Your search keyword '"Pilkington, Clarissa A."' showing total 20 results

1. Experience with the use of mycophenolate mofetil in juvenile idiopathic inflammatory myopathies.

Author

Varnier, Giulia Camilla, Consolaro, Alessandro, Cheng, Iek Leng, Riveiro, Alicia Silva, Pilkington, Clarissa, and Ravelli, Angelo

Subjects

DRUG efficacy, SKIN diseases, KRUSKAL-Wallis Test, MYCOPHENOLIC acid, RETROSPECTIVE studies, VISUAL analog scale, FISHER exact test, SEVERITY of illness index, MUSCLE strength, DESCRIPTIVE statistics, CHI-squared test, MYOSITIS, DATA analysis software, LONGITUDINAL method, DRUG administration, DRUG dosage, THERAPEUTICS, CHILDREN, ADOLESCENCE

Abstract

Objective The objective of this study was to evaluate the efficacy and safety of MMF in juvenile idiopathic inflammatory myopathies (JIIMs). Methods Patients diagnosed with JIIM and treated with MMF enrolled in the Juvenile Dermatomyositis Research Group (JDRG) in the UK or followed at the Giannina Gaslini Institute in Genoa, Italy, were included. The following information was collected retrospectively at MMF initiation, at 3, 6 and 12 months after treatment start, and at last follow-up visit: clinical manifestations, laboratory data, physicians' subjective assessment of disease activity, standardized outcome measures of muscle strength/endurance, cutaneous disease activity, physical function, global disease activity, cumulative damage, and ongoing treatment. Results Of the 29 patients included, 23 had juvenile DM and 6 had overlap myositis. During administration of MMF, improvement in measures of muscle strength, skin disease activity, and overall disease activity was seen, with an increase in the frequency of normal scores for Manual Muscle Test-8 from 50.0% to 83.3%, Childhood Myositis Activity Score from 53.5% to 88.9%, muscle component of DAS from 55.2% to 84.2%, skin component of DAS from 31.0% to 42.1%, visual analogue scale for skin disease activity from 25.0% to 47.4%, and visual analogue scale for overall disease activity from 7.1% to 42.1%. The number of patients with inactive disease increased from 10.3% at baseline to 68.5% at last follow-up. CS dose was significantly reduced, from 0.3 to 0.1 mg/kg/day. No relevant side effects were reported. Conclusion Our experience suggests that MMF is a valuable therapeutic option for the management of JIIM. [ABSTRACT FROM AUTHOR]

Published

2023

2. Prospective epidemiological study of juvenile-onset systemic lupus erythematosus in the UK and Republic of Ireland.

Author

Lythgoe, Hanna, Smith, Eve M D, Killeen, Orla G, Murphy, Ruth, Pilkington, Clarissa, Pain, Clare E, Beresford, Michael W, and Unit, in association with the British Paediatric Surveillance

Subjects

SYSTEMIC lupus erythematosus diagnosis, DISEASE progression, PEDIATRICS, DISEASE incidence, IMMUNOMODULATORS, DESCRIPTIVE statistics, AGE factors in disease, SYSTEMIC lupus erythematosus, LONGITUDINAL method, EPIDEMIOLOGICAL research, SYMPTOMS, DISEASE complications, CHILDREN, ADOLESCENCE

Abstract

Objectives The primary objective was to define the incidence of JSLE in children <16 years of age in the UK and Republic of Ireland (ROI). The secondary objective was to describe presenting features, classification criteria, initial management and disease damage in newly presenting JSLE patients. Methods A prospective JSLE epidemiological study was undertaken between September 2017 and September 2019 with support of the British Paediatric Surveillance Unit and other professional groups involved in diagnosis and management of JSLE patients. Treating consultants reported all cases of JSLE seen. A follow-up study at 1 year examined management and progression of disease and treatment. Results There were 124 incident cases included in the final analysis. Incidence was estimated using ACR-1997 classification criteria (0.36/100 000), SLICC-2012 classification criteria (0.41/100 000) and clinician expert opinion (0.46/100 000). A high disease burden was seen, with 71.0% of patients requiring ongoing systemic CS treatment at 1 year; 98.2% receiving immunomodulatory treatment; and 20.4% accruing damage in the year following diagnosis (predominantly neuropsychiatric-related), with substantial involvement from multiple speciality teams. Conclusions The minimum UK and ROI incidence of JSLE is between 0.36 and 0.46/100 000, depending on the case definition used. Challenges in classification of patients with JSLE are highlighted, but overall this study supports the use of SLICC-2012 classification criteria. The high levels of disease damage and ongoing CS use 1 year after diagnosis is concerning, highlighting the need for further interventions to improve outcomes in JSLE. [ABSTRACT FROM AUTHOR]

Published

2022

3. British Society for Rheumatology guideline on management of paediatric, adolescent and adult patients with idiopathic inflammatory myopathy.

Author

Oldroyd, Alexander G S, Lilleker, James B, Amin, Tania, Aragon, Octavio, Bechman, Katie, Cuthbert, Verna, Galloway, James, Gordon, Patrick, Gregory, William J, Gunawardena, Harsha, Hanna, Michael G, Isenberg, David, Jackman, John, Kiely, Patrick D W, Livermore, Polly, Machado, Pedro M, Maillard, Sue, McHugh, Neil, Murphy, Ruth, and Pilkington, Clarissa

Subjects

CARDIOVASCULAR disease treatment, BONE fracture prevention, AUTOIMMUNE disease treatment, AUTOANTIBODY analysis, CARDIOVASCULAR disease diagnosis, GLUCOCORTICOIDS, RITUXIMAB, THERAPEUTICS, WELL-being, COMBINATION drug therapy, DEGLUTITION, RHEUMATOLOGY, SUNSHINE, INTERSTITIAL lung diseases, CUTANEOUS manifestations of general diseases, MEDICAL screening, EARLY detection of cancer, DEGLUTITION disorders, MEDICAL protocols, ANTIRHEUMATIC agents, HEALTH behavior, QUALITY of life, MYOSITIS, IMMUNOSUPPRESSIVE agents, DISEASE management, EXERCISE therapy, DISEASE complications, CHILDREN, ADULTS, ADOLESCENCE

Abstract

The article presents a guideline from the British Society for Rheumatology for the management of patients with idiopathic inflammatory myopathy (IIM) in the United Kingdom (UK). The guideline used the Appraisal of Guidelines for Research and Evaluation II (AGREEII) methodology. The guideline includes treatment for diseases like skeletal muscle inflammation (myositis).

Published

2022

4. Limited sensitivity and specificity of the ACR/EULAR-2019 classification criteria for SLE in JSLE?—observations from the UK JSLE Cohort Study.

Author

Smith, Eve M D, Rasul, Sajida, Ciurtin, Coziana, Al-Abadi, Eslam, Armon, Kate, Bailey, Kathryn, Brennan, Mary, Gardner-Medwin, Janet, Haslam, Kirsty, Hawley, Daniel P, Lane, Steven, Leahy, Alice, Leone, Valentina, Malik, Gulshan, Mewar, Devesh, Moots, Robert, Pilkington, Clarissa, Ramanan, Athimalaipet V, Rangaraj, Satyapal, and Ratcliffe, Annie

Subjects

SYSTEMIC lupus erythematosus diagnosis, PREDICTIVE tests, CONFIDENCE intervals, AGE factors in disease, DESCRIPTIVE statistics, SYSTEMIC lupus erythematosus, ODDS ratio, MEDICAL appointments, LONGITUDINAL method, CHILDREN

Abstract

Objectives This study aimed to test the performance of the new ACR and EULAR criteria, that include ANA positivity as entry criterion, in JSLE. Methods Performance of the ACR/EULAR-2019 criteria were compared with Systemic Lupus International Collaborating Clinics (SLICC-2012), using data from children and young people (CYP) in the UK JSLE Cohort Study (n  = 482), with the ACR-1997 criteria used as reference standard. An unselected cohort of CYP positive for ANA (n  = 129) was used to calculate positive/negative predictive values of the criteria. Results At both first and last visits, the number of patients fulfilling the different classification criteria varied significantly (P < 0.001). The sensitivity of the SLICC-2012 criteria was higher when compared with that of the ACR/EULAR-2019 criteria at first and last visits (98% vs 94% for first visit, and 98% vs 96% for last visit; P < 0.001), when all available CYP were considered. The ACR/EULAR-2019 criteria were more specific when compared with the SLICC-2012 criteria (77% vs 67% for first visit, and 81% vs 71% for last visit; P < 0.001). Significant differences between the classification criteria were mainly caused by the variation in ANA positivity across ages. In the unselected cohort of ANA-positive CYP, the ACR/EULAR-2019 criteria produced the highest false-positive classification (6/129, 5%). Conclusion In CYP, the ACR/EULAR-2019 criteria are not superior to those of the SLICC-2012 or ACR-1997 criteria. If classification criteria are designed to include CYP and adult populations, paediatric rheumatologists should be included in the consensus and evaluation process, as seemingly minor changes can significantly affect outcomes. [ABSTRACT FROM AUTHOR]

Published

2021

5. Comparison of treatments and outcomes of children with juvenile dermatomyositis followed at two European tertiary care referral centers.

Author

Varnier, Giulia Camilla, Consolaro, Alessandro, Maillard, Susan, Pilkington, Clarissa, and Ravelli, Angelo

Subjects

THERAPEUTIC use of immunoglobulins, RITUXIMAB, DERMATOMYOSITIS, ACQUISITION of data methodology, AZATHIOPRINE, PEDIATRICS, TERTIARY care, RETROSPECTIVE studies, INFLIXIMAB, MYCOPHENOLIC acid, MANN Whitney U Test, FISHER exact test, TREATMENT effectiveness, CYCLOSPORINE, MEDICAL records, CYCLOPHOSPHAMIDE, DESCRIPTIVE statistics, HYDROXYCHLOROQUINE, DATA analysis software, THERAPEUTICS, CHILDREN

Abstract

Objectives To compare the treatment approaches and disease outcomes of children with JDM followed in two European tertiary care peadiatric rheumatology centres. Methods The medical notes of patients with JDM seen at Istituto Giannina Gaslini (IGG) of Genoa, Italy or Great Ormond Street Hospital (GOSH) of London, UK between January 2000 and December 2015 within 6 months after disease onset and followed for at least 6 months were reviewed. Demographic, clinical and therapeutic data were collected. At each visit, the caring physician was asked to rate the disease state subjectively. Results A total of 127 patients were included, 88 at GOSH and 39 at IGG. At 24 months, the median values of muscle strength and disease activity were at the normal end of the scale and around three quarters of patients were said to have inactive disease. Also, at 2 years, 38.6% and 36% of British and Italian patients, respectively, had damage. Cyclophosphamide, azathioprine, infliximab, rituximab and mycophenolate mofetil were used more frequently by UK physicians, whereas ciclosporin, intravenous immunoglobulin and hydroxychloroquine were prescribed by Italian physicians. Conclusion This study shows a significant difference in the choice of medications between pediatric rheumatologists practising in the two centres. Despite this, a high proportion of patients had inactive disease at 2 years and there was a low frequency of damage: modern treatments have improved outcomes. [ABSTRACT FROM AUTHOR]

Published

2021

6. The Vasculopathy of Juvenile Dermatomyositis: Endothelial Injury, Hypercoagulability, and Increased Arterial Stiffness.

Author

Papadopoulou, Charalampia, Hong, Ying, Krol, Petra, Al Obaidi, Muthana, Pilkington, Clarissa, Wedderburn, Lucy R., Brogan, Paul A., and Eleftheriou, Despina

Subjects

VASCULAR disease diagnosis, BIOMARKERS, ENDOTHELIAL cells, FLOW cytometry, CYTOKINES, BLOOD pressure, NONPARAMETRIC statistics, CAROTID artery, DERMATOMYOSITIS, ENDOTHELIUM, INFLAMMATION, CHEMILUMINESCENCE assay, BLOOD platelets, ARTERIAL diseases, BLOOD diseases, DESCRIPTIVE statistics, DISEASE duration, RADIAL artery, CHEMOKINES, VASCULAR diseases, LONGITUDINAL method, THROMBIN, DISEASE complications, CHILDREN, ADOLESCENCE

Abstract

Objective: Vasculopathy is considered central to the pathogenesis of juvenile dermatomyositis (DM) and is associated with severe extramuscular manifestations. We undertook this study to investigate the hypothesis that the vasculopathy of juvenile DM can be noninvasively tracked by examining biomarkers of endothelial injury, subclinical inflammation, hypercoagulability, and vascular arterial stiffness. Methods: The study population was a UK cohort of children with juvenile DM. Circulating endothelial cells (CECs) and microparticles (MPs) were identified using immunomagnetic bead extraction and flow cytometry, respectively. Plasma thrombin generation was determined using a fluorogenic assay. Cytokine and chemokine levels were measured by electrochemiluminescence. Arterial stiffness was assessed using pulse wave velocity (PWV). Results were expressed as the median and interquartile range (IQR), and statistical significance was assessed using nonparametric analyses. Results: Ninety patients with juvenile DM and 79 healthy control subjects were included. The median age of the patients was 10.21 years (IQR 6.68–13.40), and the median disease duration was 1.63 years (IQR 0.28–4.66). CEC counts were higher in all patients with juvenile DM compared to controls (median 96 cells/ml [IQR (40–192] and 12 cells/ml [IQR 8–24], respectively; P < 0.0001). Circulating MP numbers were also significantly higher in patients with active juvenile DM compared to controls (median 204.7 × 103/ml [IQR 87.9–412.6] and 44.3 × 103/ml [IQR 15.0–249.1], respectively; P < 0.0001). MPs were predominantly of platelet and endothelial origin. Enhanced plasma thrombin generation was demonstrated in patients with active juvenile DM compared to those with inactive disease (P = 0.0003) and controls (P < 0.0001). Carotid‐radial PWV adjusted for age was increased in patients with juvenile DM compared to controls (P = 0.003). Conclusion: We observed increased endothelial injury and increased levels of proinflammatory cytokines in patients with active juvenile DM. MP profiles reflected distinct disease activity status in juvenile DM and are markers of vascular pathology, platelet activation, and thrombotic propensity. Ongoing long‐term vascular injury may result in increased arterial stiffness in patients with juvenile DM. [ABSTRACT FROM AUTHOR]

Published

2021

7. Consensus-based recommendations for the management of juvenile systemic sclerosis.

Author

Foeldvari, Ivan, Culpo, Roberta, Sperotto, Francesca, Anton, Jordi, Avcin, Tadej, Baildam, Eileen, Boros, Christina, Chaitow, Jeffrey, Constantin, Tamas, Kasapcopur, Ozgur, Oliveira, Sheila Knupp Feitosa de, Pilkington, Clarissa, Toplak, Natasa, Royen, Annet van, Magalhaes, Claudia Saad, Vastert, Sebastiaan J, Wulffraat, Nico, and Zulian, Francesco

Subjects

CONSENSUS (Social sciences), SYSTEMATIC reviews, SYSTEMIC scleroderma, PEDIATRICS, MEDICAL protocols, SEVERITY of illness index, TREATMENT effectiveness, QUALITY assurance, SYMPTOMS, CHILDREN, ADOLESCENCE

Abstract

Juvenile systemic sclerosis (JSSc) is a rare disease of childhood and currently no international consensus exists with regard to its assessment and treatment. This SHARE (Single Hub and Access point for paediatric Rheumatology in Europe) initiative, based on expert opinion informed by the best available evidence, provides recommendations for the assessment and treatment of patients with JSSc with a view to improving their outcome. Experts focused attention not only on the skin assessment but also on the early signs of internal organ involvement whose proper treatment can significantly affect the long-term outcome. A score for disease severity is proposed in order to perform a structured assessment of outcome over time but a validation in a wider patient population is recommended. Finally, a stepwise treatment approach is proposed in order to unify the standard of care throughout Europe with the aim to reduce morbidity and mortality in this disease. [ABSTRACT FROM AUTHOR]

Published

2021

8. Introduction of a novel magnetic resonance imaging-based scoring system for assessing disease activity in children with juvenile dermatomyositis.

Author

Thyoka, Mandela, Adekunle, Oba, Pilkington, Clarissa, Walters, Stephen, Arthurs, Owen J, Humphries, Paul, Johnson, Karl, Kraft, Jeannette, Landes, Caren, and Persaud, Thara

Subjects

DERMATOMYOSITIS, BIOMARKERS, CONFIDENCE intervals, EXTREMITIES (Anatomy), MAGNETIC resonance imaging, RADIOLOGISTS, RELIABILITY (Personality trait), RESEARCH evaluation, INTER-observer reliability, SEVERITY of illness index, INTRACLASS correlation, CHILDREN, DIAGNOSIS, THERAPEUTICS

Abstract

Objectives We aimed to develop and assess the reliability of a novel MRI-based scoring system for reporting the severity of MRI findings in children with suspected JDM. Methods Nine consultant paediatric radiologists independently assessed and scored 40 axial and 30 coronal thigh MR images of children with suspected JDM on two occasions using the juvenile dermatomyositis magnetic resonance Imaging Score (JIS). JIS was calculated for both reads for each plane and each limb, with possible scores ranging from 0 (normal) to 100 (severe). Inter- and intraobserver agreement was calculated using the intraclass correlation coefficient (ICC) and two- and one-way random effects models, respectively. Bland-Altman plots of the difference in JIS against the average JIS were also produced for each rater. Results Overall, the interobserver reliability and agreement was good—for axial images, JIS ranged from 46.8 to 61.0 [ICC = 0.88 (95% CI: 0.82, 0.92)] for the left limb and 47.9–61.4 [ICC = 0.87 (95% CI: 0.81, 0.92)] for the right limb. For coronal images, JIS ranged from 56.7 to 65.1 [ICC = 0.90 (95% CI: 0.85, 0.95)] for the left limb and 55.7 to 66.8 [ICC = 0.90 (95% CI: 0.84, 0.94)] for the right limb. The intraobserver reliability and agreement was good, with ICC ranging from 0.90 to 0.94. Conclusion JIS is a semi-objective scoring system with potential to serve as a reliable biomarker of disease severity and response to therapeutic interventions in children with JDM. [ABSTRACT FROM AUTHOR]

Published

2018

9. Efficacy and Safety of Cyclophosphamide Treatment in Severe Juvenile Dermatomyositis Shown by Marginal Structural Modeling.

Author

Deakin, Claire T., Campanilho‐Marques, Raquel, Simou, Stefania, Moraitis, Elena, Wedderburn, Lucy R., Pullenayegum, Eleanor, Pilkington, Clarissa A., and the Juvenile Dermatomyositis Research Group

Subjects

SKIN disease prevention, MUSCLE diseases, CYCLOPHOSPHAMIDE, DERMATOMYOSITIS, GLUCOCORTICOIDS, WORLD health, TREATMENT effectiveness, SEVERITY of illness index, STATISTICAL models, CHILDREN, PREVENTION

Abstract

Objective: In patients with severe or refractory juvenile dermatomyositis (DM), second‐line treatments may be required. Cyclophosphamide (CYC) is used to treat some connective tissue diseases, but evidence of its efficacy in juvenile DM is limited. This study was undertaken to describe clinical improvement in juvenile DM patients treated with CYC and model the efficacy of CYC treatment compared to no CYC treatment. Methods: Clinical data on skin, global, and muscle disease for patients recruited to the Juvenile DM Cohort and Biomarker Study were analyzed. Clinical improvement following CYC treatment was described using unadjusted analysis. Marginal structural models (MSMs) were used to model treatment efficacy and adjust for confounding by indication. Results: Compared to the start of CYC treatment, there were reductions at 6, 12, and 24 months in skin disease (P = 1.3 × 10‐10), global disease (P = 2.4 × 10‐8), and muscle disease (P = 8.0 × 10‐10) for 56 patients treated with CYC in unadjusted analysis. Limited evidence suggested a reduction in glucocorticoid dose (P = 0.047) in patients treated with CYC. MSM analysis showed reduced global disease and skin disease in patients who started an ~6‐month course of CYC treatment >12 months ago compared to patients never or not yet treated with CYC. In the treated patients, the modified skin Disease Activity Score for juvenile DM was 1.19 units lower (P = 0.0085) and the physician's global assessment was 0.66 units lower (P = 0.027). Minor adverse events were reported in 3 patients within 1 year of stopping CYC. Conclusion: Our findings indicate that CYC is efficacious with no short‐term side effects. Improvements in skin, global, and muscle disease were observed. Further studies are required to evaluate longer‐term side effects. [ABSTRACT FROM AUTHOR]

Published

2018

10. 2016 American College of Rheumatology/European League Against Rheumatism Criteria for Minimal, Moderate, and Major Clinical Response in Juvenile Dermatomyositis: An International Myositis Assessment and Clinical Studies Group/Paediatric Rheumatology International Trials Organisation Collaborative Initiative

Author

Rider, Lisa G., Aggarwal, Rohit, Pistorio, Angela, Bayat, Nastaran, Erman, Brian, Feldman, Brian M., Huber, Adam M., Cimaz, Rolando, Cuttica, Rubén J., de Oliveira, Sheila Knupp, Lindsley, Carol B., Pilkington, Clarissa A., Punaro, Marilynn, Ravelli, Angelo, Reed, Ann M., Rouster‐Stevens, Kelly, van Royen‐Kerkhof, Annet, Dressler, Frank, Magalhaes, Claudia Saad, and Constantin, Tamás

Subjects

BRAINSTORMING, CLINICAL trials, CONSENSUS (Social sciences), DERMATOMYOSITIS, TEST validity, RESEARCH methodology, MEDICAL needs assessment, SCALE analysis (Psychology), SURVEYS, TREATMENT effectiveness, CHILDREN, THERAPEUTICS

Abstract

Objective To develop response criteria for juvenile dermatomyositis (DM). Methods We analyzed the performance of 312 definitions that used core set measures from either the International Myositis Assessment and Clinical Studies Group (IMACS) or the Paediatric Rheumatology International Trials Organisation (PRINTO) and were derived from natural history data and a conjoint analysis survey. They were further validated using data from the PRINTO trial of prednisone alone compared to prednisone with methotrexate or cyclosporine and the Rituximab in Myositis (RIM) trial. At a consensus conference, experts considered 14 top candidate criteria based on their performance characteristics and clinical face validity, using nominal group technique. Results Consensus was reached for a conjoint analysis-based continuous model with a total improvement score of 0-100, using absolute percent change in core set measures of minimal (≥30), moderate (≥45), and major (≥70) improvement. The same criteria were chosen for adult DM/polymyositis, with differing thresholds for improvement. The sensitivity and specificity were 89% and 91-98% for minimal improvement, 92-94% and 94-99% for moderate improvement, and 91-98% and 85-86% for major improvement, respectively, in juvenile DM patient cohorts using the IMACS and PRINTO core set measures. These criteria were validated in the PRINTO trial for differentiating between treatment arms for minimal and moderate improvement ( P = 0.009-0.057) and in the RIM trial for significantly differentiating the physician's rating for improvement ( P < 0.006). Conclusion The response criteria for juvenile DM consisted of a conjoint analysis-based model using a continuous improvement score based on absolute percent change in core set measures, with thresholds for minimal, moderate, and major improvement. [ABSTRACT FROM AUTHOR]

Published

2017

11. International validation of a urinary biomarker panel for identification of active lupus nephritis in children.

Author

Smith, Eve, Jorgensen, Andrea, Midgley, Angela, Oni, Louise, Goilav, Beatrice, Putterman, Chaim, Wahezi, Dawn, Rubinstein, Tamar, Ekdawy, Diana, Corkhill, Rachel, Jones, Caroline, Marks, Stephen, Newland, Paul, Pilkington, Clarissa, Tullus, Kjell, and Beresford, Michael

Subjects

LUPUS nephritis, BIOMARKERS, CHI-squared test, RESEARCH funding, STATISTICS, LOGISTIC regression analysis, CROSS-sectional method, RECEIVER operating characteristic curves, CHILDREN, DIAGNOSIS

Abstract

Background: Conventional markers of juvenile-onset systemic lupus erythematosus (JSLE) disease activity fail to adequately identify lupus nephritis (LN). While individual novel urine biomarkers are good at detecting LN flares, biomarker panels may improve diagnostic accuracy. The aim of this study was to assess the performance of a biomarker panel to identify active LN in two international JSLE cohorts. Methods: Novel urinary biomarkers, namely vascular cell adhesion molecule-1 (VCAM-1), monocyte chemoattractant protein 1 (MCP-1), lipocalin-like prostaglandin D synthase (LPGDS), transferrin (TF), ceruloplasmin, alpha-1-acid glycoprotein (AGP) and neutrophil gelatinase-associated lipocalin (NGAL), were quantified in a cross-sectional study that included participants of the UK JSLE Cohort Study (Cohort 1) and validated within the Einstein Lupus Cohort (Cohort 2). Binary logistic regression modelling and receiver operating characteristic curve analysis [area under the curve (AUC)] were used to identify and assess combinations of biomarkers for diagnostic accuracy. Results: A total of 91 JSLE patients were recruited across both cohorts, of whom 31 (34 %) had active LN and 60 (66 %) had no LN. Urinary AGP, ceruloplasmin, VCAM-1, MCP-1 and LPGDS levels were significantly higher in those patients with active LN than in non-LN patients [all corrected p values ( p ) < 0.05] across both cohorts. Urinary TF also differed between patient groups in Cohort 2 ( p = 0.001). Within Cohort 1, the optimal biomarker panel included AGP, ceruloplasmin, LPGDS and TF (AUC 0.920 for active LN identification). These results were validated in Cohort 2, with the same markers resulting in the optimal urine biomarker panel (AUC 0.991). Conclusion: In two international JSLE cohorts, urinary AGP, ceruloplasmin, LPGDS and TF demonstrate an 'excellent' ability for accurately identifying active LN in children. [ABSTRACT FROM AUTHOR]

Published

2017

12. Muscle Biopsy Findings in Combination With Myositis-Specific Autoantibodies Aid Prediction of Outcomes in Juvenile Dermatomyositis.

Author

Deakin, Claire T., Yasin, Shireena A., Simou, Stefania, Arnold, Katie A., Tansley, Sarah L., Betteridge, Zoe E., McHugh, Neil J., Varsani, Hemlata, Holton, Janice L., Jacques, Thomas S., Pilkington, Clarissa A., Nistala, Kiran, Wedderburn, Lucy R., Armon, Kate, Ellis‐Gage, Joe, Roper, Holly, Briggs, Vanja, Watts, Joanna, McCann, Liza, and Roberts, Ian

Subjects

DERMATOMYOSITIS, ANALYSIS of variance, AUTOANTIBODIES, BIOMARKERS, BIOPSY, CONFIDENCE intervals, ENZYME-linked immunosorbent assay, FISHER exact test, HISTOLOGICAL techniques, LONGITUDINAL method, RARE diseases, RESEARCH funding, STATISTICS, DATA analysis, VISUAL analog scale, DATA analysis software, DESCRIPTIVE statistics, ODDS ratio, KRUSKAL-Wallis Test, INTRACLASS correlation, CHILDREN, PROGNOSIS

Abstract

Objective Juvenile dermatomyositis (DM) is a rare and severe autoimmune condition characterized by rash and proximal muscle weakness. While some patients respond to standard treatment, others do not. This study was carried out to investigate whether histopathologic findings and myositis-specific autoantibodies (MSAs) have prognostic significance in juvenile DM. Methods Muscle biopsy samples (n = 101) from patients in the UK Juvenile Dermatomyositis Cohort and Biomarker Study were stained, analyzed, and scored for severity of histopathologic features. In addition, autoantibodies were measured in the serum or plasma of patients (n = 90) and longitudinal clinical data were collected (median duration of follow-up 4.9 years). Long-term treatment status (on or off medication over time) was modeled using generalized estimating equations. Results Muscle biopsy scores differed according to MSA subgroup. When the effects of MSA subgroup were accounted for, increased severity of muscle histopathologic features was predictive of an increased risk of remaining on treatment over time: for the global pathology score (histopathologist's visual analog scale [hVAS] score), 1.48-fold higher odds (95% confidence interval [95% CI] 1.12-1.96; P = 0.0058), and for the total biopsy score (determined with the standardized score tool), 1.10-fold higher odds (95% CI 1.01-1.21; P = 0.038). A protective effect was identified in patients with anti-Mi-2 autoantibodies, in whom the odds of remaining on treatment were 7.06-fold lower (95% CI 1.41-35.36; P = 0.018) despite muscle biopsy scores indicating more severe disease. In patients with anti-nuclear matrix protein 2 autoantibodies, anti-transcription intermediary factor 1γ autoantibodies, or no detectable autoantibody, increased histopathologic severity alone, without adjustment for the effect of MSA subtype, was predictive of the risk of remaining on treatment: for the hVAS global pathology score, 1.61-fold higher odds (95% CI 1.16-2.22; P = 0.004), and for the total biopsy score, 1.13-fold higher odds (95% CI 1.03-1.24; P = 0.013). Conclusion Histopathologic severity, in combination with MSA subtype, is predictive of the risk of remaining on treatment in patients with juvenile DM and may be useful for discussing probable treatment length with parents and patients. Understanding these associations may identify patients at greater risk of severe disease. [ABSTRACT FROM AUTHOR]

Published

2016

13. Eosinophilic granulomatosis with polyangiitis in childhood: retrospective experience from a tertiary referral centre in the UK.

Author

Eleftheriou, Despina, Gale, Hugo, Pilkington, Clarissa, Fenton, Matthew, Sebire, Neil J., and Brogan, Paul A.

Subjects

MORTALITY risk factors, DIFFERENTIAL diagnosis, FISHER exact test, EVALUATION of medical care, CHURG-Strauss syndrome, RETROSPECTIVE studies, SEVERITY of illness index, DATA analysis software, DESCRIPTIVE statistics, DISEASE complications, SYMPTOMS

Abstract

Objective. To describe the presenting clinical features, treatment and outcome in children with eosinophilic granulomatosis with polyangiitis (EGPA) and to define factors that predicted mortality. Methods. A retrospective case notes review of patients fulfilling the Chapel Hill Consensus Conference definition and/or ACR criteria for EGPA seen at Great Ormond Street Hospital, London. Demographics, clinical features, histopathology, treatment and outcomes were recorded. Descriptive statistics were expressed as median and range. Fisher's exact test was used for group comparisons. The Paediatric Vasculitis Activity Score and Paediatric Vasculitis Damage Index (PVDI) were calculated. Results. Thirteen children (38% female) aged at diagnosis 14.1 (4-15.6) years were identified. The median time to diagnosis was 2 (0-7.3) years. History of asthma was documented in 76%. The most common presenting features were pulmonary (69%), skin (61 %), gastrointestinal (46%), cardiac involvement (46%), paranasal sinus abnormality (38%), arthritis/arthralgia (38%) and neurological involvement (15%). Paediatric Vasculitis Activity Score at presentation was 8/63 (2-25/63); ANCA was negative in all 10/13 patients tested. Treatment included corticosteroids in all, combined with CYC in 38% or AZA in 23%. PVDI at 12 (3-48) months follow-up was 3/72 (0-13/72). Relapses were recorded in 46%. Mortality was 15%; cardiomyopathy and PVDI scores ≥5 significantly associated with mortality risk (P = 0.012). Conclusion. EGPA in the paediatric population is a rare and potentially life-threatening vasculitis. Increased awareness is essential to secure a timely diagnosis and to promptly initiate treatment since our data emphasize a high mortality, particularly in those with cardiac involvement and significant accrued damage. [ABSTRACT FROM AUTHOR]

Published

2016

14. Analysis of Published Criteria for Clinically Inactive Disease in a Large Juvenile Dermatomyositis Cohort Shows That Skin Disease Is Underestimated.

Author

Almeida, Beverley, Campanilho‐Marques, Raquel, Arnold, Katie, Pilkington, Clarissa A., Wedderburn, Lucy R., Nistala, Kiran, Armon, Kate, Briggs, Vanja, Ellis‐Gage, Joe, Roper, Holly, Watts, Joanna, Baildam, Eileen, Hanna, Louise, Lloyd, Olivia, McCann, Liza, Roberts, Ian, McGovern, Ann, Riley, Phil, Al‐Abadi, Eslam, and Ryder, Clive

Subjects

SKIN disease diagnosis, ACADEMIC medical centers, ANALYSIS of variance, BLOOD testing, CHI-squared test, CONFIDENCE intervals, DERMATOMYOSITIS, PHYSICAL diagnosis, RESEARCH funding, SKIN diseases, STATISTICS, DATA analysis, DATA analysis software, SYMPTOMS, CHILDREN, DIAGNOSIS

Abstract

Objective. The Pediatric Rheumatology International Trials Organisation (PRINTO) recently published criteria for classification of patients with juvenile dermatomyositis (DM) as having clinically inactive disease. The criteria require that at least 3 of 4 conditions be met, i.e., creatine kinase level ≤150 units/liter, Childhood Myositis Assessment Scale score ≥48, Manual Muscle Testing in 8 muscles score ≥78, and physician's global assessment of overall disease activity (PGA) ≤0.2. The present study was undertaken to test these criteria in a UK cohort of patients with juvenile DM. Methods. We assessed 1,114 patient visits for the 4 items in the PRINTO criteria for clinically inactive disease. Each visit was analyzed to determine whether skin disease was present. The Disease Activity Score (DAS) for juvenile DM was determined in 59 patients. Results. At 307 of the 1,114 visits, clinically inactive disease was achieved based on the 3 muscle criteria (but with a PGA of >0.2); rash was present at 65.8% of these visits and nailfold capillary abnormalities at 35.2%. When PGA ≤0.2 was one of the 3 criteria that were met, the frequency of skin signs was significantly lower (rash in 23.1% and nailfold capillary abnormalities in 8.7%). If PGA was considered an essential criterion for clinically inactive disease (P-CID), patients with active skin disease were less likely to be categorized as having clinically inactive disease (a median DAS skin score of 0 [of a possible maximum of 9] in visits where the PGA was ≥0.2, versus a median DAS skin score of 4 in patients meeting the 3 muscle criteria [with a PGA of >0.2]; P < 0.001). Use of the P-CID led to improvements in the positive predictive value and the positive likelihood ratio (85.4% and 11.0, respectively, compared to 72.9% and 5.1 with the current criteria). Conclusion. There was a high frequency of skin disease among patients with juvenile DM who did not meet the PGA criterion for inactive disease but met the other 3 criteria. Incorporating PGA as an essential criterion for clinically inactive disease helps prevent the misclassification of patients with active skin disease. [ABSTRACT FROM AUTHOR]

Published

2015

15. Systemic Polyarteritis Nodosa in the Young: A Single-Center Experience Over Thirty-Two Years.

Author

Eleftheriou, Despina, Dillon, Michael J., Tullus, Kjell, Marks, Stephen D., Pilkington, Clarissa A., Roebuck, Derek J., Klein, Nigel J., and Brogan, Paul A.

Subjects

IMMUNOSUPPRESSIVE agents, ACADEMIC medical centers, ANGIOGRAPHY, BIOPSY, BLOOD testing, CONFIDENCE intervals, MEDICAL records, MULTIVARIATE analysis, REGRESSION analysis, POLYARTERITIS nodosa, PROPORTIONAL hazards models, RETROSPECTIVE studies, DATA analysis software, KAPLAN-Meier estimator, SYMPTOMS, CHILDREN, DIAGNOSIS, THERAPEUTICS

Abstract

Objective Polyarteritis nodosa (PAN) is a rare disease of childhood. The aims of this study were to describe the clinical features, treatment, and outcome of systemic childhood PAN and to identify predictors of relapse. Methods A single-center retrospective medical records review of children with PAN fulfilling the European League Against Rheumatism (EULAR)/Paediatric Rheumatology European Society (PRES)/Paediatric Rheumatology International Trials Organisation (PRINTO) classification criteria who were seen over a 32-year period was performed. Data on demographic and clinical features, treatments, relapses (recurrence of clinical signs/symptoms or occurrence of new symptoms after initial remission requiring escalation or resumption of immunosuppressive therapy), and deaths were recorded. A disease activity score was retrospectively assigned using the Paediatric Vasculitis Activity Score (PVAS) instrument. Cox regression analysis was used to identify significant predictors of relapse. Results Sixty-nine children with PAN were identified; 55% were male, and their median age was 8.5 years (range 0.9-15.8 years). Their clinical features at presentation were fever (87%), myalgia (83%), skin (88%), renal (19%), severe gastrointestinal (GI) (10%), and neurologic (10%) involvement. The PVAS at presentation was 9 of 63 (range 4-24). Histopathologic analysis of the skin showed necrotizing vasculitis in biopsy samples from 40 of 50 children. Results of selective visceral arteriography suggested the presence of PAN in 96% of patients. Treatment included cyclophosphamide and corticosteroids (83%), plasma exchange (9%), and biologic agents (after 2002; 13%). The relapse rate was 35%, and the mortality rate was 4%. Severe GI involvement was associated with increased risk of relapse ( P = 0.031), while longer time to induce remission ( P = 0.022) and increased cumulative dose of cyclophosphamide ( P = 0.005) were associated with lower relapse risk. Conclusion Childhood PAN is a severe inflammatory disease of insidious onset and variable clinical presentation. Relapses occurred more frequently in those with severe GI involvement. A higher cumulative dose of cyclophosphamide was associated with a lower risk of relapse. [ABSTRACT FROM AUTHOR]

Published

2013

16. Access to care for children and young people diagnosed with localized scleroderma or juvenile SSc in the UK.

Author

Hawley, Daniel P., Baildam, Eileen M., Amin, Tania S., Cruikshank, Mary K., Davidson, Joyce E., Dixon, Jennifer, Martin, Neil S., Ohlsson, Victoria, Pilkington, Clarissa, Rangaraj, Satyapal, Riley, Philip, Sundaramoorthy, Chitra, Walsh, Jo, and Foster, Helen E.

Subjects

SYSTEMIC scleroderma, ACADEMIC medical centers, AUDITING, HEALTH services accessibility, MEDICAL cooperation, MEDICAL records, HEALTH outcome assessment, PATIENT education, RESEARCH, JUVENILE idiopathic arthritis, TREATMENT effectiveness, RETROSPECTIVE studies, EARLY medical intervention, PHYSICIANS' attitudes, CHILDREN, THERAPEUTICS

Abstract

Objectives. To describe pathways of care and referral to paediatric rheumatology from onset of first symptom (noticed by the patient or their family) to diagnosis for children and young people diagnosed with localized scleroderma (LS) or juvenile SSc (jSSc).Methods. Retrospective case note audit of patients under paediatric rheumatology care who presented during January 2005–January 2010. Data included disease subtype, sex, age at key points in the referral pathway and health care professional (HCP) contact. All patient and HCP data were pseudo-anonymized in accordance with good clinical practice.Results. Data were from eight UK centres that saw 89 cases: 62 females, 26 males; 73 LS, 16 jSSc. Median time from first symptom to first HCP review was 4 (range 0–72) months (LS) and 1 (range 0–50) month (jSSc). Median time from first symptom to paediatric rheumatology review was 15 (range 1–103) months (LS) and 7 (range 0–50) months (jSSc). Median time from first HCP review to first paediatric rheumatology review was 11 (range 0–103) months (LS) and 2 (range 0–10) months. First HCP seen (74%) was usually a general practitioner. The referring HCP to paediatric rheumatology was usually a dermatologist (56%) for LS. Median time from first symptom to diagnosis was 13 (range 1–102) months (LS) and 8 (range 1–50) months (jSSc).Conclusion. A prolonged interval occurs from first symptom to definitive diagnosis, which may adversely affect outcome. There is a need to raise awareness of this rare diagnosis and facilitate earlier recognition. [ABSTRACT FROM PUBLISHER]

Published

2012

17. Assessment of active inflammation in juvenile dermatomyositis: a novel magnetic resonance imaging-based scoring system.

Author

Davis, Warren R., Halls, James E., Offiah, Amaka C., Pilkington, Clarissa, Owens, Catherine M., and Rosendahl, Karen

Subjects

DERMATOMYOSITIS, INFLAMMATION, MAGNETIC resonance imaging, MEDICAL needs assessment, RESEARCH evaluation, JUVENILE idiopathic arthritis, STATISTICS, EQUIPMENT & supplies, RETROSPECTIVE studies, SEVERITY of illness index, DATA analysis software, CHILDREN, DIAGNOSIS

Abstract

Objective. To assess the reproducibility of a novel scoring system that we have developed for the objective assessment of acute inflammatory change in JDM. This system defines markers of inflammatory change in four muscle groups and the surrounding soft tissues.Methods. Forty-eight children (33 girls) underwent retrospective assessment of their MRI studies by two musculoskeletal paediatric radiologists for the presence of disease activity. Each observer performed the readings on two separate occasions. The degree of concordance between the two observers and between the two readings was assessed using kappa analysis. The reproducibility of the total score was determined using Bland–Altman analysis.Results. There was fair to moderate agreement between the two observers for all the examined disease activity markers in all muscle groups. There was good intra-observer agreement between the two readings. There was no difference according to the side evaluated. The mean total score (out of 20) for Observer 1 was 7.9 and for Observer 2 was 7.5 (mean difference −0.4, 95% limits of agreement −6.8 to 6.0), while the mean total scores for Observer 1 were 9.0 for the first reading and 7.9 for the second reading (mean difference 1.0, 95% limits of agreement −2.6 to 4.6).Conclusion. Markers of inflammatory change in JDM can be observed on MRI in a reliable fashion and have been used to make a reliable and objective scoring system. The accuracy of the proposed scoring system is acceptable for the single reader, although there is more variability between two different individuals. [ABSTRACT FROM PUBLISHER]

Published

2011

18. Biologic therapy in primary systemic vasculitis of the young.

Author

Eleftheriou, Despina, Melo, Marianna, Marks, Stephen D., Tullus, Kjell, Sills, John, Cleary, Gavin, Dolezalova, Pavla, Ozen, Seza, Pilkington, Clarissa, Woo, Pat, Klein, Nigel, Dillon, Michael J., and Brogan, Paul A.

Subjects

VASCULITIS, PEDIATRIC therapy, BIOLOGICALS, TREATMENT of vascular diseases, INFECTION in children

Abstract

Objectives. To describe the biologic treatment regimens and report the efficacy and safety of biologic therapies in a multicentre series of children with primary systemic vasculitis (PSV). [ABSTRACT FROM PUBLISHER]

Published

2009

19. Paediatric Idiopathic Inflammatory Muscle Disease: Recognition and Management.

Author

Pilkington, Clarissa A. and Wedderburn, Lucy R.

Subjects

*MUSCLE diseases, *PEDIATRICS, *AUTOIMMUNE diseases, *IMMUNOLOGIC diseases, *DISEASES, *MEDICINE

Abstract

The idiopathic inflammatory myopathies (IIM) of childhood are rare, multisystem autoimmune disorders, of which the most common is juvenile dermatomyositis (JDM). The criteria currently used to diagnose the paediatric IIMs, including both JDM and other childhood autoimmune conditions in which myositis may be a prominent feature, are somewhat outdated in relation to paediatric practice. Controversies surrounding the criteria for diagnosis have resulted in an international effort to define both the diagnostic and classification criteria in light of modern investigation and practice. Clinical features of these IIMs include muscle weakness and skin rash; however, these may be absent at disease onset. JDM patients require careful assessment of multiple organ systems, which can divided into musculoskeletal and extra-musculoskeletal, and examination should include validated disease measurement tools such as the Childhood Myositis Assessment Scale. Investigations include blood tests to assess generalised markers of inflammation as well as more specific markers of muscle inflammation; organ-specific investigations, such as MRI, and muscle biopsy are also often used. Treatment and management protocols include corticosteroids, methotrexate and other disease-modifying agents such as ciclosporin (cyclosporin) and intravenous immunoglobulin, as well as newer treatments such as tumour necrosis factor blockade or B-cell depletion. Management of children with JDM requires a multidisciplinary approach, including specialist physiotherapy, occupational therapy and nursing input. Two major international projects, the International Myositis and Clinical Studies Group (IMACS) and Paediatric Rheumatology International Trials Organisation (PRINTO) aim to standardise the assessment of these patients and measurement of their disease. The efforts of these large collaborative groups should provide much needed networks for mulitcentre trials in the future. [ABSTRACT FROM AUTHOR]

Published

2005

20. Introduction.

Author

Pilkington, Clarissa, Beresford, Michael W., Foster, Helen, and Walsh, Jo

Subjects

*RHEUMATISM treatment, *CHARITIES, *CONFERENCES & conventions, *CHILDREN

Abstract

An introduction to British Society for Paediatric and Adolescent Rheumatology (BSPAR), a registered society that aims to give equitable access to high-quality clinical care to all children with rheumatic disease, is presented.

Published

2012