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1. Investigating the molecular targets of antiphospholipid antibodies

Author

Ioannou, Y.

Subjects
616.97
Abstract

The antiphospholipid syndrome (APS) is characterised by the presence of pathogenic antiphospholipid antibodies (aPL) that bind phospholipid via the N-terminal domain I (DI) of the protein cofactor beta2-glycoprotein I (beta2GPI). This thesis aims to investigate and identify the nature of this interaction at the molecular level. In order to study DI, a system for expressing and purifying sufficient quantities of this protein was developed using Escherichia coli (E.coli) as the expression host. This was achieved primarily by synthesising a gene with all codons optimised for E.coli, tight regulation of expression and recovery of DI from the periplasm to facilitate folding. Recombinant purified DI bound clinically relevant human monoclonal and polyclonal purified IgG aPL in both solid an fluid phase assays. Hypotheses were generated that identified candidate epitopes for aPL binding as potentially involving residues D8, D9, E23, E26, E27, R39, G40, R43 and the DI-II interlinker region. In total, 15 mutants of DI targeting these areas were created and computer modelling employed to predict the likely structural effects of these mutations upon DI. Expressed DI mutants were then tested in both solid and fluid phase assays for binding to polyclonal IgG derived from patients with APS and compared to wild-type DI. Some mutations, such as those targeting R39, caused loss of binding to aPL in the fluid phase whilst others caused enhanced binding over wild-type DI. In conclusion, this thesis demonstrates that DI of 62GPI may be expressed using E.coli and binds clinically relevant IgG aPL. Detailed mutational studies support the concept that aPL bind discontinuous epitopes on DI involving regions D8 and D9, R39 to R43 and the DI-II interlinker which are in close proximity to each other in the tertiary structure. The ability to produce a mutant of DI with enhanced binding over wild-type holds therapeutic potential.

Published
2007

3. Development and external validation of a model predicting new-onset chronic uveitis at different disease durations in juvenile idiopathic arthritis

Author

van Straalen, Joeri W., Kearsley-Fleet, Lianne, Klotsche, Jens, de Roock, Sytze, Minden, Kirsten, Heiligenhaus, Arnd, Hyrich, Kimme L., de Boer, Joke H., Lamot, Lovro, Olivieri, Alma N., Gallizzi, Romina, Smolewska, Elzbieta, Faugier, Enrique, Pastore, Serena, Hashkes, Philip J., Herrera, Cristina N., Emminger, Wolfgang, Consolini, Rita, Wulffraat, Nico M., Ruperto, Nicolino, Swart, Joost F., Cleary, G., Baildam, E., Wedderburn, L., Davidson, J., Chieng, A., McErlane, F., Foster, H., Ciurtin, C., Ioannou, Y., Thomson, W., Kallinich, Tilmann, Dressler, Frank, Deschner, Jasmin Kümmerle, Weller-Heinemann, Frank, Horneff, Gerd, Hospach, Anton, Mönkemöller, Kirsten, Haas, Johannes Peter, Windschall, Daniel, Foeldvari, Ivan, and Foell, Dirk

Subjects
Rheumatology, Immunology, Medizin, Uveitis, Juvenile Idiopathic Arthritis, JIA, Immunology and Allergy
Abstract

Objective: To develop and externally validate a prediction model for new-onset chronic uveitis in children with juvenile idiopathic arthritis (JIA) for clinical application. Methods: Data from the international Pharmachild registry were used to develop a multivariable Cox proportional hazards model. Predictors were selected by backward selection, and missing values were handled by multiple imputation. The model was subsequently validated and recalibrated in 2 inception cohorts: the UK Childhood Arthritis Prospective Study (CAPS) study and the German Inception Cohort of Newly diagnosed patients with juvenile idiopathic arthritis (ICON) study. Model performance was evaluated by calibration plots and C statistics for the 2-, 4-, and 7-year risk of uveitis. A diagram and digital risk calculator were created for use in clinical practice. Results: A total of 5, 393 patients were included for model development, and predictor variables were age at JIA onset (hazard ratio [HR] 0.83 [95% confidence interval (95% CI) 0.77-0.89]), ANA positivity (HR 1.59 [95% CI 1.06-2.38]), and International League of Associations for Rheumatology category of JIA (HR for oligoarthritis, psoriatic arthritis, and undifferentiated arthritis versus rheumatoid factor-negative polyarthritis 1.40 [95% CI 0.91- 2.16]). Performance of the recalibrated prediction model in the validation cohorts was acceptable ; calibration plots indicated good calibration and C statistics for the 7-year risk of uveitis (0.75 [95% CI 0.72-0.79] for the ICON cohort and 0.70 [95% CI 0.64-0.76] for the CAPS cohort). Conclusion: We present for the first time a validated prognostic tool for easily predicting chronic uveitis risk for individual JIA patients using common clinical parameters. This model could be used by clinicians to inform patients/parents and provide guidance in choice of uveitis screening frequency and arthritis drug therapy.

Published
2022

7. Clinical relevance of nitrated beta 2-glycoprotein I in antiphospholipid syndrome: Implications for thrombosis risk

Author

Krilis, M., primary, Qi, M., additional, Ioannou, Y., additional, Zhang, J.Y., additional, Ahmadi, Z., additional, Wong, J.W.H., additional, Vlachoyiannopoulos, P.G., additional, Moutsopoulos, H.M., additional, Koike, T., additional, Sturgess, A.D., additional, Chong, B.H., additional, Krilis, S.A., additional, and Giannakopoulos, B., additional

Published
2021
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8. Clinical relevance of nitrated beta 2-glycoprotein I in antiphospholipid syndrome: Implications for thrombosis risk

Author

Krilis, M. Qi, M. Ioannou, Y. Zhang, J.Y. Ahmadi, Z. Wong, J.W.H. Vlachoyiannopoulos, P.G. Moutsopoulos, H.M. Koike, T. Sturgess, A.D. Chong, B.H. Krilis, S.A. Giannakopoulos, B.

Abstract

Β2-Glycoprotein I (β2GPI) is an important anti-thrombotic protein and is the major auto-antigen in the antiphospholipid syndrome (APS). The clinical relevance of nitrosative stress in post translational modification of β2GPI was examined.The effects of nitrated (n)β2GPI on its anti-thrombotic properties and its plasma levels in primary and secondary APS were determined with appropriate clinical control groups. β2-glycoprotein I was nitrated at tyrosines 218, 275 and 309. β2-glycoprotein I binds to lipid peroxidation modified products through Domains IV and V. Nitrated β2GPI loses this binding (p < 0.05) and had diminished activity in inhibiting platelet adhesion to vWF under high shear flow (p < 0.01). Levels of nβ2GPI were increased in patients with primary APS compared to patients with either secondary APS (p < 0.05), autoimmune disease without APS (p < 0.05) or non-autoimmune patients with arterial thrombosis (p < 0.01) and healthy individuals (p < 0.05).In conclusion tyrosine nitration of plasma β2GPI is demonstrated and has important implications with regards to the pathophysiology of platelet mediated thrombosis in APS. Elevated plasma levels of nβ2GPI in primary APS may be a risk factor for thrombosis warranting further investigation. © 2021 Elsevier Ltd

Published
2021

25. Oxidation of beta 2-glycoprotein I associates with IgG antibodies to domain I in patients with antiphospholipid syndrome

Author

Raimondo, MG, Pericleous, C, Radziszewska, A, Borghi, MO, Pierangeli, S, Meroni, PL, Giles, I, Rahman, A, and Ioannou, Y

Subjects
BETA(2)-GLYCOPROTEIN I, Adult, Male, Science & Technology, General Science & Technology, PATHOGENESIS, Enzyme-Linked Immunosorbent Assay, Middle Aged, Antiphospholipid Syndrome, CLASSIFICATION, Multidisciplinary Sciences, beta 2-Glycoprotein I, Immunoglobulin G, BINDING, MD Multidisciplinary, Science & Technology - Other Topics, CRITERIA, Humans, Female, Oxidation-Reduction, PATHOGENICITY, Autoantibodies
Abstract

Domain I (DI) of beta-2-glycoprotein I (β2GPI) contains the immunodominant epitope for pathogenic antiphospholipid antibodies (aPL). DI is exposed in the linear form of the molecule but not in the circular form that comprises 90% of serum β2GPI. The majority of circulating β2GPI is biochemically reduced with two free thiols in Domain V. However, increased levels of oxidised β2GPI are found in patients with antiphospholipid syndrome (APS). It is not known whether oxidation of β2GPI favours the linear form of the molecule and thus promotes development of anti-DI antibodies. We investigated whether the proportion of oxidised β2GPI associates with the presence of anti-DI in APS patients. Serum samples from 44 APS patients were screened for IgG, IgM and IgA anti-DI, anti-β2GPI, anti-cardiolipin (anti-CL) and biochemically reduced β2GPI. A negative correlation was found between the proportion of β2GPI in the biochemically reduced form and IgG anti-DI levels (r = -0.54, p = 0.0002), but not with IgM or IgA anti-DI. Moreover, the proportion of β2GPI in the reduced form was lower in IgG anti-DI positive than anti-DI negative APS patients (p = 0.02). The relative amount of reduced β2GPI was no different between patients who were positive or negative for IgG, IgM and IgA anti-β2GPI or anti-CL. This study demonstrates that oxidised β2GPI lacking free cysteine-thiol groups most closely associates with IgG anti-DI positivity compared to IgG anti-CL and anti-β2GPI. Future studies are required to ascertain the directionality of this association to define causation.

Published
2017

26. Evaluation of the ACR and SLICC classification criteria in juvenile-onset systemic lupus erythematosus: a longitudinal analysis

Author

Lythgoe, H, Morgan, T, Heaf, E, Lloyd, O, Al-Abadi, E, Armon, K, Bailey, K, Davidson, J, Friswell, M, Gardner-Medwin, J, Haslam, K, Ioannou, Y, Leahy, A, Leone, V, Pilkington, C, Rangaraj, S, Riley, P, Tizard, EJ, Wilkinson, N, Beresford, MW, and Grp, UKJSLE Study

Subjects
Male, medicine.medical_specialty, Pediatrics, Adolescent, National cohort, Disease course, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Rheumatology, Internal medicine, medicine, Humans, Lupus Erythematosus, Systemic, 030212 general & internal medicine, Longitudinal Studies, Stage (cooking), Age of Onset, Child, 030203 arthritis & rheumatology, business.industry, Clinical trial, Juvenile onset, Child, Preschool, Physical therapy, Observational study, Female, business, Cohort study, Follow-Up Studies
Abstract

Objectives The Systemic Lupus International Collaborating Clinics (SLICC) group proposed revised classification criteria for systemic lupus erythematosus (SLICC-2012 criteria). This study aimed to compare these criteria with the well-established American College of Rheumatology classification criteria (ACR-1997 criteria) in a national cohort of juvenile-onset systemic lupus erythematosus (JSLE) patients and evaluate how patients’ classification criteria evolved over time. Methods Data from patients in the UK JSLE Cohort Study with a senior clinician diagnosis of probable evolving, or definite JSLE, were analyzed. Patients were assessed using both classification criteria within 1 year of diagnosis and at latest follow up (following a minimum 12-month follow-up period). Results A total of 226 patients were included. The SLICC-2012 was more sensitive than ACR-1997 at diagnosis (92.9% versus 84.1% p Conclusions The SLICC-2012 was better able to classify patients with JSLE than the ACR-1997 and did so at an earlier stage in their disease course. SLICC-2012 should be considered for classification of JSLE patients in observational studies and clinical trial eligibility.

Published
2017

27. Notifications for child safeguarding from an acute hospital in response to presentations to healthcare by parents

Author

Gonzalez-Izquierdo, A, Ward, A, Smith, P, Walford, C, Begent, J, Ioannou, Y, and Gilbert, R

Subjects
Family Health, Male, Parents, Social Work, child safeguarding, Adolescent, victimization, Child Welfare, Original Articles, Hospitals, General, social care, humanities, Cross-Sectional Studies, Child of Impaired Parents, London, Humans, Female, Child Abuse, paediatric emergency, Child, Emergency Service, Hospital, child maltreatment, Referral and Consultation
Abstract

Background Consideration of child safeguarding is routine within maternity services but less common in other health services for adults. We audited notifications for child safeguarding from an acute general hospital where the policy includes questioning adults presenting with violence, mental health problems or drug or alcohol misuse to any department within the hospital about children at home and notifying to the local authority children's social care services if there are safeguarding concerns. Methods Cross-sectional audit of notifications for child safeguarding, including abuse, neglect or victimization, from all departments in one hospital to the local authority children's social care department during 12 months (2010/11). Results Of 681 notifications (57 per month), 40% (270/681) were triggered by parents' presentation to acute hospital services. Of these, 37% (100/270; 12 teenage mothers) presented for maternity care and 60% (162/270; 8 teenage parents) presented to the emergency department (ED). Of the 60% (411/681) of notifications prompted by children presenting for healthcare, most originated from the ED (358/411; 87%): two-thirds of these presented with injury (250/358; 70%). Conclusion Given a policy to ask adults about children at home, a substantial proportion of children notified for child safeguarding were recognized through presentations to acute healthcare by their parents. Further research and development of this policy needs to ensure that questioning results in effective interventions for the children and their parents.

Published
2014

32. Measuring IgA anti-beta 2-Glycoprotein I and IgG/IgA anti-domain I antibodies adds value to current serological assays for the antiphospholipid syndrome

Author

Pericleous, C, Ferreira, I, Borghi, O, Pregnolato, F, McDonnell, T, Garza-Garcia, A, Driscoll, P, Pierangeli, S, Isenberg, D, Ioannou, Y, Giles, I, Meroni, PL, and Rahman, A

Subjects
Adult, Male, General Science & Technology, Enzyme-Linked Immunosorbent Assay, Epitopes, Pregnancy, BETA2-GLYCOPROTEIN I, MD Multidisciplinary, Humans, Serologic Tests, SYSTEMIC-LUPUS-ERYTHEMATOSUS, BETA(2)-GLYCOPROTEIN I, REVISED CRITERIA, Science & Technology, ANTICARDIOLIPIN ANTIBODIES, Thrombosis, Middle Aged, Antiphospholipid Syndrome, PROOF-OF-CONCEPT, Immunoglobulin A, Multidisciplinary Sciences, beta 2-Glycoprotein I, Antibodies, Anticardiolipin, Immunoglobulin G, INTERNATIONAL-CONGRESS, SYNDROME APS, Antibodies, Antiphospholipid, Science & Technology - Other Topics, AUTOANTIBODIES, Female, GLYCOPROTEIN-I
Abstract

Introduction Currently available clinical assays to detect antiphospholipid antibodies (aPL) test for IgG and IgM antibodies to cardiolipin (aCL) and β2-glycoprotein I (aβ2GPI). It has been suggested that testing for IgA aPL and for antibodies to Domain I (DI), which carries the key antigenic epitopes of β2GPI, could add value to these current tests. We performed an observational, multicenter cohort study to evaluate the utility of IgG, IgM and IgA assays to each of CL, β2GPI and DI in APS. Methods Serum from 230 patients with APS (n = 111), SLE but not APS (n = 119), and 200 healthy controls were tested for IgG, IgM and IgA aCL, aβ2GPI and aDI activity. Patients with APS were further classified into thrombotic or obstetric APS. Logistic regression and receiver operator characteristic analyses were employed to compare results from the nine different assays. Results All assays displayed good specificity for APS; IgG aCL and IgG aβ2GPI assays however, had the highest sensitivity. Testing positive for IgA aβ2GPI resulted in a higher hazard ratio for APS compared to IgM aβ2GPI. Positive IgG, IgM or IgA aDI were all associated with APS, and in subjects positive for aCL and/or aβ2GPI, the presence of aDI raised the hazard ratio for APS by 3–5 fold. IgG aCL, aβ2GPI, aDI and IgA aDI were associated with thrombotic but not obstetric complications in patients with APS. Conclusion Measuring IgG aDI and IgA aβ2GPI and aDI may be useful in the management of patients with APS, particularly thrombotic APS.

Published
2016

33. Training CNNs with Low-Rank Filters for Efficient Image Classification

Author

Ioannou, Y., Robertson, D., Shotton, J., Roberto Cipolla, and Criminisi, A.

Subjects
FOS: Computer and information sciences, 0209 industrial biotechnology, Low-Rank, Neural Networks, Computer Vision and Pattern Recognition (cs.CV), Computer Vision, Computer Science - Computer Vision and Pattern Recognition, Computer Science - Neural and Evolutionary Computing, 02 engineering and technology, Machine Learning (cs.LG), Computer Science - Learning, 020901 industrial engineering & automation, Deep Learning, 0202 electrical engineering, electronic engineering, information engineering, 020201 artificial intelligence & image processing, Neural and Evolutionary Computing (cs.NE)
Abstract

We propose a new method for creating computationally efficient convolutional neural networks (CNNs) by using low-rank representations of convolutional filters. Rather than approximating filters in previously-trained networks with more efficient versions, we learn a set of small basis filters from scratch; during training, the network learns to combine these basis filters into more complex filters that are discriminative for image classification. To train such networks, a novel weight initialization scheme is used. This allows effective initialization of connection weights in convolutional layers composed of groups of differently-shaped filters. We validate our approach by applying it to several existing CNN architectures and training these networks from scratch using the CIFAR, ILSVRC and MIT Places datasets. Our results show similar or higher accuracy than conventional CNNs with much less compute. Applying our method to an improved version of VGG-11 network using global max-pooling, we achieve comparable validation accuracy using 41% less compute and only 24% of the original VGG-11 model parameters; another variant of our method gives a 1 percentage point increase in accuracy over our improved VGG-11 model, giving a top-5 center-crop validation accuracy of 89.7% while reducing computation by 16% relative to the original VGG-11 model. Applying our method to the GoogLeNet architecture for ILSVRC, we achieved comparable accuracy with 26% less compute and 41% fewer model parameters. Applying our method to a near state-of-the-art network for CIFAR, we achieved comparable accuracy with 46% less compute and 55% fewer parameters., Published as a conference paper at ICLR 2016. v3: updated ICLR status. v2: Incorporated reviewer's feedback including: Amend Fig. 2 and 5 descriptions to explain that there are no ReLUs within the figures. Fix headings of Table 5 - Fix typo in the sentence at bottom of page 6. Add ref. to Predicting Parameters in Deep Learning. Fix Table 6, GMP-LR and GMP-LR-2x had incorrect numbers of filters

Published
2016
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38. Evaluation of the ACR and SLICC classification criteria in juvenile-onset systemic lupus erythematosus: a longitudinal analysis

Author

Lythgoe, H, primary, Morgan, T, additional, Heaf, E, additional, Lloyd, O, additional, Al-Abadi, E, additional, Armon, K, additional, Bailey, K, additional, Davidson, J, additional, Friswell, M, additional, Gardner-Medwin, J, additional, Haslam, K, additional, Ioannou, Y, additional, Leahy, A, additional, Leone, V, additional, Pilkington, C, additional, Rangaraj, S, additional, Riley, P, additional, Tizard, E J, additional, Wilkinson, N, additional, and Beresford, M W, additional

Published
2017
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39. Purified IgG from patients with obstetric but not IgG from non-obstetric antiphospholipid syndrome inhibit trophoblast invasion

Author

Poulton, K, Ripoll, VM, Pericleous, C, Meroni, PL, Gerosa, M, Ioannou, Y, Rahman, A, and Giles, IP

Subjects
Adult, Immunology, MULTICENTER, TLR4/MYD88, Antiphospholipid, Cell Line, SIGNALING PATHWAYS, FACTOR EXPRESSION, DOMAIN, Pregnancy, obstetric, 1114 Paediatrics And Reproductive Medicine, Humans, TLR4, SYSTEMIC-LUPUS-ERYTHEMATOSUS, Obstetrics & Reproductive Medicine, Reproductive Biology, Science & Technology, 1103 Clinical Sciences, 1ST TRIMESTER TROPHOBLAST, Antiphospholipid Syndrome, trophoblast, Trophoblasts, Pregnancy Complications, MONOCYTES, 1107 Immunology, Immunoglobulin G, ANTIBODIES, HEPARIN, Antibodies, Antiphospholipid, Female, Life Sciences & Biomedicine
Abstract

Problem Some patients with antiphospholipid syndrome (APS) suffer pregnancy morbidity (PM) but not vascular thrombosis (VT), whilst others suffer VT only. Therefore, we compared the effects of IgG from VT+/PM− and VT−/PM+ subjects on human first‐trimester trophoblast (HTR8) cells. Method of study HTR‐8 cells were incubated with APS VT+/PM−, APS VT−/PM+ or healthy control (HC) IgG. We measured trophoblast invasion by cell invasion assay; mRNA expression of TLR4 and adaptor proteins; phosphorylation of p38 MAPK, NFκB and ERK; and expression of interleukin (IL)‐8 and IL‐6. Results VT−/PM+ IgG, but not VT+/PM− IgG significantly reduced HTR‐8 invasion. The effects on invasion were blocked by TLR‐4 inhibition. Neither VT+/PM− nor VT−/PM+ IgG altered MyD88 mRNA expression, phosphorylation of signalling molecules or cytokine expression. Conclusions VT−/PM+ IgG exert functionally relevant effects on human trophoblast cells but VT+/PM− IgG do not.

Published
2014

40. Proof-of-concept study demonstrating the pathogenicity of affinity-purified IgG antibodies directed to domain I of beta(2)-glycoprotein I in a mouse model of anti-phospholipid antibody-induced thrombosis

Author

Pericleous, C, Ruiz-Limon, P, Romay-Penabad, Z, Marin, AC, Garza-Garcia, A, Murfitt, L, Driscoll, PC, Latchman, DS, Isenberg, DA, Giles, I, Ioannou, Y, Rahman, A, and Pierangeli, SS

Subjects
Male, mouse model, anti-phospholipid antibodies, EPITOPE, Mice, Rheumatology, BINDING, beta(2)-glycoprotein I, Animals, PEPTIDE, Science & Technology, β2-glycoprotein I, Thrombosis, 1103 Clinical Sciences, Antiphospholipid Syndrome, Protein Structure, Tertiary, Arthritis & Rheumatology, anti-phospholipid syndrome, Disease Models, Animal, 1117 Public Health And Health Services, domain I, beta 2-Glycoprotein I, 1107 Immunology, Immunoglobulin G, Antibodies, Antiphospholipid, AUTOANTIBODIES, venous thrombosis, Life Sciences & Biomedicine, GLYCOPROTEIN-I
Abstract

Objective. IgG aPL against domain I of β2-glycoprotein I (β2GPI) [anti-DI (aDI)] is associated with the pathogenesis of APS, an autoimmune disease defined by thrombosis and pregnancy morbidity. To date, however, no study has demonstrated direct pathogenicity of IgG aDI in vivo. In this proof-of-concept study, we designed a novel system to affinity purify polyclonal aDI aPL in order to assess its prothrombotic ability in a well-characterized mouse microcirculation model for APS. Methods. Two polyclonal IgG fractions were isolated from serum of a patient with APS, both with high aPL activity but differing in aDI activity (aDI-rich and aDI-poor). These IgG fractions were tested for their pathogenic ability in an in vivo mouse model of thrombosis. Male CD1 mice were injected intraperitoneally with either aDI-rich or aDI-poor IgG; as a control, IgG isolated from healthy serum was used. A pinch injury was applied to the right femoral vein and thrombus dynamics and tissue factor activity in isolated tissue were evaluated. Results. Both aDI-rich and aDI-poor IgG retained aCL and anti-β2GPI activity, while only aDI-rich IgG displayed high aDI activity, as defined by our in-house cut-offs for positivity in each assay. aDI-rich IgG induced significantly larger thrombi in vivo compared with aDI-poor IgG (P < 0.0001). Similarly, aDI-rich IgG significantly enhanced the procoagulant activity of carotid artery endothelium and peritoneal macrophages isolated from experimental animals (P < 0.01). Conclusion. These data directly demonstrate that the ability to cause thrombosis in vivo is concentrated in the aDI fraction of aPL.

Published
2014

44. Novel assays of thrombogenic pathogenicity in the antiphospholipid syndrome based on the detection of molecular oxidative modification of the major autoantigen β2-glycoprotein i

Author

Ioannou, Y. Zhang, J.-Y. Qi, M. Gao, L. Qi, J.C. Yu, D.-M. Lau, H. Sturgess, A.D. Vlachoyiannopoulos, P.G. Moutsopoulos, H.M. Rahman, A. Pericleous, C. Atsumi, T. Koike, T. Heritier, S. Giannakopoulos, B. Krilis, S.A.

Abstract

Objective Beta-2-glycoprotein I (β2GPI) constitutes the major autoantigen in the antiphospholipid syndrome (APS), a common acquired cause of arterial and venous thrombosis. We recently described the novel observation that β2GPI may exist in healthy individuals in a free thiol (biochemically reduced) form. The present study was undertaken to quantify the levels of total, reduced, and posttranslationally modified oxidized β2GPI in APS patients compared to various control groups. Methods In a retrospective multicenter analysis, the proportion of β2GPI with free thiols in serum from healthy volunteers was quantified. Assays for measurement of reduced as well as total circulating β2GPI were developed and tested in the following groups: APS (with thrombosis) (n = 139), autoimmune disease with or without persistent antiphospholipid antibodies (aPL) but without APS (n = 188), vascular thrombosis without APS or aPL (n = 38), and healthy volunteers (n = 91). Results Total β2GPI was significantly elevated in patients with APS (median 216.2 μg/ml [interquartile range 173.3-263.8]) as compared to healthy subjects (median 178.4 μg/ml [interquartile range 149.4-227.5] [P < 0.0002]) or control patients with autoimmune disease or vascular thrombosis (both P < 0.0001). The proportion of total β2GPI in an oxidized form (i.e., lacking free thiols) was significantly greater in the APS group than in each of the 3 control groups (all P < 0.0001). Conclusion This large retrospective multicenter study shows that posttranslational modification of β2GPI via thiol-exchange reactions is a highly specific phenomenon in the setting of APS thrombosis. Quantification of posttranslational modifications of β2GPI in conjunction with standard laboratory tests for APS may offer the potential to more accurately predict the risk of occurrence of a thrombotic event in the setting of APS. Copyright © 2011 by the American College of Rheumatology.

Published
2011

47. Epidemiology of severe Streptococcus pyogenes disease in Europe

Author

Lamagni, T.L. Darenberg, J. Luca-Harari, B. Siljander, T. Efstratiou, A. Henriques-Normark, B. Vuopio-Varkila, J. Bouvet, A. Creti, R. Ekelund, K. Koliou, M. Reinert, R.R. Stathi, A. Strakova, L. Ungureanu, V. Schalén, C. Jasir, A. Ioannou, Y. Kriz, P. Motlova, J. Hammerum, A. Kaltoft, M.S. Iivonen, J. Loubinoux, J. Mihaila, L. Van Der Linden, M. Lütticken, R. Papaparaskevas, J. Zachariadou, L. Baldassarri, L. Orefici, G. Straut, M. Norrby-Teglund, A. Keshishian, C. Neal, S.

Abstract

The past 2 decades have brought worrying increases in severe Streptococcus pyogenes diseases globally. To investigate and compare the epidemiological patterns of these diseases within Europe, data were collected through a European Union FP-5-funded program (Strep-EURO). Prospective population-based surveillance of severe S. pyogenes infection diagnosed during 2003 and 2004 was undertaken in 11 countries across Europe (Cyprus, the Czech Republic, Denmark, Finland, France, Germany, Greece, Italy, Romania, Sweden, and the United Kingdom) using a standardized case definition. A total of 5,522 cases were identified across the 11 countries during this period. Rates of reported infection varied, reaching 3/100,000 population in the northern European countries. Seasonal patterns of infection showed remarkable congruence between countries. The risk of infection was highest among the elderly, and rates were higher in males than in females in most countries. Skin lesions/wounds were the most common predisposing factor, reported in 25% of cases; 21% had no predisposing factors reported. Skin and soft tissue were the most common foci of infection, with 32% of patients having cellulitis and 8% necrotizing fasciitis. The overall 7-day case fatality rate was 19%; it was 44% among patients who developed streptococcal toxic shock syndrome. The findings from Strep-EURO confirm a high incidence of severe S. pyogenes disease in Europe. Furthermore, these results have identified targets for public health intervention, as well as raising awareness of severe S. pyogenes disease across Europe. Copyright © 2008, American Society for Microbiology. All Rights Reserved.

Published
2008

49. Review of presentations at the 6th European Lupus Meeting 3-5 March 2005

Author

Ioannou, Y., Bowman, S. J., Rahman, A., and Giles, I. P.

Subjects
immune system diseases, Animals, Apoptosis, Arteriosclerosis, Autoantibodies, Autoantigens, Biomarkers, Complement System Proteins, Cytokines, Europe, Humans, Interferons, Lupus Erythematosus, Systemic, Lupus Nephritis, Polymorphism, Genetic, Research Design, Signal Transduction, skin and connective tissue diseases
Abstract

The 6th European Lupus Meeting was held at the Royal College of Physicians of London and was attended by 450 delegates. The conference brought together leading speakers from Europe and North America who reviewed current knowledge and exciting new developments in both clinical and basic science aspects of systemic lupus erythematosus. This review summarizes the major points covered in each session.

Published
2005

50. Proof-of-concept study demonstrating the pathogenicity of affinity-purified IgG antibodies directed to domain I of 2-glycoprotein I in a mouse model of anti-phospholipid antibody-induced thrombosis

Author

Pericleous, C., primary, Ruiz-Limon, P., additional, Romay-Penabad, Z., additional, Marin, A. C., additional, Garza-Garcia, A., additional, Murfitt, L., additional, Driscoll, P. C., additional, Latchman, D. S., additional, Isenberg, D. A., additional, Giles, I., additional, Ioannou, Y., additional, Rahman, A., additional, and Pierangeli, S. S., additional

Published
2014
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