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1. Effects of nintedanib in patients with limited cutaneous systemic sclerosis and interstitial lung disease

Author

Allanore, Y., Khanna, D., Smith, V., Aringer, M., Hoffmann-Vold, A.M., Kuwana, M., Merkel, P.A., Stock, C., Vonk, M.C., Sambevski, S., Denton, C.P., Allanore, Y., Khanna, D., Smith, V., Aringer, M., Hoffmann-Vold, A.M., Kuwana, M., Merkel, P.A., Stock, C., Vonk, M.C., Sambevski, S., and Denton, C.P.

Abstract

Contains fulltext : 305344.pdf (Publisher’s version ) (Open Access), OBJECTIVES: To investigate the course of interstitial lung disease (ILD) and the effects of nintedanib in patients with limited cutaneous systemic sclerosis (lcSSc). METHODS: In the SENSCIS trial, patients with SSc-ILD were randomized to receive nintedanib or placebo. Patients who completed the SENSCIS trial were eligible to enter SENSCIS-ON, in which all patients received open-label nintedanib. RESULTS: Among 277 patients with lcSSc treated in the SENSCIS trial, the rate (s.e.) of decline in forced vital capacity (FVC; ml/year) over 52 weeks was -74.5 (19.2) in the placebo group and -49.1 (19.8) in the nintedanib group (difference: 25.3 [95% CI -28.9, 79.6]). Among 249 patients with data at week 52, mean (s.e.) change in FVC at week 52 was -86.4 (21.1) ml in the placebo group and -39.1 (22.2) ml in the nintedanib group. Among 183 patients with lcSSc who participated in SENSCIS-ON and had data at week 52, mean (s.e.) change in FVC from baseline to week 52 of SENSCIS-ON was -41.5 (24.0) ml in patients who took placebo in the SENSCIS trial and initiated nintedanib in SENSCIS-ON and -45.1 (19.1) ml in patients who took nintedanib in the SENSCIS trial and continued it in SENSCIS-ON. CONCLUSION: Patients with lcSSc may develop progressive fibrosing ILD. By targeting pulmonary fibrosis, nintedanib slows decline in lung function in patients with lcSSc and ILD. TRIAL REGISTRATION: ClinicalTrials.gov (https://clinicaltrials.gov), NCT02597933 and NCT03313180.

Published
2024

2. Poursuite du traitement par le nintédanib chez les patients atteints de sclérodermie systémique cutanée limitée (SCSCL) et de pneumopathie interstitielle diffuse (PID)

Author

Allanore, Y., primary, Khanna, D., additional, Smith, V., additional, Aringer, M., additional, Hoffmann-Vold, A.M., additional, Kuwana, M., additional, Merkel, P.A., additional, James, A., additional, Sambeski, S., additional, Alves, M., additional, and Denton, C.P., additional

Published
2022
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4. Systemic sclerosis and COVID-19 vaccines: A SPIN Cohort study [Comment]

Author

Gordon, J.K., Showalter, K., Wu, Y., Kwakkenbos, L., Carrier, M.E., Henry, R.S., Ostbo, N., Nordlund, J., Bourgeault, A., Cañedo-Ayala, M., Carboni-Jiménez, A., Denton, C.P., Mouthon, L., Thombs, B.D., Spiera, R.F., Gordon, J.K., Showalter, K., Wu, Y., Kwakkenbos, L., Carrier, M.E., Henry, R.S., Ostbo, N., Nordlund, J., Bourgeault, A., Cañedo-Ayala, M., Carboni-Jiménez, A., Denton, C.P., Mouthon, L., Thombs, B.D., and Spiera, R.F.

Abstract

Item does not contain fulltext

Published
2022

5. Systemic sclerosis in the time of COVID-19

Author

Hoffmann-Vold, A.M., Distler, O., Bruni, C., Denton, C.P., Vries-Bouwstra, J. de, Cerinic, M. Matucci, Vonk, M.C., Gabrielli, A., Hoffmann-Vold, A.M., Distler, O., Bruni, C., Denton, C.P., Vries-Bouwstra, J. de, Cerinic, M. Matucci, Vonk, M.C., and Gabrielli, A.

Abstract

Item does not contain fulltext, The COVID-19 pandemic represents one of the biggest challenges of the 21st century. In addition to the general effect on society and health-care systems, patients with systemic sclerosis and their physicians face specific challenges related to the chronic nature of their disease, the involvement of multiple organs, and the use of immunosuppressive treatments. Data from registries and single centre cohorts indicate that the risk of contracting SARS-CoV-2 does not seem to increase substantially in people with systemic sclerosis; conversely, severe COVID-19 outcomes are seen more frequently in these patients than in the general population. Vaccination against SARS-CoV-2 is therefore highly recommended for patients with systemic sclerosis; however, no specific recommendations are available regarding the different vaccine platforms. Both patients and physicians should be aware that the effectiveness of vaccines might be reduced in patients taking immunosuppressive therapy, because antibody responses might be blunted, specifically in patients treated with rituximab and mycophenolate mofetil.

Published
2022

6. Complement component C4 structural variation and quantitative traits contribute to sex-biased vulnerability in systemic sclerosis

Author

Kerick, M., Acosta-Herrera, M., Simeón-Aznar, C.P., Callejas, J.L., Assassi, S., Proudman, S.M., Nikpour, M., Hunzelmann, N., Moroncini, G., Vries-Bouwstra, J.K. de, Orozco, G., Barton, A., Herrick, A.L., Terao, C., Allanore, Y., Fonseca, C., Alarcón-Riquelme, M.E., Radstake, T.R., Beretta, L., Denton, C.P., Vonk, M.C., Mayes, M.D., Martin, J., Kerick, M., Acosta-Herrera, M., Simeón-Aznar, C.P., Callejas, J.L., Assassi, S., Proudman, S.M., Nikpour, M., Hunzelmann, N., Moroncini, G., Vries-Bouwstra, J.K. de, Orozco, G., Barton, A., Herrick, A.L., Terao, C., Allanore, Y., Fonseca, C., Alarcón-Riquelme, M.E., Radstake, T.R., Beretta, L., Denton, C.P., Vonk, M.C., Mayes, M.D., and Martin, J.

Abstract

Item does not contain fulltext, Copy number (CN) polymorphisms of complement C4 play distinct roles in many conditions, including immune-mediated diseases. We investigated the association of C4 CN with systemic sclerosis (SSc) risk. Imputed total C4, C4A, C4B, and HERV-K CN were analyzed in 26,633 individuals and validated in an independent cohort. Our results showed that higher C4 CN confers protection to SSc, and deviations from CN parity of C4A and C4B augmented risk. The protection contributed per copy of C4A and C4B differed by sex. Stronger protection was afforded by C4A in men and by C4B in women. C4 CN correlated well with its gene expression and serum protein levels, and less C4 was detected for both in SSc patients. Conditioned analysis suggests that C4 genetics strongly contributes to the SSc association within the major histocompatibility complex locus and highlights classical alleles and amino acid variants of HLA-DRB1 and HLA-DPB1 as C4-independent signals.

Published
2022

7. Biological and clinical insights from a randomized phase 2 study of an anti-oncostatin M monoclonal antibody in systemic sclerosis

Author

Denton, C.P., Galdo, F. Del, Khanna, D., Vonk, M.C., Chung, L., Johnson, S.R., Varga, J., Furst, D.E., Temple, J., Zecchin, C., Csomor, E., Lee, A, Wisniacki, N., Flint, S.M., Reid, J., Denton, C.P., Galdo, F. Del, Khanna, D., Vonk, M.C., Chung, L., Johnson, S.R., Varga, J., Furst, D.E., Temple, J., Zecchin, C., Csomor, E., Lee, A, Wisniacki, N., Flint, S.M., and Reid, J.

Abstract

Item does not contain fulltext, OBJECTIVES: The cytokine oncostatin M (OSM) is implicated in the pathology of SSc. Inhibiting OSM signalling using GSK2330811 (an anti-OSM monoclonal antibody) in patients with SSc has the potential to slow or stop the disease process. METHODS: This multicentre, randomized, double-blind, placebo-controlled study enrolled participants ≥18 years of age with active dcSSc. Participants were randomized 3:1 (GSK2330811:placebo) in one of two sequential cohorts to receive GSK2330811 (cohort 1: 100 mg; cohort 2: 300 mg) or placebo s.c. every other week for 12 weeks. The primary endpoint was safety; blood and skin biopsy samples were collected to explore mechanistic effects on inflammation and fibrosis. Clinical efficacy was an exploratory endpoint. RESULTS: Thirty-five participants were randomized to placebo (n = 8), GSK2330811 100 mg (n = 3) or GSK2330811 300 mg (n = 24). Proof of mechanism, measured by coordinate effects on biomarkers of inflammation or fibrosis, was not demonstrated following GSK2330811 treatment. There were no meaningful differences between GSK2330811 and placebo for any efficacy endpoints. The safety and tolerability of GSK2330811 were not favourable in the 300 mg group, with on-target, dose-dependent adverse events related to decreases in haemoglobin and platelet count that were not observed in the 100 mg or placebo groups. CONCLUSION: Despite a robust and novel experimental medicine approach and evidence of target engagement, anticipated SSc-related biologic effects of GSK2330811 were not different from placebo and safety was unfavourable, suggesting OSM inhibition may not be a useful therapeutic strategy in SSc. TRIAL REGISTRATION NUMBER: ClinicalTrials.gov, NCT03041025; EudraCT, 2016-003417-95.

Published
2022

8. Systemic sclerosis and COVID-19 vaccines: A SPIN Cohort study

Author

Gordon, J.K., Showalter, K., Wu, Y., Kwakkenbos, L., Carrier, M.E., Henry, R.S., Ostbo, N., Nordlund, J., Bourgeault, A., Cañedo-Ayala, M., Carboni-Jiménez, A., Denton, C.P., Mouthon, L., Thombs, B.D., Spiera, R.F., Gordon, J.K., Showalter, K., Wu, Y., Kwakkenbos, L., Carrier, M.E., Henry, R.S., Ostbo, N., Nordlund, J., Bourgeault, A., Cañedo-Ayala, M., Carboni-Jiménez, A., Denton, C.P., Mouthon, L., Thombs, B.D., and Spiera, R.F.

Abstract

Item does not contain fulltext

Published
2022

9. European dermatology forum S1‐guideline on the diagnosis and treatment of sclerosing diseases of the skin, Part 2: Scleromyxedema, scleredema and nephrogenic systemic fibrosis

Author

Knobler, R., Moinzadeh, P., Hunzelmann, N., Kreuter, A., Cozzio, A., Mouthon, L., Cutolo, M., Rongioletti, F., Denton, C.P., Rudnicka, L., Frasin, L.A., Smith, V., Gabrielli, A., Aberer, E., Bagot, M., Bali, G., Bouaziz, J., Braae Olesen, A., Foeldvari, I., Frances, C., Jalili, A., Just, U., Kähäri, V., Kárpáti, S., Kofoed, K., Krasowska, D., Olszewska, M., Orteu, C., Panelius, J., Parodi, A., Petit, A., Quaglino, P., Ranki, A., Sanchez Schmidt, J.M., Seneschal, J., Skrok, A., Sticherling, M., Sunderkötter, C., Taieb, A., Tanew, A., Wolf, P., Worm, M., Wutte, N.J., and Krieg, T.

Published
2017
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10. European Dermatology Forum S1‐guideline on the diagnosis and treatment of sclerosing diseases of the skin, Part 1: localized scleroderma, systemic sclerosis and overlap syndromes

Author

Knobler, R., Moinzadeh, P., Hunzelmann, N., Kreuter, A., Cozzio, A., Mouthon, L., Cutolo, M., Rongioletti, F., Denton, C.P., Rudnicka, L., Frasin, L.A., Smith, V., Gabrielli, A., Aberer, E., Bagot, M., Bali, G., Bouaziz, J., Braae Olesen, A., Foeldvari, I., Frances, C., Jalili, A., Just, U., Kähäri, V., Kárpáti, S., Kofoed, K., Krasowska, D., Olszewska, M., Orteu, C., Panelius, J., Parodi, A., Petit, A., Quaglino, P., Ranki, A., Sanchez Schmidt, J.M., Seneschal, J., Skrok, A., Sticherling, M., Sunderkötter, C., Taieb, A., Tanew, A., Wolf, P., Worm, M., Wutte, N.J., and Krieg, T.

Published
2017
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11. Rituximab versus Cyclophosphamide for the Treatment of Connective Tissue Disease Associated Interstitial Lung Disease (RECITAL): A Multi-Centre Randomised Controlled Trial

Author

Maher, T.M., primary, Tudor, V., additional, Saunders, P., additional, Gibbons, M., additional, Fletcher, S., additional, Parfrey, H., additional, Denton, C.P., additional, Renzoni, E., additional, Kokosi, M., additional, Wells, A.U., additional, Ashby, D., additional, Szigeti, M., additional, and Molyneaux, P.L., additional

Published
2022
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12. Vaccination against COVID-19: self-reported experiences of patients with systemic sclerosis in the Scleroderma Patient-centered Intervention Network (SPIN) Cohort

Author

Showalter, K., Gordon, J.K., Wu, Y., Kwakkenbos, L., Carrier, M.E., Henry, R.S., Ostbo, N., Nordlund, J., Bourgeault, A., Cañedo-Ayala, M., Discepola, M.N., Carboni-Jiménez, A., Denton, C.P., Mouthon, L., Thombs, B.D., and Spiera, R.F.

Subjects
Experimental Psychopathology and Treatment
Abstract

Item does not contain fulltext 3 p.

Published
2021

14. Perceptions and concerns regarding COVID-19 vaccination in patients with systemic sclerosis in the Scleroderma Patient-centered Intervention Network (SPIN) Cohort

Author

Gordon, J.K., Showalter, K., Wu, Y., Kwakkenbos, L., Carrier, M.E., Henry, R.S., Ostbo, N., Nordlund, J., Bourgeault, A., Cañedo-Ayala, M., Discepola, M.N., Carboni-Jiménez, A., Denton, C.P., Mouthon, L., Thombs, B.D., and Spiera, R.F.

Subjects
Experimental Psychopathology and Treatment
Abstract

Item does not contain fulltext 4 p.

Published
2021

15. Primary systemic sclerosis heart involvement: A systematic literature review and preliminary data-driven, consensus-based WSF/HFA definition

Author

Bruni, C. Buch, M.H. Furst, D.E. De Luca, G. Djokovic, A. Dumitru, R.B. Giollo, A. Polovina, M. Steelandt, A. Bratis, K. Suliman, Y.A. Milinkovic, I. Baritussio, A. Hasan, G. Xintarakou, A. Isomura, Y. Markousis-Mavrogenis, G. Tofani, L. Mavrogeni, S. Gargani, L. Caforio, A.L.P. Tschöpe, C. Ristic, A. Klingel, K. Plein, S. Behr, E.R. Allanore, Y. Kuwana, M. Denton, C.P. Khanna, D. Krieg, T. Marcolongo, R. Galetti, I. Zanatta, E. Tona, F. Seferovic, P. Matucci-Cerinic, M.

Abstract

Introduction: Primary heart involvement in systemic sclerosis may cause morpho-functional and electrical cardiac abnormalities and is a common cause of death. The absence of a clear definition of primary heart involvement in systemic sclerosis limits our understanding and ability to focus on clinical research. We aimed to create an expert consensus definition for primary heart involvement in systemic sclerosis. Methods: A systematic literature review of cardiac involvement and manifestations in systemic sclerosis was conducted to inform an international and multi-disciplinary task force. In addition, the nominal group technique was used to derive a definition that was then subject to voting. A total of 16 clinical cases were evaluated to test face validity, feasibility, reliability and criterion validity of the newly created definition. Results: In total, 171 publications met eligibility criteria. Using the nominal group technique, experts added their opinion, provided statements to consider and ranked them to create the consensus definition, which received 100% agreement on face validity. A median 60(5–300) seconds was taken for the feasibility on a single case. Inter-rater agreement was moderate (mKappa (95% CI) = 0.56 (0.46–1.00) for the first round and 0.55 (0.44–1.00) for the second round) and intra-rater agreement was good (mKappa (95% CI) = 0.77 (0.47–1.00)). Criterion validity showed a 78 (73–84)% correctness versus gold standard. Conclusion: A preliminary primary heart involvement in systemic sclerosis consensus-based definition was created and partially validated, for use in future clinical research. © The Author(s) 2021.

Published
2021

16. Efficacy and safety of nintedanib in patients with systemic sclerosis-associated interstitial lung disease treated with mycophenolate: a subgroup analysis of the SENSCIS trial

Author

Highland, K.B., Distler, O., Kuwana, M., Allanore, Y., Assassi, S., Azuma, A., Bourdin, A., Denton, C.P., Distler, J.H., Hoffmann-Vold, A.M., Khanna, D., Mayes, M.D., Raghu, G., Vonk, M.C., Gahlemann, M., Clerisme-Beaty, E., Girard, M., Stowasser, S., Zoz, D., Maher, T.M., Highland, K.B., Distler, O., Kuwana, M., Allanore, Y., Assassi, S., Azuma, A., Bourdin, A., Denton, C.P., Distler, J.H., Hoffmann-Vold, A.M., Khanna, D., Mayes, M.D., Raghu, G., Vonk, M.C., Gahlemann, M., Clerisme-Beaty, E., Girard, M., Stowasser, S., Zoz, D., and Maher, T.M.

Abstract

Item does not contain fulltext, BACKGROUND: In the Safety and Efficacy of Nintedanib in Systemic Sclerosis (SENSCIS) trial, nintedanib reduced the rate of decline in forced vital capacity (FVC) in patients with systemic sclerosis-associated interstitial lung disease (SSc-ILD). Patients on stable treatment with mycophenolate for at least 6 months before randomisation could participate. The aim of this subgroup analysis was to examine the efficacy and safety of nintedanib by mycophenolate use at baseline. METHODS: The SENSCIS trial was a randomised, double-blind, placebo-controlled trial, in which patients with SSc-ILD were randomly assigned (1:1) to receive 150 mg of oral nintedanib twice daily or placebo for at least 52 weeks. In a prespecified subgroup analysis, we analysed the primary endpoint of rate of decline in FVC over 52 weeks by mycophenolate use at baseline. In a post-hoc analysis, we analysed the proportion of patients with an absolute decrease in FVC of at least 3·3% predicted at week 52 (proposed minimal clinically important difference estimate for worsening of FVC in patients with SSc-ILD) in subgroups by mycophenolate use at baseline. Adverse events were reported in subgroups by mycophenolate use at baseline. Analyses were done in all participants who received at least one dose of study drug. We analysed the annual rate of decline in FVC using a random coefficient regression model (with random slopes and intercepts) including anti-topoisomerase I antibody status, age, height, sex, and baseline FVC as covariates and terms for baseline-by-time, treatment-by-subgroup, and treatment-by-subgroup-by-time interactions. SENSCIS is registered with ClinicalTrials.gov, NCT02597933, and is now complete. FINDINGS: Between Nov 30, 2015, and Oct 31, 2017, 819 participants were screened and 576 were enrolled, randomly assigned to, and treated with nintedanib (n=288) or placebo (n=288). 139 (48%) of 288 in the nintedanib group and 140 (49%) of 288 in the placebo group were taking mycophenolate at ba

Published
2021

20. Standardisation of nailfold capillaroscopy for the assessment of patients with Raynaud's phenomenon and systemic sclerosis

Author

Smith, V., Herrick, A.L., Ingegnoli, F., Damjanov, N., Angelis, R. De, Denton, C.P., Distler, O., Espejo, K., Foeldvari, I., Frech, T., Garro, B., Gutierrez, M., Gyger, G., Hachulla, E., Hesselstrand, R., Iagnocco, A., Kayser, C., Melsens, K., Muller-Ladner, U., Paolino, S., Pizzorni, C., Radic, M., Riccieri, V., Snow, M., Stevens, W.B.C., Sulli, A., Laar, J.M. van, Vonk, M.C., Vanhaecke, A., Cutolo, M., Smith, V., Herrick, A.L., Ingegnoli, F., Damjanov, N., Angelis, R. De, Denton, C.P., Distler, O., Espejo, K., Foeldvari, I., Frech, T., Garro, B., Gutierrez, M., Gyger, G., Hachulla, E., Hesselstrand, R., Iagnocco, A., Kayser, C., Melsens, K., Muller-Ladner, U., Paolino, S., Pizzorni, C., Radic, M., Riccieri, V., Snow, M., Stevens, W.B.C., Sulli, A., Laar, J.M. van, Vonk, M.C., Vanhaecke, A., and Cutolo, M.

Abstract

Contains fulltext : 219902.pdf (Publisher’s version ) (Open Access), Capillaroscopy is a non-invasive and safe tool which allows the evaluation of the morphology of the microcirculation. Since its recent incorporation in the 2013 American College of Rheumatology (ACR)/European League Against Rheumatism (EULAR) classification criteria for systemic sclerosis together with its assessed role to monitor disease progression, capillaroscopy became a 'mainstream' investigation for rheumatologists. Given its increasing use by a variety of physicians internationally both in daily practice to differentiate primary from secondary Raynaud's phenomenon, as well as in research context to predict disease progression and monitor treatment effects, standardisation in capillaroscopic image acquisition and analysis seems paramount. To step forward to this need, experts in the field of capillaroscopy/microcirculation provide in this very consensus paper their view on image acquisition and analysis, different capillaroscopic techniques, normal and abnormal capillaroscopic characteristics and their meaning, scoring systems and reliability of image acquisition and interpretation.

Published
2020

21. Analysis of Anti-RNA Polymerase III Antibody-positive Systemic Sclerosis and Altered GPATCH2L and CTNND2 Expression in Scleroderma Renal Crisis

Author

Stern, E.P., Guerra, S. G., Chinque, H., Acquaah, V., González-Serna, David, Ponticos, M., Martín, J., Ong, V.H., Khan, K., Nihtyanova, S.I., Harber, M., Burns, A., Mayes, Maureen D., Assassi, S., Fonseca, Carmen, Denton, C.P., Stern, E.P., Guerra, S. G., Chinque, H., Acquaah, V., González-Serna, David, Ponticos, M., Martín, J., Ong, V.H., Khan, K., Nihtyanova, S.I., Harber, M., Burns, A., Mayes, Maureen D., Assassi, S., Fonseca, Carmen, and Denton, C.P.

Abstract

OBJECTIVE: Scleroderma renal crisis (SRC) is a life-threatening complication of systemic sclerosis (SSc) strongly associated with anti-RNA polymerase III antibody (ARA) autoantibodies. We investigated genetic susceptibility and altered protein expression in renal biopsy specimens in ARA-positive patients with SRC. METHODS: ARA-positive patients (n = 99) with at least 5 years' follow-up (49% with a history of SRC) were selected from a well characterized SSc cohort (n = 2254). Cases were genotyped using the Illumina Human Omni-express chip. Based on initial regression analysis, 9 single-nucleotide polymorphisms (SNP) were chosen for validation in a separate cohort of 256 ARA-positive patients (40 with SRC). Immunostaining of tissue sections from SRC or control kidney was used to quantify expression of candidate proteins based upon genetic analysis of the discovery cohort. RESULTS: Analysis of 641,489 SNP suggested association of POU2F1 (rs2093658; P = 1.98 × 10-5), CTNND2 (rs1859082; P = 5.58 × 10-5), HECW2 (rs16849716; P = 1.2 × 10-4), and GPATCH2L (rs935332; P = 4.92 × 10-5) with SRC. Further, the validation cohort showed an association between rs935332 within the GPATCH2L region, with SRC (P = 0.025). Immunostaining of renal biopsy sections showed increased tubular expression of GPATCH2L (P = 0.026) and glomerular expression of CTNND2 (P = 0.026) in SRC samples (n = 8) compared with normal human kidney controls (n = 8), despite absence of any genetic replication for the associated SNP. CONCLUSION: Increased expression of 2 candidate proteins, GPATCH2L and CTNND2, in SRC compared with control kidney suggests a potential role in pathogenesis of SRC. For GPATCH2L, this may reflect genetic susceptibility in ARA-positive patients with SSc based upon 2 independent cohorts.

Published
2020

22. Clinical features and prognosis of primary biliary cirrhosis associated with systemic sclerosis

Author

Rigamonti, C., Shand, L.M., Feudjo, M., Bunn, C.C., Black, C.M., Denton, C.P., and Burroughs, A.K.

Subjects
Biliary cirrhosis -- Development and progression, Biliary cirrhosis -- Patient outcomes, Scleroderma (Disease) -- Complications and side effects, Scleroderma (Disease) -- Patient outcomes, Systemic scleroderma -- Complications and side effects, Systemic scleroderma -- Patient outcomes, Health
Published
2006

23. Efficacité et tolérance du nintédanib chez des patients atteints de pneumopathie interstitielle diffuse associée à la sclérodermie systémique (SSc-PID) en fonction de l’indice de masse corporelle (IMC) à l’inclusion : analyse en sous-groupes de l’étude SENSCIS

Author

Jouneau, S., primary, Lescoat, A., additional, Crestani, B., additional, Riemekasten, G., additional, Kondoh, Y., additional, Smith, V., additional, Patel, M.P., additional, Huggins, J.T., additional, Stock, C., additional, Gahlemann, M., additional, Alves, M., additional, and Denton, C.P., additional

Published
2021
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24. Le taux de déclin de la fonction pulmonaire est-il le même chez les patients atteints d’une pneumopathie interstitielle diffuse associée à la sclérodermie systémique (PID-ScS) qui présentent une perte de poids ? Données de l’étude SENSCIS

Author

Lescoat, A., primary, Jouneau, S., additional, Crestani, B., additional, Riemekasten, G., additional, Kondoh, Y., additional, Smith, V., additional, Patel, N.M., additional, Huggins, J.T., additional, Stock, C., additional, Gahlemann, M., additional, Alves, M., additional, and Denton, C.P., additional

Published
2020
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31. An open-label pilot study of infliximab therapy in diffuse cutaneous systemic sclerosis

Author

Denton, C.P., Engelhart, M., Tvede, N., Wilson, H., Khan, K., Shiwen, X., Carreira, P.E., Diaz Gonzalez, F., Black, C.M., and van den Hoogen, F.H.

Subjects
Scleroderma (Disease) -- Drug therapy, Scleroderma (Disease) -- Research, Systemic scleroderma -- Drug therapy, Systemic scleroderma -- Research, Infliximab -- Dosage and administration, Infliximab -- Research, Immunosuppression -- Research, Health
Published
2009

32. Geographical variation of disease manifestations in systemic sclerosis: a report from the EULAR Scleroderma Trials and Research (EUSTAR) group database

Author

Walker, U.A., Tyndall, A., Czirjak, L., Denton, C.P., Farge-Bancel, D., Kowal-Bielecka, O., Muller-Ladner, U., and Matucci-Cerinic, M.

Subjects
Scleroderma (Disease) -- Research, Scleroderma (Disease) -- Demographic aspects, Scleroderma (Disease) -- Genetic aspects, Systemic scleroderma -- Research, Systemic scleroderma -- Demographic aspects, Systemic scleroderma -- Genetic aspects, Collagen -- Research, Collagen -- Physiological aspects, Health
Published
2009

33. GWAS for systemic sclerosis identifies multiple risk loci and highlights fibrotic and vasculopathy pathways

Author

López-Isac, E., Acosta-Herrera, M., Kerick, M., Assassi, S., Satpathy, A.T., Granja, J., Mumbach, M.R., Beretta, L., Simeón, C.P., Carreira, P., Ortego-Centeno, N., Castellvi, I., Bossini-Castillo, L., Carmona, F.D., Orozco, G., Hunzelmann, N., Distler, J.H.W., Franke, A., Lunardi, C., Moroncini, G., Gabrielli, A., de Vries-Bouwstra, J., Wijmenga, C., Koeleman, B.P.C., Nordin, A., Padyukov, L., Hoffmann-Vold, A.-M., Lie, B., Ríos, R., Callejas, J.L., Vargas-Hitos, J.A., García-Portales, R., Camps, M.T., Fernández-Nebro, A., González-Escribano, M.F., García-Hernández, F.J., Castillo, M.J., Aguirre, M.A., Gómez-Gracia, I., Fernández-Gutiérrez, B., Rodríguez-Rodríguez, L., García de la Peña, P., Vicente, E., Andreu, J.L., Fernández de Castro, M., López-Longo, F.J., Martínez, L., Fonollosa, V., Guillén, A., Espinosa, G., Tolosa, C., Pros, A., Rodríguez-Carballeira, M., Narváez, F.J., Rubio-Rivas, M., Ortiz-Santamaría, V, Madroñero, A.B., González-Gay, M.A., Díaz, B., Trapiella, L., Sousa, A., Egurbide, M.V., Fanlo-Mateo, P., Sáez-Comet, L., Díaz, F., Hernández, V, Beltrán, E., Román-Ivorra, J.A., Grau E., Alegre-Sancho, J.J., Freire, M., Blanco-García, F.J., Oreiro, N., Witte, T., Kreuter, A., Riemekasten, G., Airó P., Magro, C., Voskuyl, A.E., Vonk, M.C., Hesselstrand, R., Proudman S., Stevens, W., Nikpour, M., Zochling, J., Sahhar, J., Roddy, J., Nash, P., Tymms, K., Rischmueller, M., Lester, S., Vyse, T., Herrick, A.L., Worthington, J., Denton C.P., Allanore, Y., Brown, M.A., Radstake, T.R.D.J., Fonseca, C., Chang H.Y., Mayes, M.D., Martin, J., European Scleroderma Group, Australian Scleroderma Interest Group (ASIG), Universidad de Salamanca, Ministerio de Economía y Competitividad (España), Junta de Andalucía, Ministerio de Educación, Cultura y Deporte (España), Instituto de Salud Carlos III, Howard Hughes Medical Institute, Federal Ministry of Education and Research (Germany), Universidad de Cantabria, [López-Isac E, Acosta-Herrera M, Kerick M] Institute of Parasitology and Biomedicine López-Neyra, IPBLN-CSIC, Granada, Spain. [Assassi S] The University of Texas Health Science Center-Houston, Houston, USA. [Satpathy AT, Granja J] Center for Personal Dynamic Regulomes, Stanford University School of Medicine, Stanford, USA. Howard Hughes Medical Institute, Stanford University, Stanford, USA. [Simeón CP] Servei de Medicina Interna, Vall d'Hebron Hospital Universitari, Barcelona, Spain, Vall d'Hebron Barcelona Hospital Campus, Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Rheumatology, and AII - Inflammatory diseases

Subjects
0301 basic medicine, Chemistry(all), AUTOIMMUNITY, Àcids nucleics, General Physics and Astronomy, Genome-wide association study, Disease, VARIANTS, Biochemistry, ANNOTATION, 0302 clinical medicine, Phosphopantothenoylcysteine decarboxylase, Single nucleotide, Non-U.S. Gov't, lcsh:Science, skin and connective tissue diseases, características del estudio::metaanálisis [CARACTERÍSTICAS DE PUBLICACIONES], Multidisciplinary, Nucleid acid conformation, integumentary system, Research Support, Non-U.S. Gov't, High-Throughput Nucleotide Sequencing, Genètica - Tècnica, 3. Good health, Nucleic acids, Sequence analysis DNA, Medical genetics, medicine.medical_specialty, Chromatin Immunoprecipitation, GENES, Investigative Techniques::Epidemiologic Methods::Epidemiologic Research Design::Genome-Wide Association Study [ANALYTICAL, DIAGNOSTIC AND THERAPEUTIC TECHNIQUES, AND EQUIPMENT], Science, Non-P.H.S, Single-nucleotide polymorphism, Scleroderma systemic, Computational biology, Physics and Astronomy(all), Biology, Research Support, Study Characteristics::Meta-Analysis [PUBLICATION CHARACTERISTICS], Genetic polymorphisms, enfermedades de la piel y tejido conjuntivo::enfermedades del tejido conjuntivo::esclerodermia sistémica [ENFERMEDADES], Polymorphism, Single Nucleotide, General Biochemistry, Genetics and Molecular Biology, Functional genomics, Genome-wide association studies, Systemic sclerosis, Rheumatic diseases, CLASSIFICATION, N.I.H, 03 medical and health sciences, Research Support, N.I.H., Extramural, Diacylglycerol kinase theta, Molecular genetics, REVEALS, Journal Article, medicine, Humans, Vascular Diseases, Risk factor, Polymorphism, Genomes, GENOME-WIDE ASSOCIATION, METAANALYSIS, 030203 arthritis & rheumatology, Scleroderma, Systemic, Biochemistry, Genetics and Molecular Biology(all), Polimorfisme genètic, HUMAN-CELLS, Extramural, Bayes Theorem, General Chemistry, Sequence Analysis, DNA, Fibrosis, 030104 developmental biology, Scleroderma (Disease), Skin and Connective Tissue Diseases::Connective Tissue Diseases::Scleroderma, Systemic [DISEASES], técnicas de investigación::métodos epidemiológicos::diseño de la investigación epidemiológica::estudio de asociación genómica completa [TÉCNICAS Y EQUIPOS ANALÍTICOS, DIAGNÓSTICOS Y TERAPÉUTICOS], Nucleic Acid Conformation, VISUALIZATION, lcsh:Q, U.S. Gov't, Esclerodèrmia, Research Support, U.S. Gov't, Non-P.H.S, Metaanàlisi, Genetics and Molecular Biology(all), Genome-Wide Association Study
Abstract

Systemic sclerosis (SSc) is an autoimmune disease that shows one of the highest mortality rates among rheumatic diseases. We perform a large genome-wide association study (GWAS), and meta-analysis with previous GWASs, in 26,679 individuals and identify 27 independent genome-wide associated signals, including 13 new risk loci. The novel associations nearly double the number of genome-wide hits reported for SSc thus far. We define 95% credible sets of less than 5 likely causal variants in 12 loci. Additionally, we identify specific SSc subtype-associated signals. Functional analysis of high-priority variants shows the potential function of SSc signals, with the identification of 43 robust target genes through HiChIP. Our results point towards molecular pathways potentially involved in vasculopathy and fibrosis, two main hallmarks in SSc, and highlight the spectrum of critical cell types for the disease. This work supports a better understanding of the genetic basis of SSc and provides directions for future functional experiments., We thank Sofia Vargas, Sonia García, and Gema Robledo for their excellent technical assistance and all the patients and control donors for their essential collaboration. We thank National DNA Bank Carlos III (University of Salamanca, Spain) that supplied part of the control DNA samples from Spain, WTCCC and EIRA Consortiums, and PopGen 2.0 network. This work was supported by Spanish Ministry of Economy and Competitiveness (grant ref. SAF2015-66761-P), Consejeria de Innovacion, Ciencia y Tecnologia, Junta de Andalucía (P12-BIO-1395), Ministerio de Educación, Cultura y Deporte through the program FPU, Juan de la Cierva fellowship (FJCI-2015-24028), Red de Investigación en Inflamación y Enfermadades Reumaticas (RIER) from Instituto de Salud Carlos III (RD16/0012/0013), and Scleroderma Research Foundation and NIH P50- HG007735 (to H.Y.C.). H.Y.C. is an Investigator of the Howard Hughes Medical Institute. PopGen 2.0 is supported by a grant from the German Ministry for Education and Research (01EY1103). M.D.M and S.A. are supported by grant DoD W81XWH-18-1- 0423 and DoD W81XWH-16-1-0296, respectively

Published
2019

34. Long-term effects of bosentan on quality of life, survival, safety and tolerability in pulmonary arterial hypertension related to connective tissue diseases

Author

Denton, C.P., Pope, J.E., Peter, H.-H., Gabrielli, A., Boonstra, A., van den Hoogen, F.H.J., Riemekasten, G., De Vita, S., Morganti, A., Dolberg, M., Berkani, O., and Guillevin, L.

Subjects
Bosentan -- Dosage and administration, Bosentan -- Research, Pulmonary hypertension -- Care and treatment, Connective tissue diseases -- Complications and side effects, Connective tissue diseases -- Care and treatment, Quality of life -- Research, Health
Published
2008

36. Clinical burden of digital vasculopathy in limited and diffuse cutaneous systemic sclerosis

Author

Nihtyanova, S.I., Brough, G.M., Black, C.M., and Denton, C.P.

Subjects
Scleroderma (Disease) -- Complications and side effects, Scleroderma (Disease) -- Development and progression, Systemic scleroderma -- Complications and side effects, Systemic scleroderma -- Development and progression, Blood circulation disorders -- Development and progression, Fingers -- Diseases, Health
Published
2008

37. Can CCL2 serum levels be used in risk stratification or to monitor treatmen tresponse in systemic sclerosis?

Author

Carulli, M.T., Handler, C., Coghlan, J.G., Black, C.M., and Denton, C.P.

Subjects
Biological markers -- Research, Scleroderma (Disease) -- Care and treatment, Scleroderma (Disease) -- Patient outcomes, Scleroderma (Disease) -- Risk factors, Systemic scleroderma -- Care and treatment, Systemic scleroderma -- Patient outcomes, Systemic scleroderma -- Risk factors, Chemokines -- Research, Chemokines -- Measurement, Health
Published
2008

38. Submaximal exercise testing in the assessment of interstitial lung disease secondary to systemic sclerosis: reproducibility and correlations of the 6-min walk test

Author

Buch, M.H., Denton, C.P., Furst, D.E., Guillevin, L., Rubin, L.J., Wells, A.U., Matucci-Cerinic, M., Riemekasten, G., Emery, P., Chadha-Boreham, H., Charef, P., Roux, S., Black, C.M., and Seibold, J.R.

Subjects
Lung diseases, Interstitial -- Patient outcomes, Lung diseases, Interstitial -- Research, Exercise tests -- Analysis, Health
Published
2007

40. Systemic sclerosis associated pulmonary hypertension: improved survival in the current era

Author

Williams, M.H., Das, C., Handler, C.E., Akram, M.R., Davar, J., Denton, C.P., Smith, C.J., Black, C.M., and Coghlan, J.G.

Subjects
Pulmonary hypertension -- Research, Pulmonary hypertension -- Care and treatment, Pulmonary hypertension -- Patient outcomes, Scleroderma (Disease) -- Patient outcomes, Scleroderma (Disease) -- Care and treatment, Scleroderma (Disease) -- Research, Systemic scleroderma -- Patient outcomes, Systemic scleroderma -- Care and treatment, Systemic scleroderma -- Research, Health
Published
2006

44. Fast track algorithm: How to differentiate a 'scleroderma pattern' from a 'non-scleroderma pattern'

Author

Smith, V., Vanhaecke, A., Herrick, A.L., Distler, O., Guerra, M.G., Denton, C.P., Deschepper, E., Foeldvari, I., Gutierrez, M., Hachulla, E., Ingegnoli, F., Kubo, S., Muller-Ladner, U., Riccieri, V., Sulli, A., Laar, J.M. van, Vonk, M.C., Walker, U.A., Cutolo, M., Smith, V., Vanhaecke, A., Herrick, A.L., Distler, O., Guerra, M.G., Denton, C.P., Deschepper, E., Foeldvari, I., Gutierrez, M., Hachulla, E., Ingegnoli, F., Kubo, S., Muller-Ladner, U., Riccieri, V., Sulli, A., Laar, J.M. van, Vonk, M.C., Walker, U.A., and Cutolo, M.

Abstract

Contains fulltext : 215793.pdf (publisher's version ) (Open Access), OBJECTIVES: This study was designed to propose a simple "Fast Track algorithm" for capillaroscopists of any level of experience to differentiate "scleroderma patterns" from "non-scleroderma patterns" on capillaroscopy and to assess its inter-rater reliability. METHODS: Based on existing definitions to categorise capillaroscopic images as "scleroderma patterns" and taking into account the real life variability of capillaroscopic images described standardly according to the European League Against Rheumatism (EULAR) Study Group on Microcirculation in Rheumatic Diseases, a fast track decision tree, the "Fast Track algorithm" was created by the principal expert (VS) to facilitate swift categorisation of an image as "non-scleroderma pattern (category 1)" or "scleroderma pattern (category 2)". Mean inter-rater reliability between all raters (experts/attendees) of the 8th EULAR course on capillaroscopy in Rheumatic Diseases (Genoa, 2018) and, as external validation, of the 8th European Scleroderma Trials and Research group (EUSTAR) course on systemic sclerosis (SSc) (Nijmegen, 2019) versus the principal expert, as well as reliability between the rater pairs themselves was assessed by mean Cohen's and Light's kappa coefficients. RESULTS: Mean Cohen's kappa was 1/0.96 (95% CI 0.95-0.98) for the 6 experts/135 attendees of the 8th EULAR capillaroscopy course and 1/0.94 (95% CI 0.92-0.96) for the 3 experts/85 attendees of the 8th EUSTAR SSc course. Light's kappa was 1/0.92 at the 8th EULAR capillaroscopy course, and 1/0.87 at the 8th EUSTAR SSc course. CONCLUSION: For the first time, a clinical expert based fast track decision algorithm has been developed to differentiate a "non-scleroderma" from a "scleroderma pattern" on capillaroscopic images, demonstrating excellent reliability when applied by capillaroscopists with varying levels of expertise versus the principal expert and corroborated with external validation.

Published
2019

45. GWAS for systemic sclerosis identifies multiple risk loci and highlights fibrotic and vasculopathy pathways.

Author

Vicente E., Mumbach M.R., Granja J., Beretta L., Simeon C.P., Carreira P., Ortego-Centeno N., Castellvi I., Bossini-Castillo L., Carmona F.D., Orozco G., Hunzelmann N., Distler J.H.W., Franke A., Lunardi C., Moroncini G., Gabrielli A., de Vries-Bouwstra J., Wijmenga C., Koeleman B.P.C., Nordin A., Padyukov L., Hoffmann-Vold A.-M., Lie B., Rios R., Callejas J.L., Vargas-Hitos J.A., Garcia-Portales R., Camps M.T., Fernandez-Nebro A., Gonzalez-Escribano M.F., Garcia-Hernandez F.J., Castillo M.J., Aguirre M.A., Gomez-Gracia I., Fernandez-Gutierrez B., Rodriguez-Rodriguez L., Garcia de la Pena P., Andreu J.L., Fernandez de Castro M., Lopez-Longo F.J., Martinez L., Fonollosa, Guillen A., Espinosa G., Tolosa C., Pros A., Rodriguez-Carballeira M., Narvaez F.J., Rubio-Rivas M., Ortiz-Santamaria, Madronero A.B., Gonzalez-Gay M.A., Diaz B., Trapiella L., Sousa A., Egurbide M.V., Fanlo-Mateo P., Saez-Comet L., Diaz F., Hernandez, Beltran E., Roman-Ivorra J.A., Grau E., Alegre-Sancho J.J., Freire M., Blanco-Garcia F.J., Oreiro N., Witte T., Kreuter A., Riemekasten G., Airo P., Magro C., Voskuyl A.E., Vonk M.C., Hesselstrand R., Proudman S., Stevens W., Nikpour M., Zochling J., Sahhar J., Roddy J., Nash P., Tymms K., Rischmueller M., Lester S., Vyse T., Herrick A.L., Worthington J., Denton C.P., Allanore Y., Brown M.A., Radstake T.R.D.J., Fonseca C., Chang H.Y., Mayes M.D., Martin J., Lopez-Isac E., Acosta-Herrera M., Kerick M., Assassi S., Satpathy A.T., Vicente E., Mumbach M.R., Granja J., Beretta L., Simeon C.P., Carreira P., Ortego-Centeno N., Castellvi I., Bossini-Castillo L., Carmona F.D., Orozco G., Hunzelmann N., Distler J.H.W., Franke A., Lunardi C., Moroncini G., Gabrielli A., de Vries-Bouwstra J., Wijmenga C., Koeleman B.P.C., Nordin A., Padyukov L., Hoffmann-Vold A.-M., Lie B., Rios R., Callejas J.L., Vargas-Hitos J.A., Garcia-Portales R., Camps M.T., Fernandez-Nebro A., Gonzalez-Escribano M.F., Garcia-Hernandez F.J., Castillo M.J., Aguirre M.A., Gomez-Gracia I., Fernandez-Gutierrez B., Rodriguez-Rodriguez L., Garcia de la Pena P., Andreu J.L., Fernandez de Castro M., Lopez-Longo F.J., Martinez L., Fonollosa, Guillen A., Espinosa G., Tolosa C., Pros A., Rodriguez-Carballeira M., Narvaez F.J., Rubio-Rivas M., Ortiz-Santamaria, Madronero A.B., Gonzalez-Gay M.A., Diaz B., Trapiella L., Sousa A., Egurbide M.V., Fanlo-Mateo P., Saez-Comet L., Diaz F., Hernandez, Beltran E., Roman-Ivorra J.A., Grau E., Alegre-Sancho J.J., Freire M., Blanco-Garcia F.J., Oreiro N., Witte T., Kreuter A., Riemekasten G., Airo P., Magro C., Voskuyl A.E., Vonk M.C., Hesselstrand R., Proudman S., Stevens W., Nikpour M., Zochling J., Sahhar J., Roddy J., Nash P., Tymms K., Rischmueller M., Lester S., Vyse T., Herrick A.L., Worthington J., Denton C.P., Allanore Y., Brown M.A., Radstake T.R.D.J., Fonseca C., Chang H.Y., Mayes M.D., Martin J., Lopez-Isac E., Acosta-Herrera M., Kerick M., Assassi S., and Satpathy A.T.

Abstract

Systemic sclerosis (SSc) is an autoimmune disease that shows one of the highest mortality rates among rheumatic diseases. We perform a large genome-wide association study (GWAS), and meta-analysis with previous GWASs, in 26,679 individuals and identify 27 independent genome-wide associated signals, including 13 new risk loci. The novel associations nearly double the number of genome-wide hits reported for SSc thus far. We define 95% credible sets of less than 5 likely causal variants in 12 loci. Additionally, we identify specific SSc subtype-associated signals. Functional analysis of high-priority variants shows the potential function of SSc signals, with the identification of 43 robust target genes through HiChIP. Our results point towards molecular pathways potentially involved in vasculopathy and fibrosis, two main hallmarks in SSc, and highlight the spectrum of critical cell types for the disease. This work supports a better understanding of the genetic basis of SSc and provides directions for future functional experiments.Copyright © 2019, The Author(s).

Published
2019

46. Progressive fibrosing interstitial lung diseases: current practice in diagnosis and management

Author

Wijsenbeek-Lourens, M.S. (Marlies), Kreuter, M. (Michael), Olson, A. (Amy), Fischer, A. (Aryeh), Bendstrup, E. (Elisabeth), Wells, C.D. (Christopher D.), Denton, C.P. (Christopher P.), Mounir, B. (Baher), Zouad-Lejour, L. (Leila), Quaresma, M. (Manuel), Cottin, V. (Vincent), Wijsenbeek-Lourens, M.S. (Marlies), Kreuter, M. (Michael), Olson, A. (Amy), Fischer, A. (Aryeh), Bendstrup, E. (Elisabeth), Wells, C.D. (Christopher D.), Denton, C.P. (Christopher P.), Mounir, B. (Baher), Zouad-Lejour, L. (Leila), Quaresma, M. (Manuel), and Cottin, V. (Vincent)

Abstract

Objective: Some patients with interstitial lung diseases (ILDs) other than idiopathic pulmonary fibrosis (IPF) develop a progressive fibrosing phenotype. We investigated the diagnosis and management of non-IPF ILDs using data from a survey of physicians and from US insurance claims. Methods: Pulmonologists, rheumatologists and internists in France, Germany, Italy, Japan, Spain, UK and US who had managed ≥10 patients with non-IPF ILDs in the past year, including those with progressive fibrosing ILDs, completed an online survey. Data on US insurance and prescription claims were obtained from a repository that aggregates data on claims routed from providers or pharmacies to payers. Results: In May–June 2017, 243 pulmonologists, 203 rheumatologists and 40 internists completed an online survey. Respondents estimated that 18–32% of patients diagnosed with non-IPF ILDs develop progressive fibrosis and that time from symptom onset to death in these patients was 61–80 months. Drug treatment was given to 50–75% of patients with non-IPF progressive fibrosing ILDs. Reasons for patients not being treated included that physicians considered patients to have mild or slowly progressing disease, or did not believe that available treatments are effective or well tolerated. Corticosteroids were the preferred first-line treatment for all types of non-IPF ILD. There was considerable heterogeneity in preferences for second- and third-line treatments. US insurance claims data from 3823 patients indicated that, in 2016, 50–75% of patients with ILDs received drug treatment (mostly corticosteroids) for their ILD. Conclusions: Physicians estimate that 18–32% of patients diagnosed with non-IPF ILDs develop a progressive fibrosing phenotype and that these patients experience significant delays in the diagnosis of ILD and the detection of progressive fibrosis. Between 25% and 50% of patients with progressive fibrosing ILDs do not receive drug therapy. There is an unmet need for effective and wel

Published
2019
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48. Brief Report: IRF4 Newly Identified as a Common Susceptibility Locus for Systemic Sclerosis and Rheumatoid Arthritis in a Cross-Disease Meta-Analysis of Genome-Wide Association Studies

Author

Lopez-Isac, E., Martin, J.E., Assassi, S., Simeon, C.P., Carreira, P., Ortego-Centeno, N., Freire, M., Beltran, E., Narvaez, J., Alegre-Sancho, J.J., Fernandez-Gutierrez, B., Balsa, A., Ortiz, A.M., Gonzalez-Gay, M.A., Beretta, L., Santaniello, A., Bellocchi, C., Lunardi, C., Moroncini, G., Gabrielli, A., Witte, T. de, Hunzelmann, N., Distler, J.H., Riekemasten, G., Mil, A.H.V. van der Helm-va, Vries-Bouwstra, J. de, Magro-Checa, C., Voskuyl, A.E., Vonk, M.C., Molberg, O., Merriman, T., Hesselstrand, R., Nordin, A., Padyukov, L., Herrick, A., Eyre, S., Koeleman, B.P.C., Denton, C.P., Fonseca, C., Radstake, T.R., Worthington, J., Mayes, M.D., and Martin, J.

Subjects
Scleroderma, Systemic, integumentary system, Rheumatoid Arthritis, Systemic Sclerosis, Arthritis, Rheumatoid, Genetic Loci, Risk Factors, IRF4, Interferon Regulatory Factors, Inflammatory diseases Radboud Institute for Health Sciences [Radboudumc 5], Humans, Genetic Predisposition to Disease, Systemic Sclerosis, Rheumatoid Arthritis, IRF4, skin and connective tissue diseases, Genome-Wide Association Study
Abstract

Contains fulltext : 172048.pdf (Publisher’s version ) (Closed access) OBJECTIVE: Systemic sclerosis (SSc) and rheumatoid arthritis (RA) are autoimmune diseases that have similar clinical and immunologic characteristics. To date, several shared SSc-RA genetic loci have been identified independently. The aim of the current study was to systematically search for new common SSc-RA loci through an interdisease meta-genome-wide association (meta-GWAS) strategy. METHODS: The study was designed as a meta-analysis combining GWAS data sets of patients with SSc and patients with RA, using a strategy that allowed identification of loci with both same-direction and opposite-direction allelic effects. The top single-nucleotide polymorphisms were followed up in independent SSc and RA case-control cohorts. This allowed an increase in the sample size to a total of 8,830 patients with SSc, 16,870 patients with RA, and 43,393 healthy controls. RESULTS: This cross-disease meta-analysis of the GWAS data sets identified several loci with nominal association signals (P < 5 x 10(-6) ) that also showed evidence of association in the disease-specific GWAS scans. These loci included several genomic regions not previously reported as shared loci, as well as several risk factors that were previously found to be associated with both diseases. Follow-up analyses of the putatively new SSc-RA loci identified IRF4 as a shared risk factor for these 2 diseases (Pcombined = 3.29 x 10(-12) ). Analysis of the biologic relevance of the known SSc-RA shared loci identified the type I interferon and interleukin-12 signaling pathways as the main common etiologic factors. CONCLUSION: This study identified a novel shared locus, IRF4, for the risk of SSc and RA, and highlighted the usefulness of a cross-disease GWAS meta-analysis strategy in the identification of common risk loci.

Published
2016

50. Changes in macrophage transcriptome associate with systemic sclerosis and mediate GSDMA contribution to disease risk

Author

Moreno-Moral, Aida, Bagnati, M., Koturan, S., Ko, J.H., Fonseca, C., Harmston, N., Game, Laurence, Martín, J., Ong, V., Abraham, D. J., Denton, C.P., Behmoaras, J., Petretto, E., Medical Research Council (UK), Duke-NUS Medical School, Arthritis Research UK, NHS Foundation Trust, and Medical Research Council (MRC)

Subjects
Adult, Male, SUSCEPTIBILITY LOCI, Adolescent, Genotyping Techniques, systemic sclerosis, Quantitative Trait Loci, macrophage, VARIANTS, IMMUNITY, PYROPTOSIS, 1117 Public Health and Health Services, Young Adult, Rheumatology, Risk Factors, Humans, Genetic Predisposition to Disease, GENOME-WIDE ASSOCIATION, Child, skin and connective tissue diseases, Basic and Translational Research, GENE-EXPRESSION, Skin, Science & Technology, Scleroderma, Systemic, IDENTIFICATION, integumentary system, Macrophages, 1103 Clinical Sciences, TIME, Neoplasm Proteins, Arthritis & Rheumatology, 1107 Immunology, eQTL analysis, Case-Control Studies, Child, Preschool, CELLS, Female, Transcriptome, Life Sciences & Biomedicine, GSDMA, Signal Transduction
Abstract

Objectives Several common and rare risk variants have been reported for systemic sclerosis (SSc), but the effector cell(s) mediating the function of these genetic variants remains to be elucidated. While innate immune cells have been proposed as the critical targets to interfere with the disease process underlying SSc, no studies have comprehensively established their effector role. Here we investigated the contribution of monocyte-derived macrophages (MDMs) in mediating genetic susceptibility to SSc. Methods We carried out RNA sequencing and genome-wide genotyping in MDMs from 57 patients with SSc and 15 controls. Our differential expression and expression quantitative trait locus (eQTL) analysis in SSc was further integrated with epigenetic, expression and eQTL data from skin, monocytes, neutrophils and lymphocytes. Results We identified 602 genes upregulated and downregulated in SSc macrophages that were significantly enriched for genes previously implicated in SSc susceptibility (P=5×10 -4), and 270 cis-regulated genes in MDMs. Among these, GSDMA was reported to carry an SSc risk variant (rs3894194) regulating expression of neighbouring genes in blood. We show that GSDMA is upregulated in SSc MDMs (P=8.4×10 -4) but not in the skin, and is a significant eQTL in SSc macrophages and lipopolysaccharide/interferon gamma (IFNα)-stimulated monocytes. Furthermore, we identify an SSc macrophage transcriptome signature characterised by upregulation of glycolysis, hypoxia and mTOR signalling and a downregulation of IFNα response pathways. Conclusions Our data further establish the link between macrophages and SSc, and suggest that the contribution of the rs3894194 risk variant to SSc susceptibility can be mediated by GSDMA expression in macrophages., Fundingthis work was supported by the Medical research Council (Mr/M004716/1 to JB and Ep, and Mr/n01121x/1 to JB), by the nMrC (grant CBrG15may062) and duke-nUS Medical School (to Ep), by the Arthritis research UK (19427), Scleroderma & raynaud’s UK and the royal Free Charity (to dJA, Vo and Cpd), and by grant SAF2015 66761 p (to JM)

Published
2018

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