fetal contributory factors should provide insight into the pathogenesis of CHB and the rarity of irreversible injury., (copyright 2004 Wiley-Liss, Inc.)

Published

2004

4. Cytokine polymorphisms and histologic expression in autopsy studies: contribution of TNF-alpha and TGF-beta 1 to the pathogenesis of autoimmune-associated congenital heart block.

Author

Clancy RM, Backer CB, Yin X, Kapur RP, Molad Y, and Buyon JP

Subjects

Arginine genetics, Autoimmune Diseases congenital, Autoimmune Diseases pathology, Autopsy, Child, Exanthema genetics, Exanthema metabolism, Exanthema pathology, Female, Fetal Diseases genetics, Fetal Diseases pathology, Gene Frequency, Genetic Predisposition to Disease, Heart Block congenital, Heart Block immunology, Heart Block pathology, Humans, Leucine genetics, Mothers, RNA, Messenger biosynthesis, Transforming Growth Factor beta genetics, Transforming Growth Factor beta1, Autoimmune Diseases genetics, Cytokines biosynthesis, Cytokines genetics, Heart Block genetics, Polymorphism, Genetic immunology, Transforming Growth Factor beta physiology, Tumor Necrosis Factor-alpha physiology

Abstract

Although Abs to SSA/Ro-SSB/La are necessary for the development of congenital heart block (CHB), the low frequency suggests that fetal factors are contributory. Because CHB involves a cascade from inflammation to scarring, polymorphisms of the TNF-alpha promoter region and codons 10 and 25 of the TGF-beta gene were evaluated in 88 children (40 CHB, 17 rash, 31 unaffected siblings) and 74 mothers from the Research Registry for Neonatal Lupus (NL). Cytokine expression was assessed in autopsy material from two fetuses with CHB. Significantly increased frequency of the -308A (high-producer) allele of TNF-alpha was observed in all NL groups compared with controls. In contrast, the TGF-beta polymorphism Leu(10) (associated with increased fibrosis) was significantly higher in CHB children (genotypic frequency 60%, allelic frequency 78%) than unaffected offspring (genotypic frequency 29%, p = 0.016; allelic frequency 56%, p = 0.011) and controls, while there were no significant differences between controls and other NL groups. For the TGF-beta polymorphism, Arg(25), there were no significant differences between NL groups and controls. In fetal CHB hearts, protein expression of TGF-beta, but not TNF-alpha, was demonstrated in septal regions, extracellularly in the fibrous matrix, and intracellularly in macrophage infiltrates. Age-matched fetal hearts from voluntary terminations expressed neither cytokine. TNF-alpha may be one of several factors that amplify susceptibility; however, the genetic studies, backed by the histological data, more convincingly link TGF-beta to the pathogenesis of CHB. This profibrosing cytokine and its secretion/activation circuitry may provide a novel direction for evaluating fetal factors in the development of a robust animal model of CHB as well as therapeutic strategies in humans.

Published

2003

5. Does the cellular localization of antigens in or on apoptotic blebs influence the pathogenicity or benefit of cognate antibodies? Comment on the article by Dieudé et al.

Author

Clancy RM, Chan EK, Chandrashekhar S, and Buyon JP

Subjects

Humans, Apoptosis immunology, Autoantibodies immunology, Autoantigens immunology, Autoimmune Diseases immunology

Published

2003

6. From antibody insult to fibrosis in neonatal lupus - the heart of the matter.

Author

Buyon JP and Clancy RM

Subjects

Adult, Antibodies, Antinuclear immunology, Atrioventricular Node embryology, Atrioventricular Node immunology, Autoimmune Diseases complications, Autoimmune Diseases embryology, Autoimmune Diseases immunology, Autoimmune Diseases pathology, Female, Fetal Heart immunology, Fetal Heart pathology, Fibroblasts pathology, Fibrosis, Heart Block etiology, Heart Block immunology, Heart Block pathology, Humans, Infant, Newborn, Inflammation, Isoantibodies immunology, Isoantibodies metabolism, Lupus Erythematosus, Systemic complications, Lupus Erythematosus, Systemic embryology, Lupus Erythematosus, Systemic immunology, Lupus Erythematosus, Systemic pathology, Macrophages pathology, Myocytes, Cardiac immunology, Myocytes, Cardiac pathology, Pregnancy, Ribonucleoproteins immunology, SS-B Antigen, Atrioventricular Node pathology, Autoantigens, Autoimmune Diseases congenital, Heart Block congenital, Immunity, Maternally-Acquired, Lupus Erythematosus, Systemic congenital, RNA, Small Cytoplasmic

Abstract

Few diseases exemplify the integration of research from bench to bedside as well as neonatal lupus, often referred to as a model of passively acquired autoimmunity. In essence, this disease encompasses two patients, both the mother and her child. The signature histologic lesion of autoimmune-associated congenital heart block is fibrosis of the conducting tissue, and in some cases the surrounding myocardium. It is astounding how rapid and, in most cases, irreversible is the fibrotic response to injury. The mechanism by which maternal anti-SSA/Ro-SSB/La antibodies initiate and perpetuate inflammation, and eventuate in scarring of the atrioventricular node, is not yet defined. In vitro and in vivo studies suggest that one pathologic cascade leading to scarring may be initiated via apoptosis, resulting in translocation of SSA/Ro-SSB/La antigens and subsequent surface binding by maternal autoantibodies. These opsonized cardiocytes are phagocytosed by macrophages, which secrete factors that transdifferentiate fibroblasts into myofibroblasts, a scarring phenotype. Dissecting the individual components in this fibrotic pathway should provide insights into the rarity of irreversible injury and should form the basis of rational approaches to prevention and treatment.

Published

2003

7. 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

8. Apolipoprotein L1 risk variants associate with prevalent atherosclerotic disease in African American systemic lupus erythematosus patients.

Author

Blazer, Ashira, Wang, Binhuan, Simpson, Danny, Kirchhoff, Tomas, Heffron, Sean, Clancy, Robert M., Heguy, Adriana, Ray, Karina, Snuderl, Matija, and Buyon, Jill P.

Subjects

SYSTEMIC lupus erythematosus, APOLIPOPROTEINS, ATHEROSCLEROSIS prevention, CARDIOVASCULAR diseases, MYOCARDIAL infarction, CAROTID artery diseases, HYPERTENSION, CALCIFICATIONS of the breast, PATIENTS

Abstract

Objective: Atherosclerosis is exaggerated in African American (AA) systemic lupus erythematosus (SLE) patients, with doubled cardiovascular disease (CVD) risk compared to White patients. The extent to which common Apolipoprotein L1 (APOL1) risk alleles (RA) contribute to this trend is unknown. This retrospective cohort study assessed prevalent atherosclerotic disease across APOL1 genotypes in AA SLE patients. Methods: One hundred thirteen AA SLE subjects were APOL1-genotyped and stratified as having: zero risk alleles, one risk allele, or two risk alleles. Chart review assessed CVD manifestations including abdominal aortic aneurysm, angina, carotid artery disease, coronary artery disease, myocardial infarction, peripheral vascular disease, stroke, and vascular calcifications. Associations between the genotypes and a composite endpoint defined as one or more CVD manifestations were calculated using logistic regression. Symptomatic atherosclerotic disease, excluding incidental vascular calcifications, was also assessed. Results: The 0-risk-allele, 1-risk-allele and 2-risk-allele groups, respectively, comprised 34%, 53%, and 13% of the cohort. Respectively, 13.2%, 41.7%, and 60.0% of the 0-risk allele, 1-risk-allele, and 2-risk-allele groups met the composite endpoint of atherosclerotic CVD (p = 0.001). Adjusting for risk factors–including smoking, ESRD, BMI >25 and hypertension–we observed an association between carrying one or more RA and atherosclerotic CVD (OR = 7.1; p = 0.002). For symptomatic disease, the OR was 3.5 (p = 0.02). In a time-to-event analysis, the proportion of subjects free from the composite primary endpoint, symptomatic atherosclerotic CVD, was higher in the 0-risk-allele group compared to the 1-risk-allele and 2-risk-allele groups (χ2 = 6.5; p = 0.04). Conclusions: Taken together, the APOL1 RAs associate with prevalent atherosclerotic CVD in this cohort of AA SLE patients, perhaps reflecting a potentiating effect of SLE on APOL1-related cardiovascular phenotypes. [ABSTRACT FROM AUTHOR]

Published

2017

9. Brief Report: IRF5 systemic lupus erythematosus risk haplotype is associated with asymptomatic serologic autoimmunity and progression to clinical autoimmunity in mothers of children with neonatal lupus.

Author

Cherian, Tharian S., Kariuki, Silvia N., Franek, Beverly S., Buyon, Jill P., Clancy, Robert M., and Niewold, Timothy B.

Subjects

AUTOIMMUNE diseases, SYSTEMIC lupus erythematosus, CONFIDENCE intervals, ENZYME-linked immunosorbent assay, EPIDEMIOLOGY, FISHER exact test, GENES, GENETIC polymorphisms, MOTHERS, RESEARCH funding, RISK assessment, SJOGREN'S syndrome, LOGISTIC regression analysis, DATA analysis, CHILDREN, DISEASE risk factors, GENETICS

Abstract

Objective Variation in the interferon regulatory factor 5 (IRF5) gene has been associated with risk of developing systemic lupus erythematosus (SLE), and this association is largely dependent upon anti-Ro autoantibodies. This study was undertaken to determine if the IRF5 genotype is associated with maternal diagnosis or progression of autoimmunity. Methods Genotyping of haplotype-tagging polymorphisms in IRF5 was performed in 93 subjects of European ancestry who were recruited to the Research Registry for Neonatal Lupus. All subjects had high-titer anti-Ro autoantibodies and had a child with neonatal lupus (NL); allele frequencies were compared to those in nonautoimmune controls. The mothers had SLE, Sjögren's syndrome (SS), or undifferentiated autoimmune syndrome (UAS), or were asymptomatic. Results The SLE risk haplotype of IRF5 was enriched in all anti-Ro-positive subjects except in those with SS (odds ratio [OR] 2.55, P = 8.8 × 10−4). The SLE risk haplotype was even enriched in asymptomatic individuals with anti-Ro antibodies (OR 2.69, P = 0.019). The same haplotype was more prevalent in subjects who were initially asymptomatic but developed symptomatic SLE during followup (OR 5.83, P = 0.0024). Interestingly, SS was associated with 2 minor IRF5 haplotypes, and these same haplotypes were decreased in frequency in mothers with SLE and those with UAS. Conclusion The IRF5 SLE risk haplotype was associated with anti-Ro antibody positivity in asymptomatic individuals, as well as with progression to SLE in asymptomatic anti-Ro-positive individuals. SS in mothers of children with NL was associated with different IRF5 haplotypes. These data suggest that IRF5 polymorphisms play a role in serologic autoimmunity in humans and may promote the progression to clinical autoimmunity. [ABSTRACT FROM AUTHOR]

Published

2012

10. Recurrence Rates of Cardiac Manifestations Associated With Neonatal Lupus and Maternal/Fetal Risk Factors.

Author

Llanos, Carolina, Izmirly, Peter M., Katholi, Margaret, Clancy, Robert M., Friedman, Deborah M., Kim, Mimi Y., and Buyon, Jill P.

Subjects

LUPUS erythematosus, PREGNANCY, NEONATAL infections, AUTOIMMUNE diseases, PREGNANT women, DISEASE risk factors

Abstract

The article presents a study on the recurrence rates of cardiac neonatal lupus (NL) and risk factors for NL. Rates of recurrence for cardiac NL and risk factors were evaluated in pregnancies immediately following the birth of an affected child. The study found that the overall recurrence rate for the women studied was 17.4%. 23% of mothers with an undifferentiated autoimmune syndrome had a second child with cardiac NL. Recurrence rates were not affected by maternal health or steroid use.

Published

2009

11. Congenital heart block: Identification of autoantibody binding site on the extracellular loop (domain I, S5–S6) of α1D L-type Ca channel

Author

Karnabi, Eddy, Qu, Yongxia, Wadgaonkar, Raj, Mancarella, Salvatore, Yue, Yuankun, Chahine, Mohamed, Clancy, Robert M., Buyon, Jill P., and Boutjdir, Mohamed

Subjects

*HEART block, *CONGENITAL heart disease in children, *AUTOANTIBODIES, *BINDING sites, *CALCIUM channels, *AUTOIMMUNE diseases, *NUCLEOPROTEINS, *ATRIOVENTRICULAR node

Abstract

Abstract: Congenital heart block (CHB) is an autoimmune disease associated with autoantibodies against intracellular ribonucleoproteins SSB/La and SSA/Ro. The hallmark of CHB is complete atrioventricular block. We have recently established that anti-SSA/Ro -SSB/La autoantibodies inhibit α1D L-type Ca current, ICa-L, and cross-react with the α1D Ca channel protein. This study aims at identifying the possible binding sites on α1D protein for autoantibodies from sera of mothers with CHB children. GST fusion proteins of the extracellular regions between the transmembrane segments (S5–S6) of each of the four α1D Ca channel protein domains I–IV were prepared and tested for reactivity with sera from mothers with CHB children and controls using ELISA. Sera containing anti-Ro/La autoantibodies from 118 mothers with CHB children and from 15 mothers with anti-Ro/La autoantibodies but have healthy children, and from 28 healthy mothers without anti-Ro/La autoantibodies and healthy children were evaluated. Seventeen of 118 (14.4%) sera from mothers with CHB children reacted with the extracellular loop of domain I S5–S6 region (E1). In contrast, only 2 of 28 (7%) of sera from healthy mothers (−anti-Ro/La) and healthy children reacted with E1 loop and none (0 of 15) of sera from healthy mothers (+anti-Ro/La) and healthy children reacted with the E1 loop. Preincubation of E1 loop with the positive sera decreased the O.D reading establishing the specificity of the response. Electrophysiological characterization of the ELISA positive sera and purified IgG showed inhibition (44.1% and 49.8%, respectively) of the α1D ICa-L expressed in tsA201 cells. The inhibition was abolished when the sera were pre-incubated with E1 fusion protein. The results identified the extracellular loop of domain I S5–S6 of L-type Ca channel α1D subunit as a target for autoantibodies from a subset of mothers with CHB children. This novel finding provides insights into the potential development of therapeutic peptides that could bind to the pathogenic antibodies and prevent CHB. [Copyright &y& Elsevier]

Published

2010